Evidence for a connection between coronavirus disease-19 and exposure to radiofrequency radiation from wireless communications including 5G

md_a

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Abstract​

Background and Aim:​

Coronavirus disease (COVID-19) public health policy has focused on the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) virus and its effects on human health while environmental factors have been largely ignored. In considering the epidemiological triad (agent-host-environment) applicable to all disease, we investigated a possible environmental factor in the COVID-19 pandemic: ambient radiofrequency radiation from wireless communication systems including microwaves and millimeter waves. SARS-CoV-2, the virus that caused the COVID-19 pandemic, surfaced in Wuhan, China shortly after the implementation of city-wide (fifth generation [5G] of wireless communications radiation [WCR]), and rapidly spread globally, initially demonstrating a statistical correlation to international communities with recently established 5G networks. In this study, we examined the peer-reviewed scientific literature on the detrimental bioeffects of WCR and identified several mechanisms by which WCR may have contributed to the COVID-19 pandemic as a toxic environmental cofactor. By crossing boundaries between the disciplines of biophysics and pathophysiology, we present evidence that WCR may: (1) cause morphologic changes in erythrocytes including echinocyte and rouleaux formation that can contribute to hypercoagulation; (2) impair microcirculation and reduce erythrocyte and hemoglobin levels exacerbating hypoxia; (3) amplify immune system dysfunction, including immunosuppression, autoimmunity, and hyperinflammation; (4) increase cellular oxidative stress and the production of free radicals resulting in vascular injury and organ damage; (5) increase intracellular Ca2+ essential for viral entry, replication, and release, in addition to promoting pro-inflammatory pathways; and (6) worsen heart arrhythmias and cardiac disorders.

3. Results​

Table 1 lists the manifestations common to COVID-19 including disease progression and the corresponding adverse bioeffects from WCR exposure. Although these effects are delineated into categories — blood changes, oxidative stress, immune system disruption and activation, increased intracellular calcium (Ca2+), and cardiac effects — it must be emphasized that these effects are not independent of each other. For example, blood clotting and inflammation have overlapping mechanisms, and oxidative stress is implicated in erythrocyte morphological changes as well as in hypercoagulation, inflammation, and organ damage.

Table 1​

Bioeffects of Wireless Communication Radiation (WCR) exposure in relation to COVID-19 manifestations and their progression
Wireless communications radiation (WCR) exposure bioeffects​
COVID-19 manifestations​
Blood changes
 Short-term: rouleaux, echinocytes
 Long-term: reduced blood clotting time, reduced hemoglobin, hemodynamic disorders​
Blood changes
 Rouleaux, echinocytes
 Hemoglobin effects; vascular effects
 →Reduced hemoglobin in severe disease; autoimmune hemolytic anemia; hypoxemia and hypoxia
 →Endothelial injury; impaired microcirculation; hypercoagulation; disseminated intravascular coagulopathy (DIC); pulmonary embolism; stroke​
Oxidative stress
 Glutathione level decrease; free radicals and lipid peroxide increase; superoxide dismutase activity decrease; oxidative injury in tissues and organs​
Oxidative stress
 Glutathione level decrease; free radical increase and damage; apoptosis→Oxidative injury; organ damage in severe disease​
Immune system disruption and activation
 Immune suppression in some studies; immune hyperactivation in other studies
 Long-term: suppression of T-lymphocytes; inflammatory biomarkers increased; autoimmunity; organ injury​
Immune system disruption and activation
 Decreased production of T-lymphocytes; elevated inflammatory biomarkers.
 →Immune hyperactivation and inflammation; cytokine storm in severe disease; cytokine-induced hypo-perfusion with resulting hypoxia; organ injury; organ failure​
Increased intracellular calcium
 From activation of voltage-gated calcium channels on cell membranes, with numerous secondary effects​
Increased intracellular calcium
 →Increased virus entry, replication, and release
 →Increased NF-κB, pro-inflammatory processes, coagulation, and thrombosis​
Cardiac effects
 Up-regulation of sympathetic nervous system; palpitations and arrhythmias​
Cardiac effects
 Arrhythmias
 →Myocarditis; myocardial ischemia; cardiac injury; cardiac failure​
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Supportive evidence including study details and citations are provided in the text under each subject heading, i.e., blood changes, oxidative stress, etc.

3.1. Blood changes​

WCR exposure can cause morphologic changes in blood readily seen through phase contrast or dark-field microscopy of live peripheral blood samples. In 2013, Havas observed erythrocyte aggregation including rouleaux (rolls of stacked red blood cells) in live peripheral blood samples following 10 min human exposure to a 2.4 GHz cordless phone [50]. Although not peer reviewed, one of us (Rubik) investigated the effect of 4G LTE mobile phone radiation on the peripheral blood of ten human subjects, each of whom had been exposed to cell phone radiation for two consecutive 45-min intervals [51]. Two types of effects were observed: increased stickiness and clumping of red blood cells with rouleaux formation, and subsequent formation of echinocytes (spiky red blood cells). Red blood cell clumping and aggregation are known to be actively involved in blood clotting [52]. The prevalence of this phenomenon on exposure to WCR in the human population has not yet been determined. Larger controlled studies should be performed to further investigate this phenomenon.
Similar red blood cell changes have been described in peripheral blood of COVID-19 patients [53]. Rouleaux formation has been observed in 1/3 of COVID-19 patients, whereas spherocytes and echinocyte formation is more variable. Spike protein engagement with ACE2 receptors on cells lining the blood vessels can lead to endothelial damage, even when isolated [54]. Rouleaux formation, particularly in the setting of underlying endothelial damage, can clog the microcirculation, impeding oxygen transport, contributing to hypoxia, and increasing the risk of thrombosis [52]. Thrombogenesis associated with SARS-CoV-2 infection may also be caused by direct viral binding to ACE2 receptors on platelets [55].
Additional blood effects have been observed in both humans and animals exposed to WCR. In 1977, a Russian study reported that rodents irradiated with 5 – 8 mm waves (60 – 37 GHz) at 1 mW/cm2 for 15 min/day over 60 days developed hemodynamic disorders, suppressed red blood cell formation, reduced hemoglobin, and an inhibition of oxygen utilization (oxidative phosphorylation by the mitochondria) [56]. In 1978, a 3-year Russian study on 72 engineers exposed to millimeter wave generators emitting at 1 mW/cm2 or less showed a decrease in their hemoglobin levels and red blood cell counts, and a tendency toward hypercoagulation, whereas a control group showed no changes [57]. Such deleterious hematologic effects from WCR exposure may also contribute to the development of hypoxia and blood clotting observed in COVID-19 patients.
It has been proposed that the SARS-CoV-2 virus attacks erythrocytes and causes degradation of hemoglobin [11]. Viral proteins may attack the 1-beta chain of hemoglobin and capture the porphyrin, along with other proteins from the virus catalyzing the dissociation of iron from heme [58]. In principle this would reduce the number of functional erythrocytes and cause the release of free iron ions that could cause oxidative stress, tissue damage, and hypoxia. With hemoglobin partially destroyed and lung tissue damaged by inflammation, patients would be less able to exchange carbon dioxide (CO2) and oxygen (O2), and would become oxygen depleted. In fact, some COVID-19 patients show reduced hemoglobin levels, measuring 7.1 g/L and even as low as 5.9 g/L in severe cases [59]. Clinical studies of almost 100 patients from Wuhan revealed that the hemoglobin levels in the blood of most patients infected with SARS-CoV-2 are significantly lowered resulting in compromised delivery of oxygen to tissues and organs [60]. In a meta-analysis of four studies with a total of 1210 patients and 224 with severe disease, hemoglobin values were reduced in COVID-19 patients with severe disease compared to those with milder forms [59]. In another study on 601 COVID-19 patients, 14.7% of anemic COVID-19 ICU patients and 9% of non-ICU COVID-19 patients had autoimmune hemolytic anemia [61]. In patients with severe COVID-19 disease, decreased hemoglobin along with elevated erythrocyte sedimentation rate (ESR), C-reactive protein, lactate dehydrogenase, albumin [62], serum ferritin [63], and low oxygen saturation [64] provide additional support for this hypothesis. In addition, packed red blood cell transfusion may promote recovery of COVID-19 patients with acute respiratory failure [65].
In short, both WCR exposure and COVID-19 may cause deleterious effects on red blood cells and reduced hemoglobin levels contributing to hypoxia in COVID-19. Endothelial injury may further contribute to hypoxia and many of the vascular complications seen in COVID-19 [66] that are discussed in the next section.

3.2. Oxidative stress​

Oxidative stress is a non-specific pathological condition reflecting an imbalance between an increased production of ROS and an inability of the organism to detoxify the ROS or to repair the damage they cause to biomolecules and tissues [67]. Oxidative stress can disrupt cell signaling, cause the formation of stress proteins, and generate highly reactive free radicals, which can cause DNA and cell membrane damage.
SARS-CoV-2 inhibits intrinsic pathways designed to reduce ROS levels, thereby increasing morbidity. Immune dysregulation, that is, the upregulation of interleukin (IL)-6 and tumor necrosis factor α (TNF-α) [68] and suppression of interferon (IFN) α and IFN β [69] have been identified in the cytokine storm accompanying severe COVID-19 infections and generates oxidative stress [10]. Oxidative stress and mitochondrial dysfunction may further perpetuate the cytokine storm, worsening tissue damage, and increasing the risk of severe illness and death.
Similarly low-level WCR generates ROS in cells that cause oxidative damage. In fact, oxidative stress is considered to be one of the primary mechanisms in which WCR exposure causes cellular damage. Among 100 currently available peer-reviewed studies investigating oxidative effects of low-intensity WCR, 93 of these studies confirmed that WCR induces oxidative effects in biological systems [17]. WCR is an oxidative agent with a high pathogenic potential especially when exposure is continuous [70].
Oxidative stress is also an accepted mechanism causing endothelial damage [71]. This may manifest in patients with severe COVID-19 in addition to increasing the risk for blood clot formation and worsening hypoxemia [10]. Low levels of glutathione, the master antioxidant, have been observed in a small group of COVID-19 patients, with the lowest level found in the most severe cases [72]. The finding of low glutathione levels in these patients further supports oxidative stress as a component of this disease [72]. In fact, glutathione, the major source of sulfhydryl-based antioxidant activity in the human body, may be pivotal in COVID-19 [73]. Glutathione deficiency has been proposed as the most likely cause of serious manifestations in COVID-19 [72]. The most common co-morbidities, hypertension [74]; obesity [75]; diabetes [76]; and chronic obstructive pulmonary disease [74] support the concept that pre-existing conditions causing low levels of glutathione may work synergistically to create the “perfect storm” for both the respiratory and vascular complications of severe infection. Another paper citing two cases of COVID-19 pneumonia treated successfully with intravenous glutathione also supports this hypothesis [77].
Many studies report oxidative stress in humans exposed to WCR. Peraica et al. [78] found diminished blood levels of glutathione in workers exposed to WCR from radar equipment (0.01 mW/cm2 – 10 mW/cm2; 1.5 – 10.9 GHz). Garaj-Vrhovac et al. [79] studied bioeffects following exposure to non-thermal pulsed microwaves from marine radar (3 GHz, 5.5 GHz, and 9.4 GHz) and reported reduced glutathione levels and increased malondialdehyde (marker for oxidative stress) in an occupationally exposed group [79]. Blood plasma of individuals residing near mobile phone base stations showed significantly reduced glutathione, catalase, and superoxide dismutase levels over unexposed controls [80]. In a study on human exposure to WCR from mobile phones, increased blood levels of lipid peroxide were reported, while enzymatic activities of superoxide dismutase and glutathione peroxidase in the red blood cells decreased, indicating oxidative stress [81].
In a study on rats exposed to 2450 MHz (wireless router frequency), oxidative stress was implicated in causing red blood cell lysis (hemolysis) [82]. In another study, rats exposed to 945 MHz (base station frequency) at 0.367 mW/cm2 for 7 h/day, over 8 days, demonstrated low glutathione levels and increased malondialdehyde and superoxide dismutase enzyme activity, hallmarks for oxidative stress [83]. In a long-term controlled study on rats exposed to 900 MHz (mobile phone frequency) at 0.0782 mW/cm2 for 2 h/day for 10 months, there was a significant increase in malondialdehyde and total oxidant status over controls [84]. In another long-term controlled study on rats exposed to two mobile phone frequencies, 1800 MHz and 2100 MHz, at power densities 0.04 – 0.127 mW/cm2 for 2 h/day over 7 months, significant alterations in oxidant-antioxidant parameters, DNA strand breaks, and oxidative DNA damage were found [85].
There is a correlation between oxidative stress and thrombogenesis [86]. ROS can cause endothelial dysfunction and cellular damage. The endothelial lining of the vascular system contains ACE2 receptors that are targeted by SARS-CoV-2. The resulting endotheliitis can cause luminal narrowing and result in diminished blood flow to downstream structures. Thrombi in arterial structures can further obstruct blood flow causing ischemia and/or infarcts in involved organs, including pulmonary emboli and strokes. Abnormal blood coagulation leading to micro-emboli was a recognized complication early in the history of COVID-19 [87]. Out of 184 ICU COVID-19 patients, 31% showed thrombotic complications [88]. Cardiovascular clotting events are a common cause of COVID-19 deaths [12]. Pulmonary embolism, disseminated intravascular coagulation (DIC), liver, cardiac, and renal failure have all been observed in COVID-19 patients [89].
Patients with the highest cardiovascular risk factors in COVID-19 includ males, the elderly, diabetics, and obese and hypertensive patients. However, increased incidence of strokes in younger patients with COVID-19 has also been described [90].
Oxidative stress is caused by WCR exposure and is known to be implicated in cardiovascular disease. Ubiquitous environmental exposure to WCR may contribute to cardiovascular disease by creating a chronic state of oxidative stress [91]. This would lead to oxidative damage to cellular constituents and alter signal transduction pathways. In addition, pulse-modulated WCR can cause oxidative injury in liver, lung, testis, and heart tissues mediated by lipid peroxidation, increased levels of nitric oxides, and suppression of the antioxidant defense mechanism [92].
In summary, oxidative stress is a major component in the pathophysiology of COVID-19 as well as in cellular damage caused by WCR exposure.

3.3. Immune system disruption and activation​

When SARS-CoV-2 first infects the human body, it attacks cells lining the nose, throat, and upper airway harboring ACE2 receptors. Once the virus gains access to a host cell through one of its spike proteins, which are the multiple protuberances projecting from the viral envelope that bind to ACE2 receptors, it converts the cell into a virus self-replicating entity.
In response to COVID-19 infection, both an immediate systemic innate immune response as well as a delayed adaptive response has been shown to occur [93]. The virus can also cause a dysregulation of the immune response, particularly in the decreased production of T-lymphocytes. [94]. Severe cases tend to have lower lymphocyte counts, higher leukocyte counts and neutrophil-lymphocyte ratios, as well as lower percentages of monocytes, eosinophils, and basophils [94]. Severe cases of COVID-19 show the greatest impairment in T-lymphocytes.
In comparison, low-level WCR studies on laboratory animals also show impaired immune function [95]. Findings include physical alterations in immune cells, a degradation of immunological responses, inflammation, and tissue damage. Baranski [96] exposed guinea pigs and rabbits to continuous or pulse-modulated 3000 MHz microwaves at an average power density of 3.5 mW/cm2 for 3 h/day over 3 months and found nonthermal changes in lymphocyte counts, abnormalities in nuclear structure, and mitosis in the erythroblastic cell series in the bone marrow and in lymphoid cells in lymph nodes and spleen. Other investigators have shown diminished T-lymphocytes or suppressed immune function in animals exposed to WCR. Rabbits exposed to 2.1 GHz at 5mW/cm2 for 3 h/day, 6 days/week, for 3 months, showed suppression of T-lymphocytes [97]. Rats exposed to 2.45 GHz and 9.7 GHz for 2 h/day, 7 days/week, for 21 months showed a significant decrease in the levels of lymphocytes and an increase in mortality at 25 months in the irradiated group [98]. Lymphocytes harvested from rabbits irradiated with 2.45 GHz for 23 h/day for 6 months show a significant suppression in immune response to a mitogen [99].
In 2009, Johansson conducted a literature review, which included the 2007 Bioinitiative Report. He concluded that electromagnetic fields (EMF) exposure, including WCR, can disturb the immune system and cause allergic and inflammatory responses at exposure levels significantly less than current national and international safety limits and raise the risk for systemic disease [100]. A review conducted by Szmigielski in 2013 concluded that weak RF/microwave fields, such as those emitted by mobile phones, can affect various immune functions both in vitro and in vivo [101]. Although the effects are historically somewhat inconsistent, most research studies document alterations in the number and activity of immune cells from RF exposure. In general, short-term exposure to weak microwave radiation may temporarily stimulate an innate or adaptive immune response, but prolonged irradiation inhibits those same functions.
In the acute phase of COVID-19 infection, blood tests demonstrate elevated ESR, C-reactive protein, and other elevated inflammatory markers [102], typical of an innate immune response. Rapid viral replication can cause death of epithelial and endothelial cells and result in leaky blood vessels and pro-inflammatory cytokine release [103]. Cytokines, proteins, peptides, and proteoglycans that modulate the body’s immune response, are modestly elevated in patients with mild-to-moderate disease severity [104]. In those with severe disease, an uncontrolled release of pro-inflammatory cytokines--a cytokine storm--can occur. Cytokine storms originate from an imbalance in T-cell activation with dysregulated release of IL-6, IL-17, and other cytokines. Programmed cell death (apoptosis), ARDS, DIC, and multi-organ system failure can all result from a cytokine storm and increase the risk of mortality.
By comparison, Soviet researchers found in the 1970s that radiofrequency radiation can damage the immune system of animals. Shandala [105] exposed rats to 0.5 mW/cm2 microwaves for 1 month, 7 h/day, and found impaired immune competence and induction of autoimmune disease. Rats irradiated with 2.45 GHz at 0.5 mW/cm2 for 7 h daily for 30 days produced autoimmune reactions, and 0.1 – 0.5 mW/cm2 produced persistent pathological immune reactions [106]. Exposure to microwave radiation, even at low levels (0.1 – 0.5 mW/cm2), can impair immune function, causing physical alterations in the essential cells of the immune system and a degradation of immunologic responses [107]. Szabo et al. [108] examined the effects of 61.2 GHz exposure on epidermal keratinocytes and found an increase in IL-1b, a pro-inflammatory cytokine. Makar et al. [109] found that immunosuppressed mice irradiated 30 min/day for 3 days by 42.2 GHz showed increased levels of TNF-α, a cytokine produced by macrophages.
In short, COVID-19 can lead to immune dysregulation as well as cytokine storms. By comparison, exposure to low-level WCR as observed in animal studies can also compromise the immune system, with chronic daily exposure producing immunosuppression or immune dysregulation including hyperactivation.

3.4. Increased intracellular calcium​

In 1992, Walleczek first suggested that ELF electromagnetic fields (<3000 Hz) may be affecting membrane-mediated Ca2+ signaling and lead to increased intracellular Ca2+ [110]. The mechanism of irregular gating of voltage-gated ion channels in cell membranes by polarized and coherent, oscillating electric or magnetic fields was first presented in 2000 and 2002 [40,111]. Pall [112] in his review of WCR-induced bioeffects combined with use of calcium channel blockers (CCB) noted that voltage-gated calcium channels play a major role in WCR bioeffects. Increased intracellular Ca+2 results from the activation of voltage-gated calcium channels, and this may be one of the primary mechanisms of action of WCR on organisms.
Intracellular Ca2+ is essential for virus entry, replication, and release. It has been reported that some viruses can manipulate voltage-gated calcium channels to increase intracellular Ca2+ thereby facilitating viral entry and replication [113]. Research has shown that the interaction between a virus and voltage-gated calcium channels promote virus entry at the virus-host cell fusion step [113]. Thus, after the virus binds to its receptor on a host cell and enters the cell through endocytosis, the virus takes over the host cell to manufacture its components. Certain viral proteins then manipulate calcium channels, thereby increasing intracellular Ca2+, which facilitates further viral replication.
Even though direct evidence has not been reported, there is indirect evidence that increased intracellular Ca2+ may be involved in COVID-19. In a recent study, elderly hospitalized COVID-19 patients treated with CCBs, amlodipine or nifedipine, were more likely to survive and less likely to require intubation or mechanical ventilation than controls [114]. Furthermore, CCBs strongly limit SARS-CoV-2 entry and infection in cultured epithelial lung cells [115]. CCBs also block the increase of intracellular Ca2+ caused by WCR exposure as well as exposure to other electromagnetic fields [112].
Intracellular Ca2+ is a ubiquitous second messenger relaying signals received by cell surface receptors to effector proteins involved in numerous biochemical processes. Increased intracellular Ca2+ is a significant factor in upregulation of transcription nuclear factor KB (NF-κB) [116], an important regulator of pro-inflammatory cytokine production as well as coagulation and thrombotic cascades. NF-κB is hypothesized to be a key factor underlying severe clinical manifestations of COVID-19 [117].
In short, WCR exposure, therefore, may enhance the infectivity of the virus by increasing intracellular Ca2+ that may also indirectly contribute to inflammatory processes and thrombosis.

3.5. Cardiac effects​

Cardiac arrhythmias are more commonly encountered in critically ill patients with COVID-19 [118]. The cause for arrhythmia in COVID-19 patients is multifactorial and includes cardiac and extra-cardiac processes [119]. Direct infection of the heart muscle by SARS-CoV-19 causing myocarditis, myocardial ischemia caused by a variety of etiologies, and heart strain secondary to pulmonary or systemic hypertension can result in cardiac arrhythmia. Hypoxemia caused by diffuse pneumonia, ARDS, or extensive pulmonary emboli represent extra-cardiac causes of arrhythmia. Electrolyte imbalances, intravascular fluid imbalance, and side effects from pharmacologic regimens can also result in arrhythmias in COVID-19 patients. Patients admitted to ICUs have been shown to have a higher increase in cardiac arrhythmias, 16.5% in one study [120]. Although no correlation between EMFs and arrhythmia in COVID-19 patients has been described in the literature, many ICUs are equipped with wireless patient monitoring equipment and communication devices producing a wide range of EMF pollution [121].
COVID-19 patients commonly show increased levels of cardiac troponin, indicating damage to the heart muscle [122]. Cardiac damage has been associated with arrhythmias and increased mortality. Cardiac injury is thought to be more often secondary to pulmonary emboli and viral sepsis, but direct infection of the heart, that is, myocarditis, can occur through direct viral binding to ACE2 receptors on cardiac pericytes, affecting local, and regional cardiac blood flow [60].
Immune system activation along with alterations in the immune system may result in atherosclerotic plaque instability and vulnerability, that is, presenting an increased risk for thrombus formation, and contributing to development of acute coronary events and cardiovascular disease in COVID-19.
Regarding WCR exposure bioeffects, in 1969 Christopher Dodge of the Biosciences Division, U.S. Naval Observatory in Washington DC, reviewed 54 papers and reported that radiofrequency radiation can adversely affect all major systems of the body, including impeding blood circulation; altering blood pressure and heart rate; affecting electrocardiograph readings; and causing chest pain and heart palpitations [123]. In the 1970s Glaser reviewed more than 2000 publications on radiofrequency radiation exposure bioeffects and concluded that microwave radiation can alter the electrocardiogram, cause chest pain, hypercoagulation, thrombosis, and hypertension in addition to myocardial infarction [27,28]. Seizures, convulsions, and alteration of the autonomic nervous system response (increased sympathetic stress response) have also been observed.
Since then, many other researchers have concluded that WCR exposure can affect the cardiovascular system. Although the nature of the primary response to millimeter waves and consequent events are poorly understood, a possible role for receptor structures and neural pathways in the development of continuous millimeter wave-induced arrhythmia has been proposed [47]. In 1997, a review reported that some investigators discovered cardiovascular changes including arrhythmias in humans from long-term low-level exposure to WCR including microwaves [124]. However, the literature also shows some unconfirmed findings as well as some contradictory findings [125]. Havas et al. [126] reported that human subjects in a controlled, double-blinded study were hyper-reactive when exposed to 2.45 GHz, digitally pulsed (100 Hz) microwave radiation, developing either an arrhythmia or tachycardia and upregulation of the sympathetic nervous system, which is associated with the stress response. Saili et al. [127] found that exposure to Wi-Fi (2.45 GHz pulsed at 10 Hz) affects heart rhythm, blood pressure, and the efficacy of catecholamines on the cardiovascular system, indicating that WCR can act directly and/or indirectly on the cardiovascular system. Most recently, Bandara and Weller [91] present evidence that people who live near radar installations (millimeter waves: 5G frequencies) have a greater risk of developing cancer and experiencing heart attacks. Similarly, those occupationally exposed have a greater risk of coronary heart disease. Microwave radiation affects the heart, and some people are more vulnerable if they have an underlying heart abnormality [128]. More recent research suggests that millimeter waves may act directly on the pacemaker cells of the sinoatrial node of the heart to change the beat frequency, which may underlie arrhythmias and other cardiac issues [47].
In short, both COVID-19 and WCR exposure can affect the heart and cardiovascular system, directly and/or indirectly.
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4. Discussion​

Epidemiologists, including those at the CDC, consider multiple causal factors when evaluating the virulence of an agent and understanding its ability to spread and cause disease. Most importantly, these variables include environmental cofactors and the health status of the host. Evidence from the literature summarized here suggests a possible connection between several adverse health effects of WCR exposure and the clinical course of COVID-19 in that WCR may have worsened the COVID-19 pandemic by weakening the host and exacerbating COVID-19 disease. However, none of the observations discussed here prove this linkage. Specifically, the evidence does not confirm causation. Clearly COVID-19 occurs in regions with little wireless communication. Furthermore, the relative morbidity caused by WCR exposure in COVID-19 is unknown.
We recognize that many factors have influenced the pandemic’s course. Before restrictions were imposed, travel patterns facilitated the seeding of the virus, causing early rapid global spread. Population density, higher mean population age, and socioeconomic factors certainly influenced early viral spread. Air pollution, especially particulate matter PM2.5 (2.5 micro-particulates), likely increased symptoms in patients with COVID-19 lung disease [129].
We postulate that WCR possibly contributed to the early spread and severity of COVID-19. Once an agent becomes established in a community, its virulence increases [130]. This premise can be applied to the COVID-19 pandemic. We surmise that “hot spots” of the disease that initially spread around the world were perhaps seeded by air travel, which in some areas were associated with 5G implementation. However, once the disease became established in those communities, it was able to spread more easily to neighboring regions where populations were less exposed to WCR. Second and third waves of the pandemic disseminated widely throughout communities with and without WCR, as might be expected.
The COVID-19 pandemic has offered us an opportunity to delve further into the potential adverse effects of WCR exposure on human health. Human exposure to ambient WCR significantly increased in 2020 as a “side effect” to the pandemic. Stay-at-home measures designed to reduce the spread of COVID-19 inadvertently resulted in greater public exposure to WCR, as people conducted more business and school related activities through wireless communications. Telemedicine created another source of WCR exposure. Even hospital inpatients, particular ICU patients, experienced increased WCR exposure as new monitoring devices utilized wireless communication systems that may exacerbate health disorders. It would potentially provide valuable information to measure ambient WCR power densities in home and work environments when comparing disease severity in patient populations with similar risk factors.
The question of causation could be investigated in future studies. For example, a clinical study could be conducted in COVID-19 patient populations with similar risk factors, to measure the WCR daily dose in COVID-19 patients and look for a correlation with disease severity and progression over time. As wireless device carrier frequencies and modulations may differ, and the power densities of WCR fluctuate constantly at a given location, this study would require patients to wear personal microwave dosimeters (monitoring badges). In addition, controlled laboratory studies could be conducted on animals, for example, humanized mice infected with SARS-CoV-2, in which groups of animals exposed to minimal WCR (control group) as well as medium and high power densities of WCR could be compared for disease severity and progression.
A major strength of this paper is that the evidence rests on a large body of scientific literature reported by many scientists worldwide and over several decades--experimental evidence of adverse bioeffects of WCR exposure at nonthermal levels on humans, animals, and cells. The Bioinitiative Report [42], updated in 2020, summarizes hundreds of peer-reviewed scientific papers documenting evidence of nonthermal effects from exposures ≤1 mW/cm2. Even so, some laboratory studies on the adverse health effects of WCR have sometimes utilized power densities exceeding 1mW/cm2. In this paper, almost all of the studies that we reviewed included experimental data at power densities ≤1 mW/cm2.
A potential criticism of this paper is that adverse bioeffects from nonthermal exposures are not yet universally accepted in science. Moreover, they are not yet considered in establishing public health policy in many nations. Decades ago, Russians and Eastern Europeans compiled considerable data on nonthermal bioeffects, and subsequently set guidelines at lower radiofrequency radiation exposure limits than the US and Canada, that is, below levels where nonthermal effects are observed. However, the Federal Communications Commission (FCC, a US government entity) and ICNIRP guidelines operate on thermal limits based on outdated data from decades ago, allowing the public to be exposed to considerably higher radiofrequency radiation power densities. Regarding 5G, the telecommunication industry claims that it is safe because it complies with current radiofrequency radiation exposure guidelines of the FCC and ICNIRP. These guidelines were established in 1996 [131], are antiquated, and are not safety standards. Thus, there are no universally accepted safety standards for wireless communication radiation exposure. Recently international bodies, such as the EMF Working Group of the European Academy of Environmental Medicine, have proposed much lower guidelines, taking into account nonthermal bioeffects from WCR exposure in multiple sources [132].
Another weakness of this paper is that some of the bioeffects from WCR exposure are inconsistently reported in the literature. Replicated studies are often not true replications. Small differences in method, including unreported details, such as prior history of exposure of the organisms, non-uniform body exposure, and other variables can lead to inadvertent inconsistency. Moreover, not surprisingly, industry-sponsored studies tend to show less adverse bioeffects than studies conducted by independent researchers, suggesting industry bias [133]. Some experimental studies that are not industry-sponsored have also shown no evidence of harmful effects of WCR exposure. It is noteworthy, however, that studies employing real-life WCR exposures from commercially available devices have shown high consistency in revealing adverse effects [134].
WCR bioeffects depend on specific values of wave parameters including frequency, power density, polarization, exposure duration, modulation characteristics, as well as the cumulative history of exposure and background levels of electromagnetic, electric and magnetic fields. In laboratory studies, bioeffects observed also depend on genetic parameters and physiological parameters such as oxygen concentration [135]. The reproducibility of bioeffects of WCR exposure has sometimes been difficult due to failure to report and/or control all of these parameters. Similar to ionizing radiation, the bioeffects of WCR exposure can be subdivided into deterministic, that is, dose-dependent effects and stochastic effects that are seemingly random. Importantly, WCR bioeffects can also involve “response windows” of specific parameters whereby extremely low-level fields can have disproportionally detrimental effects [136]. This nonlinearity of WCR bioeffects can result in biphasic responses such as immune suppression from one range of parameters, and immune hyperactivation from another range of parameters, leading to variations that may appear inconsistent.
In gathering reports and examining existing data for this paper, we looked for outcomes providing evidence to support a proposed connection between the bioeffects of WCR exposure and COVID-19. We did not make an attempt to weigh the evidence. The radiofrequency radiation exposure literature is extensive and currently contains over 30,000 research reports dating back several decades. Inconsistencies in nomenclature, reporting of details, and cataloging of keywords make it difficult to navigate this enormous literature.
Another shortcoming of this paper is that we do not have access to experimental data on 5G exposures. In fact, little is known about population exposure from real-world WCR, which includes exposure to WCR infrastructure and the plethora of WCR emitting devices. In relation to this, it is difficult to accurately quantify the average power density at a given location, which varies greatly, depending on the time, specific location, time-averaging interval, frequency, and modulation scheme. For a specific municipality it depends on the antenna density, which network protocols are used, as, for example, 2G, 3G, 4G, 5G, Wi-Fi, WiMAX (Worldwide Interoperability for Microwave Access), DECT (Digitally Enhanced Cordless Telecommunications), and RADAR (Radio Detection and Ranging). There is also WCR from ubiquitous radio wave transmitters, including antennas, base stations, smart meters, mobile phones, routers, satellites, and other wireless devices currently in use. All of these signals superimpose to yield the total average power density at a given location that typically fluctuates greatly over time. No experimental studies on adverse health effects or safety issues of 5G have been reported, and none are currently planned by the industry, although this is sorely needed.
Finally, there is an inherent complexity to WCR that makes it very difficult to fully characterize wireless signals in the real world that may be associated with adverse bioeffects. Real world digital communication signals, even from single wireless devices, have highly variable signals: variable power density, frequency, modulation, phase, and other parameters changing constantly and unpredictably each moment, as associated with the short, rapid pulsations used in digital wireless communication [137]. For example, in using a mobile phone during a typical phone conversation, the intensity of emitted radiation varies significantly each moment depending on signal reception, number of subscribers sharing the frequency band, location within the wireless infrastructure, presence of objects and metallic surfaces, and “speaking” versus “non-speaking” mode, among others. Such variations may reach 100% of the average signal intensity. The carrier radiofrequency constantly changes between different values within the available frequency band. The greater the amount of information (text, speech, internet, video, etc.), the more complex the communication signals become. Therefore, we cannot estimate accurately the values of these signal parameters including ELF components or predict their variability over time. Thus, studies on the bioeffects of WCR in the laboratory can only be representative of real-world exposures [137].
This paper points to the need for further research on nonthermal WCR exposure and its potential role in COVID-19. Moreover, some of the WCR exposure bioeffects that we discuss here — oxidative stress, inflammation, and immune system disruption — are common to many chronic diseases, including autoimmune disease and diabetes. Thus, we hypothesize that WCR exposure may also be a potential contributing factor in many chronic diseases.
When a course of action raises threats of harm to human health, precautionary measures should be taken, even if clear causal relationships are not yet fully established. Therefore, we must apply the Precautionary Principle [138] regarding wireless 5G. The authors urge policymakers to execute an immediate worldwide moratorium on wireless 5G infrastructure until its safety can be assured.
Several unresolved safety issues should be addressed before wireless 5G is further implemented. Questions have been raised about 60 GHz, a key 5G frequency planned for extensive use, which is a resonant frequency of the oxygen molecule [139]. It is possible that adverse bioeffects might ensue from oxygen absorption of 60 GHz. In addition, water shows broad absorption in the GHz spectral region along with resonance peaks, for example, strong absorption at 2.45 GHz that is used in 4G Wi-Fi routers. This raises safety issues about GHz exposure of the biosphere, since organisms are comprised of mostly water, and changes in the structure of water due to GHz absorption have been reported that affect organisms [140]. Bioeffects from prolonged WCR exposure of the whole body need to be investigated in animal and human studies, and long-term exposure guidelines need to be considered. Independent scientists in particular should conduct concerted research to determine the biological effects of real-world exposure to WCR frequencies with digital modulation from the multiplicity of wireless communication devices. Testing could also include real-life exposures to multiple toxins (chemical and biological) [141], because multiple toxins may lead to synergistic effects. Environmental impact assessments are also needed. Once the long-term biological effects of wireless 5G are understood, we can set clear safety standards of public exposure limits and design an appropriate strategy for safe deployment.
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5. Conclusion​

There is a substantial overlap in pathobiology between COVID-19 and WCR exposure. The evidence presented here indicates that mechanisms involved in the clinical progression of COVID-19 could also be generated, according to experimental data, by WCR exposure. Therefore, we propose a link between adverse bioeffects of WCR exposure from wireless devices and COVID-19.
Specifically, evidence presented here supports a premise that WCR and, in particular, 5G, which involves densification of 4G, may have exacerbated the COVID-19 pandemic by weakening host immunity and increasing SARS-CoV-2 virulence by (1) causing morphologic changes in erythrocytes including echinocyte and rouleaux formation that may be contributing to hypercoagulation; (2) impairing microcirculation and reducing erythrocyte and hemoglobin levels exacerbating hypoxia; (3) amplifying immune dysfunction, including immunosuppression, autoimmunity, and hyperinflammation; (4) increasing cellular oxidative stress and the production of free radicals exacerbating vascular injury and organ damage; (5) increasing intracellular Ca2+ essential for viral entry, replication, and release, in addition to promoting pro-inflammatory pathways; and (6) worsening heart arrhythmias and cardiac disorders.
WCR exposure is a widespread, yet often neglected, environmental stressor that can produce a wide range of adverse bioeffects. For decades, independent research scientists worldwide have emphasized the health risks and cumulative damage caused by WCR [42,45]. The evidence presented here is consistent with a large body of established research. Healthcare workers and policymakers should consider WCR a potentially toxic environmental stressor. Methods for reducing WCR exposure should be provided to all patients and the general population.


 

blob69

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The greater the amount of information (text, speech, internet, video, etc.), the more complex the communication signals become.
It has been shown by some scientists studying RF radiation that the information being transmitted is the main factor as far as the amount of damage the radiation causes. This means that one can be exposed to a strong signal (carrier wave) but if no-one is sending data through it, it will not cause (much) damage. It's because the modulation signal - lower frequency - is the harmful one. It's evidently how telecom companies have managed to avoid prosecution: by designing studies so that the carrier wave was not modulated, which resulted in radiation not causing damage.

One of the most obvious things that happened during the COVID era was the increase in streaming and other information transfer due to working from home, virtual events, families being connected only digitally etc. This increased the amount of information being transmitted via RF exponentially. I think this, and not 5G per se, might be one of the main reasons for increased sickness. But perhaps the simultaneous reduction in plane and automobile exhausts offered some benefits to balance things a bit.
 

Kris

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It has been shown by some scientists studying RF radiation that the information being transmitted is the main factor as far as the amount of damage the radiation causes. This means that one can be exposed to a strong signal (carrier wave) but if no-one is sending data through it, it will not cause (much) damage. It's because the modulation signal - lower frequency - is the harmful one. It's evidently how telecom companies have managed to avoid prosecution: by designing studies so that the carrier wave was not modulated, which resulted in radiation not causing damage.

One of the most obvious things that happened during the COVID era was the increase in streaming and other information transfer due to working from home, virtual events, families being connected only digitally etc. This increased the amount of information being transmitted via RF exponentially. I think this, and not 5G per se, might be one of the main reasons for increased sickness. But perhaps the simultaneous reduction in plane and automobile exhausts offered some benefits to balance things a bit.

well, people lived in their laptops and wifi for a long time. it must be the 5G. all the events of 'pandemics' in this century are linked to some electric/magnetic waves being introduced. and now we have the 5G. i guess most people electric system in their bodies cannot adapt to it.
 

Lollipop2

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It's evidently how telecom companies have managed to avoid prosecution: by designing studies so that the carrier wave was not modulated, which resulted in radiation not causing damage.
Criminal.
 

JamesGatz

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I definitely believe it - 5G has really effected me when near it - really dangerous stuff I need to get rich asap and buy a cabin in the middle of the woods
 

Ben.

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I definitely believe it - 5G has really effected me when near it - really dangerous stuff I need to get rich asap and buy a cabin in the middle of the woods

Make sure you still measure if the middle of the wood isn't assaulted by emf aswell. I've read from someone living away from citys still having had alot alof of exposure until a "professional" found a celltower and certain devices in his house despite the efforts put in by the woodcabin guy.

Gates and Musk blanking the sky/space with satelites for 5g isn't realy reassuring either.

Edit: There is EMF protecting clothing but one t-shirt costs 100+ euros/dollars ...prolly synthetic material too...
 

Kris

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Yes, Musk is a criminal. He has so much money, he thinks he can do whatever he wants.

Considering that the 'pandemic' happened close to the release of 5G, I would think that this is the main contributing factor. We are electric beings, our body can respond violently to the change of electromagnetic radiation. I believe that we can adapt as we adapted to the globalisation of the electric grid (in meantime we had of course the Spanish Flu), but this is not in contradiction that these things are bad for us. I would not wear a special suit and stuff, because we cannot escape this reality, but turning off wifi when not needed and not sleeping near electric sockets (my friend actually measured the radiation of these sockets; you basically need to sleep a couple of matters away from them), is something that should be become a habit. by the way, i have another friend who is very sensitive to mobiles - he gets severe headaches by talking through the phone, even when using loud speaker. He is a living radiation detector.

I personally do not believe in viruses, but it is possible that body releases different DNA or RNA particles via exosomes to fight infection, and create communication between cells. If this is true, so 'viruses' are actually positive things. Can they be infectious? It is theoretically possible that by contacting an individual who is sick, that DNA or RNA information can trigger similar response in other people because they have a predisposition for that kind of infection or they have a dormant kind of infection. I am now just speculating.
 
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yerrag

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Abstract​

Background and Aim:​

Coronavirus disease (COVID-19) public health policy has focused on the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) virus and its effects on human health while environmental factors have been largely ignored. In considering the epidemiological triad (agent-host-environment) applicable to all disease, we investigated a possible environmental factor in the COVID-19 pandemic: ambient radiofrequency radiation from wireless communication systems including microwaves and millimeter waves. SARS-CoV-2, the virus that caused the COVID-19 pandemic, surfaced in Wuhan, China shortly after the implementation of city-wide (fifth generation [5G] of wireless communications radiation [WCR]), and rapidly spread globally, initially demonstrating a statistical correlation to international communities with recently established 5G networks. In this study, we examined the peer-reviewed scientific literature on the detrimental bioeffects of WCR and identified several mechanisms by which WCR may have contributed to the COVID-19 pandemic as a toxic environmental cofactor. By crossing boundaries between the disciplines of biophysics and pathophysiology, we present evidence that WCR may: (1) cause morphologic changes in erythrocytes including echinocyte and rouleaux formation that can contribute to hypercoagulation; (2) impair microcirculation and reduce erythrocyte and hemoglobin levels exacerbating hypoxia; (3) amplify immune system dysfunction, including immunosuppression, autoimmunity, and hyperinflammation; (4) increase cellular oxidative stress and the production of free radicals resulting in vascular injury and organ damage; (5) increase intracellular Ca2+ essential for viral entry, replication, and release, in addition to promoting pro-inflammatory pathways; and (6) worsen heart arrhythmias and cardiac disorders.

3. Results​

Table 1 lists the manifestations common to COVID-19 including disease progression and the corresponding adverse bioeffects from WCR exposure. Although these effects are delineated into categories — blood changes, oxidative stress, immune system disruption and activation, increased intracellular calcium (Ca2+), and cardiac effects — it must be emphasized that these effects are not independent of each other. For example, blood clotting and inflammation have overlapping mechanisms, and oxidative stress is implicated in erythrocyte morphological changes as well as in hypercoagulation, inflammation, and organ damage.

Table 1​

Bioeffects of Wireless Communication Radiation (WCR) exposure in relation to COVID-19 manifestations and their progression
Wireless communications radiation (WCR) exposure bioeffects​
COVID-19 manifestations​
Blood changes
 Short-term: rouleaux, echinocytes
 Long-term: reduced blood clotting time, reduced hemoglobin, hemodynamic disorders​
Blood changes
 Rouleaux, echinocytes
 Hemoglobin effects; vascular effects
 →Reduced hemoglobin in severe disease; autoimmune hemolytic anemia; hypoxemia and hypoxia
 →Endothelial injury; impaired microcirculation; hypercoagulation; disseminated intravascular coagulopathy (DIC); pulmonary embolism; stroke​
Oxidative stress
 Glutathione level decrease; free radicals and lipid peroxide increase; superoxide dismutase activity decrease; oxidative injury in tissues and organs​
Oxidative stress
 Glutathione level decrease; free radical increase and damage; apoptosis→Oxidative injury; organ damage in severe disease​
Immune system disruption and activation
 Immune suppression in some studies; immune hyperactivation in other studies
 Long-term: suppression of T-lymphocytes; inflammatory biomarkers increased; autoimmunity; organ injury​
Immune system disruption and activation
 Decreased production of T-lymphocytes; elevated inflammatory biomarkers.
 →Immune hyperactivation and inflammation; cytokine storm in severe disease; cytokine-induced hypo-perfusion with resulting hypoxia; organ injury; organ failure​
Increased intracellular calcium
 From activation of voltage-gated calcium channels on cell membranes, with numerous secondary effects​
Increased intracellular calcium
 →Increased virus entry, replication, and release
 →Increased NF-κB, pro-inflammatory processes, coagulation, and thrombosis​
Cardiac effects
 Up-regulation of sympathetic nervous system; palpitations and arrhythmias​
Cardiac effects
 Arrhythmias
 →Myocarditis; myocardial ischemia; cardiac injury; cardiac failure​
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Supportive evidence including study details and citations are provided in the text under each subject heading, i.e., blood changes, oxidative stress, etc.

3.1. Blood changes​

WCR exposure can cause morphologic changes in blood readily seen through phase contrast or dark-field microscopy of live peripheral blood samples. In 2013, Havas observed erythrocyte aggregation including rouleaux (rolls of stacked red blood cells) in live peripheral blood samples following 10 min human exposure to a 2.4 GHz cordless phone [50]. Although not peer reviewed, one of us (Rubik) investigated the effect of 4G LTE mobile phone radiation on the peripheral blood of ten human subjects, each of whom had been exposed to cell phone radiation for two consecutive 45-min intervals [51]. Two types of effects were observed: increased stickiness and clumping of red blood cells with rouleaux formation, and subsequent formation of echinocytes (spiky red blood cells). Red blood cell clumping and aggregation are known to be actively involved in blood clotting [52]. The prevalence of this phenomenon on exposure to WCR in the human population has not yet been determined. Larger controlled studies should be performed to further investigate this phenomenon.
Similar red blood cell changes have been described in peripheral blood of COVID-19 patients [53]. Rouleaux formation has been observed in 1/3 of COVID-19 patients, whereas spherocytes and echinocyte formation is more variable. Spike protein engagement with ACE2 receptors on cells lining the blood vessels can lead to endothelial damage, even when isolated [54]. Rouleaux formation, particularly in the setting of underlying endothelial damage, can clog the microcirculation, impeding oxygen transport, contributing to hypoxia, and increasing the risk of thrombosis [52]. Thrombogenesis associated with SARS-CoV-2 infection may also be caused by direct viral binding to ACE2 receptors on platelets [55].
Additional blood effects have been observed in both humans and animals exposed to WCR. In 1977, a Russian study reported that rodents irradiated with 5 – 8 mm waves (60 – 37 GHz) at 1 mW/cm2 for 15 min/day over 60 days developed hemodynamic disorders, suppressed red blood cell formation, reduced hemoglobin, and an inhibition of oxygen utilization (oxidative phosphorylation by the mitochondria) [56]. In 1978, a 3-year Russian study on 72 engineers exposed to millimeter wave generators emitting at 1 mW/cm2 or less showed a decrease in their hemoglobin levels and red blood cell counts, and a tendency toward hypercoagulation, whereas a control group showed no changes [57]. Such deleterious hematologic effects from WCR exposure may also contribute to the development of hypoxia and blood clotting observed in COVID-19 patients.
It has been proposed that the SARS-CoV-2 virus attacks erythrocytes and causes degradation of hemoglobin [11]. Viral proteins may attack the 1-beta chain of hemoglobin and capture the porphyrin, along with other proteins from the virus catalyzing the dissociation of iron from heme [58]. In principle this would reduce the number of functional erythrocytes and cause the release of free iron ions that could cause oxidative stress, tissue damage, and hypoxia. With hemoglobin partially destroyed and lung tissue damaged by inflammation, patients would be less able to exchange carbon dioxide (CO2) and oxygen (O2), and would become oxygen depleted. In fact, some COVID-19 patients show reduced hemoglobin levels, measuring 7.1 g/L and even as low as 5.9 g/L in severe cases [59]. Clinical studies of almost 100 patients from Wuhan revealed that the hemoglobin levels in the blood of most patients infected with SARS-CoV-2 are significantly lowered resulting in compromised delivery of oxygen to tissues and organs [60]. In a meta-analysis of four studies with a total of 1210 patients and 224 with severe disease, hemoglobin values were reduced in COVID-19 patients with severe disease compared to those with milder forms [59]. In another study on 601 COVID-19 patients, 14.7% of anemic COVID-19 ICU patients and 9% of non-ICU COVID-19 patients had autoimmune hemolytic anemia [61]. In patients with severe COVID-19 disease, decreased hemoglobin along with elevated erythrocyte sedimentation rate (ESR), C-reactive protein, lactate dehydrogenase, albumin [62], serum ferritin [63], and low oxygen saturation [64] provide additional support for this hypothesis. In addition, packed red blood cell transfusion may promote recovery of COVID-19 patients with acute respiratory failure [65].
In short, both WCR exposure and COVID-19 may cause deleterious effects on red blood cells and reduced hemoglobin levels contributing to hypoxia in COVID-19. Endothelial injury may further contribute to hypoxia and many of the vascular complications seen in COVID-19 [66] that are discussed in the next section.

3.2. Oxidative stress​

Oxidative stress is a non-specific pathological condition reflecting an imbalance between an increased production of ROS and an inability of the organism to detoxify the ROS or to repair the damage they cause to biomolecules and tissues [67]. Oxidative stress can disrupt cell signaling, cause the formation of stress proteins, and generate highly reactive free radicals, which can cause DNA and cell membrane damage.
SARS-CoV-2 inhibits intrinsic pathways designed to reduce ROS levels, thereby increasing morbidity. Immune dysregulation, that is, the upregulation of interleukin (IL)-6 and tumor necrosis factor α (TNF-α) [68] and suppression of interferon (IFN) α and IFN β [69] have been identified in the cytokine storm accompanying severe COVID-19 infections and generates oxidative stress [10]. Oxidative stress and mitochondrial dysfunction may further perpetuate the cytokine storm, worsening tissue damage, and increasing the risk of severe illness and death.
Similarly low-level WCR generates ROS in cells that cause oxidative damage. In fact, oxidative stress is considered to be one of the primary mechanisms in which WCR exposure causes cellular damage. Among 100 currently available peer-reviewed studies investigating oxidative effects of low-intensity WCR, 93 of these studies confirmed that WCR induces oxidative effects in biological systems [17]. WCR is an oxidative agent with a high pathogenic potential especially when exposure is continuous [70].
Oxidative stress is also an accepted mechanism causing endothelial damage [71]. This may manifest in patients with severe COVID-19 in addition to increasing the risk for blood clot formation and worsening hypoxemia [10]. Low levels of glutathione, the master antioxidant, have been observed in a small group of COVID-19 patients, with the lowest level found in the most severe cases [72]. The finding of low glutathione levels in these patients further supports oxidative stress as a component of this disease [72]. In fact, glutathione, the major source of sulfhydryl-based antioxidant activity in the human body, may be pivotal in COVID-19 [73]. Glutathione deficiency has been proposed as the most likely cause of serious manifestations in COVID-19 [72]. The most common co-morbidities, hypertension [74]; obesity [75]; diabetes [76]; and chronic obstructive pulmonary disease [74] support the concept that pre-existing conditions causing low levels of glutathione may work synergistically to create the “perfect storm” for both the respiratory and vascular complications of severe infection. Another paper citing two cases of COVID-19 pneumonia treated successfully with intravenous glutathione also supports this hypothesis [77].
Many studies report oxidative stress in humans exposed to WCR. Peraica et al. [78] found diminished blood levels of glutathione in workers exposed to WCR from radar equipment (0.01 mW/cm2 – 10 mW/cm2; 1.5 – 10.9 GHz). Garaj-Vrhovac et al. [79] studied bioeffects following exposure to non-thermal pulsed microwaves from marine radar (3 GHz, 5.5 GHz, and 9.4 GHz) and reported reduced glutathione levels and increased malondialdehyde (marker for oxidative stress) in an occupationally exposed group [79]. Blood plasma of individuals residing near mobile phone base stations showed significantly reduced glutathione, catalase, and superoxide dismutase levels over unexposed controls [80]. In a study on human exposure to WCR from mobile phones, increased blood levels of lipid peroxide were reported, while enzymatic activities of superoxide dismutase and glutathione peroxidase in the red blood cells decreased, indicating oxidative stress [81].
In a study on rats exposed to 2450 MHz (wireless router frequency), oxidative stress was implicated in causing red blood cell lysis (hemolysis) [82]. In another study, rats exposed to 945 MHz (base station frequency) at 0.367 mW/cm2 for 7 h/day, over 8 days, demonstrated low glutathione levels and increased malondialdehyde and superoxide dismutase enzyme activity, hallmarks for oxidative stress [83]. In a long-term controlled study on rats exposed to 900 MHz (mobile phone frequency) at 0.0782 mW/cm2 for 2 h/day for 10 months, there was a significant increase in malondialdehyde and total oxidant status over controls [84]. In another long-term controlled study on rats exposed to two mobile phone frequencies, 1800 MHz and 2100 MHz, at power densities 0.04 – 0.127 mW/cm2 for 2 h/day over 7 months, significant alterations in oxidant-antioxidant parameters, DNA strand breaks, and oxidative DNA damage were found [85].
There is a correlation between oxidative stress and thrombogenesis [86]. ROS can cause endothelial dysfunction and cellular damage. The endothelial lining of the vascular system contains ACE2 receptors that are targeted by SARS-CoV-2. The resulting endotheliitis can cause luminal narrowing and result in diminished blood flow to downstream structures. Thrombi in arterial structures can further obstruct blood flow causing ischemia and/or infarcts in involved organs, including pulmonary emboli and strokes. Abnormal blood coagulation leading to micro-emboli was a recognized complication early in the history of COVID-19 [87]. Out of 184 ICU COVID-19 patients, 31% showed thrombotic complications [88]. Cardiovascular clotting events are a common cause of COVID-19 deaths [12]. Pulmonary embolism, disseminated intravascular coagulation (DIC), liver, cardiac, and renal failure have all been observed in COVID-19 patients [89].
Patients with the highest cardiovascular risk factors in COVID-19 includ males, the elderly, diabetics, and obese and hypertensive patients. However, increased incidence of strokes in younger patients with COVID-19 has also been described [90].
Oxidative stress is caused by WCR exposure and is known to be implicated in cardiovascular disease. Ubiquitous environmental exposure to WCR may contribute to cardiovascular disease by creating a chronic state of oxidative stress [91]. This would lead to oxidative damage to cellular constituents and alter signal transduction pathways. In addition, pulse-modulated WCR can cause oxidative injury in liver, lung, testis, and heart tissues mediated by lipid peroxidation, increased levels of nitric oxides, and suppression of the antioxidant defense mechanism [92].
In summary, oxidative stress is a major component in the pathophysiology of COVID-19 as well as in cellular damage caused by WCR exposure.

3.3. Immune system disruption and activation​

When SARS-CoV-2 first infects the human body, it attacks cells lining the nose, throat, and upper airway harboring ACE2 receptors. Once the virus gains access to a host cell through one of its spike proteins, which are the multiple protuberances projecting from the viral envelope that bind to ACE2 receptors, it converts the cell into a virus self-replicating entity.
In response to COVID-19 infection, both an immediate systemic innate immune response as well as a delayed adaptive response has been shown to occur [93]. The virus can also cause a dysregulation of the immune response, particularly in the decreased production of T-lymphocytes. [94]. Severe cases tend to have lower lymphocyte counts, higher leukocyte counts and neutrophil-lymphocyte ratios, as well as lower percentages of monocytes, eosinophils, and basophils [94]. Severe cases of COVID-19 show the greatest impairment in T-lymphocytes.
In comparison, low-level WCR studies on laboratory animals also show impaired immune function [95]. Findings include physical alterations in immune cells, a degradation of immunological responses, inflammation, and tissue damage. Baranski [96] exposed guinea pigs and rabbits to continuous or pulse-modulated 3000 MHz microwaves at an average power density of 3.5 mW/cm2 for 3 h/day over 3 months and found nonthermal changes in lymphocyte counts, abnormalities in nuclear structure, and mitosis in the erythroblastic cell series in the bone marrow and in lymphoid cells in lymph nodes and spleen. Other investigators have shown diminished T-lymphocytes or suppressed immune function in animals exposed to WCR. Rabbits exposed to 2.1 GHz at 5mW/cm2 for 3 h/day, 6 days/week, for 3 months, showed suppression of T-lymphocytes [97]. Rats exposed to 2.45 GHz and 9.7 GHz for 2 h/day, 7 days/week, for 21 months showed a significant decrease in the levels of lymphocytes and an increase in mortality at 25 months in the irradiated group [98]. Lymphocytes harvested from rabbits irradiated with 2.45 GHz for 23 h/day for 6 months show a significant suppression in immune response to a mitogen [99].
In 2009, Johansson conducted a literature review, which included the 2007 Bioinitiative Report. He concluded that electromagnetic fields (EMF) exposure, including WCR, can disturb the immune system and cause allergic and inflammatory responses at exposure levels significantly less than current national and international safety limits and raise the risk for systemic disease [100]. A review conducted by Szmigielski in 2013 concluded that weak RF/microwave fields, such as those emitted by mobile phones, can affect various immune functions both in vitro and in vivo [101]. Although the effects are historically somewhat inconsistent, most research studies document alterations in the number and activity of immune cells from RF exposure. In general, short-term exposure to weak microwave radiation may temporarily stimulate an innate or adaptive immune response, but prolonged irradiation inhibits those same functions.
In the acute phase of COVID-19 infection, blood tests demonstrate elevated ESR, C-reactive protein, and other elevated inflammatory markers [102], typical of an innate immune response. Rapid viral replication can cause death of epithelial and endothelial cells and result in leaky blood vessels and pro-inflammatory cytokine release [103]. Cytokines, proteins, peptides, and proteoglycans that modulate the body’s immune response, are modestly elevated in patients with mild-to-moderate disease severity [104]. In those with severe disease, an uncontrolled release of pro-inflammatory cytokines--a cytokine storm--can occur. Cytokine storms originate from an imbalance in T-cell activation with dysregulated release of IL-6, IL-17, and other cytokines. Programmed cell death (apoptosis), ARDS, DIC, and multi-organ system failure can all result from a cytokine storm and increase the risk of mortality.
By comparison, Soviet researchers found in the 1970s that radiofrequency radiation can damage the immune system of animals. Shandala [105] exposed rats to 0.5 mW/cm2 microwaves for 1 month, 7 h/day, and found impaired immune competence and induction of autoimmune disease. Rats irradiated with 2.45 GHz at 0.5 mW/cm2 for 7 h daily for 30 days produced autoimmune reactions, and 0.1 – 0.5 mW/cm2 produced persistent pathological immune reactions [106]. Exposure to microwave radiation, even at low levels (0.1 – 0.5 mW/cm2), can impair immune function, causing physical alterations in the essential cells of the immune system and a degradation of immunologic responses [107]. Szabo et al. [108] examined the effects of 61.2 GHz exposure on epidermal keratinocytes and found an increase in IL-1b, a pro-inflammatory cytokine. Makar et al. [109] found that immunosuppressed mice irradiated 30 min/day for 3 days by 42.2 GHz showed increased levels of TNF-α, a cytokine produced by macrophages.
In short, COVID-19 can lead to immune dysregulation as well as cytokine storms. By comparison, exposure to low-level WCR as observed in animal studies can also compromise the immune system, with chronic daily exposure producing immunosuppression or immune dysregulation including hyperactivation.

3.4. Increased intracellular calcium​

In 1992, Walleczek first suggested that ELF electromagnetic fields (<3000 Hz) may be affecting membrane-mediated Ca2+ signaling and lead to increased intracellular Ca2+ [110]. The mechanism of irregular gating of voltage-gated ion channels in cell membranes by polarized and coherent, oscillating electric or magnetic fields was first presented in 2000 and 2002 [40,111]. Pall [112] in his review of WCR-induced bioeffects combined with use of calcium channel blockers (CCB) noted that voltage-gated calcium channels play a major role in WCR bioeffects. Increased intracellular Ca+2 results from the activation of voltage-gated calcium channels, and this may be one of the primary mechanisms of action of WCR on organisms.
Intracellular Ca2+ is essential for virus entry, replication, and release. It has been reported that some viruses can manipulate voltage-gated calcium channels to increase intracellular Ca2+ thereby facilitating viral entry and replication [113]. Research has shown that the interaction between a virus and voltage-gated calcium channels promote virus entry at the virus-host cell fusion step [113]. Thus, after the virus binds to its receptor on a host cell and enters the cell through endocytosis, the virus takes over the host cell to manufacture its components. Certain viral proteins then manipulate calcium channels, thereby increasing intracellular Ca2+, which facilitates further viral replication.
Even though direct evidence has not been reported, there is indirect evidence that increased intracellular Ca2+ may be involved in COVID-19. In a recent study, elderly hospitalized COVID-19 patients treated with CCBs, amlodipine or nifedipine, were more likely to survive and less likely to require intubation or mechanical ventilation than controls [114]. Furthermore, CCBs strongly limit SARS-CoV-2 entry and infection in cultured epithelial lung cells [115]. CCBs also block the increase of intracellular Ca2+ caused by WCR exposure as well as exposure to other electromagnetic fields [112].
Intracellular Ca2+ is a ubiquitous second messenger relaying signals received by cell surface receptors to effector proteins involved in numerous biochemical processes. Increased intracellular Ca2+ is a significant factor in upregulation of transcription nuclear factor KB (NF-κB) [116], an important regulator of pro-inflammatory cytokine production as well as coagulation and thrombotic cascades. NF-κB is hypothesized to be a key factor underlying severe clinical manifestations of COVID-19 [117].
In short, WCR exposure, therefore, may enhance the infectivity of the virus by increasing intracellular Ca2+ that may also indirectly contribute to inflammatory processes and thrombosis.

3.5. Cardiac effects​

Cardiac arrhythmias are more commonly encountered in critically ill patients with COVID-19 [118]. The cause for arrhythmia in COVID-19 patients is multifactorial and includes cardiac and extra-cardiac processes [119]. Direct infection of the heart muscle by SARS-CoV-19 causing myocarditis, myocardial ischemia caused by a variety of etiologies, and heart strain secondary to pulmonary or systemic hypertension can result in cardiac arrhythmia. Hypoxemia caused by diffuse pneumonia, ARDS, or extensive pulmonary emboli represent extra-cardiac causes of arrhythmia. Electrolyte imbalances, intravascular fluid imbalance, and side effects from pharmacologic regimens can also result in arrhythmias in COVID-19 patients. Patients admitted to ICUs have been shown to have a higher increase in cardiac arrhythmias, 16.5% in one study [120]. Although no correlation between EMFs and arrhythmia in COVID-19 patients has been described in the literature, many ICUs are equipped with wireless patient monitoring equipment and communication devices producing a wide range of EMF pollution [121].
COVID-19 patients commonly show increased levels of cardiac troponin, indicating damage to the heart muscle [122]. Cardiac damage has been associated with arrhythmias and increased mortality. Cardiac injury is thought to be more often secondary to pulmonary emboli and viral sepsis, but direct infection of the heart, that is, myocarditis, can occur through direct viral binding to ACE2 receptors on cardiac pericytes, affecting local, and regional cardiac blood flow [60].
Immune system activation along with alterations in the immune system may result in atherosclerotic plaque instability and vulnerability, that is, presenting an increased risk for thrombus formation, and contributing to development of acute coronary events and cardiovascular disease in COVID-19.
Regarding WCR exposure bioeffects, in 1969 Christopher Dodge of the Biosciences Division, U.S. Naval Observatory in Washington DC, reviewed 54 papers and reported that radiofrequency radiation can adversely affect all major systems of the body, including impeding blood circulation; altering blood pressure and heart rate; affecting electrocardiograph readings; and causing chest pain and heart palpitations [123]. In the 1970s Glaser reviewed more than 2000 publications on radiofrequency radiation exposure bioeffects and concluded that microwave radiation can alter the electrocardiogram, cause chest pain, hypercoagulation, thrombosis, and hypertension in addition to myocardial infarction [27,28]. Seizures, convulsions, and alteration of the autonomic nervous system response (increased sympathetic stress response) have also been observed.
Since then, many other researchers have concluded that WCR exposure can affect the cardiovascular system. Although the nature of the primary response to millimeter waves and consequent events are poorly understood, a possible role for receptor structures and neural pathways in the development of continuous millimeter wave-induced arrhythmia has been proposed [47]. In 1997, a review reported that some investigators discovered cardiovascular changes including arrhythmias in humans from long-term low-level exposure to WCR including microwaves [124]. However, the literature also shows some unconfirmed findings as well as some contradictory findings [125]. Havas et al. [126] reported that human subjects in a controlled, double-blinded study were hyper-reactive when exposed to 2.45 GHz, digitally pulsed (100 Hz) microwave radiation, developing either an arrhythmia or tachycardia and upregulation of the sympathetic nervous system, which is associated with the stress response. Saili et al. [127] found that exposure to Wi-Fi (2.45 GHz pulsed at 10 Hz) affects heart rhythm, blood pressure, and the efficacy of catecholamines on the cardiovascular system, indicating that WCR can act directly and/or indirectly on the cardiovascular system. Most recently, Bandara and Weller [91] present evidence that people who live near radar installations (millimeter waves: 5G frequencies) have a greater risk of developing cancer and experiencing heart attacks. Similarly, those occupationally exposed have a greater risk of coronary heart disease. Microwave radiation affects the heart, and some people are more vulnerable if they have an underlying heart abnormality [128]. More recent research suggests that millimeter waves may act directly on the pacemaker cells of the sinoatrial node of the heart to change the beat frequency, which may underlie arrhythmias and other cardiac issues [47].
In short, both COVID-19 and WCR exposure can affect the heart and cardiovascular system, directly and/or indirectly.
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4. Discussion​

Epidemiologists, including those at the CDC, consider multiple causal factors when evaluating the virulence of an agent and understanding its ability to spread and cause disease. Most importantly, these variables include environmental cofactors and the health status of the host. Evidence from the literature summarized here suggests a possible connection between several adverse health effects of WCR exposure and the clinical course of COVID-19 in that WCR may have worsened the COVID-19 pandemic by weakening the host and exacerbating COVID-19 disease. However, none of the observations discussed here prove this linkage. Specifically, the evidence does not confirm causation. Clearly COVID-19 occurs in regions with little wireless communication. Furthermore, the relative morbidity caused by WCR exposure in COVID-19 is unknown.
We recognize that many factors have influenced the pandemic’s course. Before restrictions were imposed, travel patterns facilitated the seeding of the virus, causing early rapid global spread. Population density, higher mean population age, and socioeconomic factors certainly influenced early viral spread. Air pollution, especially particulate matter PM2.5 (2.5 micro-particulates), likely increased symptoms in patients with COVID-19 lung disease [129].
We postulate that WCR possibly contributed to the early spread and severity of COVID-19. Once an agent becomes established in a community, its virulence increases [130]. This premise can be applied to the COVID-19 pandemic. We surmise that “hot spots” of the disease that initially spread around the world were perhaps seeded by air travel, which in some areas were associated with 5G implementation. However, once the disease became established in those communities, it was able to spread more easily to neighboring regions where populations were less exposed to WCR. Second and third waves of the pandemic disseminated widely throughout communities with and without WCR, as might be expected.
The COVID-19 pandemic has offered us an opportunity to delve further into the potential adverse effects of WCR exposure on human health. Human exposure to ambient WCR significantly increased in 2020 as a “side effect” to the pandemic. Stay-at-home measures designed to reduce the spread of COVID-19 inadvertently resulted in greater public exposure to WCR, as people conducted more business and school related activities through wireless communications. Telemedicine created another source of WCR exposure. Even hospital inpatients, particular ICU patients, experienced increased WCR exposure as new monitoring devices utilized wireless communication systems that may exacerbate health disorders. It would potentially provide valuable information to measure ambient WCR power densities in home and work environments when comparing disease severity in patient populations with similar risk factors.
The question of causation could be investigated in future studies. For example, a clinical study could be conducted in COVID-19 patient populations with similar risk factors, to measure the WCR daily dose in COVID-19 patients and look for a correlation with disease severity and progression over time. As wireless device carrier frequencies and modulations may differ, and the power densities of WCR fluctuate constantly at a given location, this study would require patients to wear personal microwave dosimeters (monitoring badges). In addition, controlled laboratory studies could be conducted on animals, for example, humanized mice infected with SARS-CoV-2, in which groups of animals exposed to minimal WCR (control group) as well as medium and high power densities of WCR could be compared for disease severity and progression.
A major strength of this paper is that the evidence rests on a large body of scientific literature reported by many scientists worldwide and over several decades--experimental evidence of adverse bioeffects of WCR exposure at nonthermal levels on humans, animals, and cells. The Bioinitiative Report [42], updated in 2020, summarizes hundreds of peer-reviewed scientific papers documenting evidence of nonthermal effects from exposures ≤1 mW/cm2. Even so, some laboratory studies on the adverse health effects of WCR have sometimes utilized power densities exceeding 1mW/cm2. In this paper, almost all of the studies that we reviewed included experimental data at power densities ≤1 mW/cm2.
A potential criticism of this paper is that adverse bioeffects from nonthermal exposures are not yet universally accepted in science. Moreover, they are not yet considered in establishing public health policy in many nations. Decades ago, Russians and Eastern Europeans compiled considerable data on nonthermal bioeffects, and subsequently set guidelines at lower radiofrequency radiation exposure limits than the US and Canada, that is, below levels where nonthermal effects are observed. However, the Federal Communications Commission (FCC, a US government entity) and ICNIRP guidelines operate on thermal limits based on outdated data from decades ago, allowing the public to be exposed to considerably higher radiofrequency radiation power densities. Regarding 5G, the telecommunication industry claims that it is safe because it complies with current radiofrequency radiation exposure guidelines of the FCC and ICNIRP. These guidelines were established in 1996 [131], are antiquated, and are not safety standards. Thus, there are no universally accepted safety standards for wireless communication radiation exposure. Recently international bodies, such as the EMF Working Group of the European Academy of Environmental Medicine, have proposed much lower guidelines, taking into account nonthermal bioeffects from WCR exposure in multiple sources [132].
Another weakness of this paper is that some of the bioeffects from WCR exposure are inconsistently reported in the literature. Replicated studies are often not true replications. Small differences in method, including unreported details, such as prior history of exposure of the organisms, non-uniform body exposure, and other variables can lead to inadvertent inconsistency. Moreover, not surprisingly, industry-sponsored studies tend to show less adverse bioeffects than studies conducted by independent researchers, suggesting industry bias [133]. Some experimental studies that are not industry-sponsored have also shown no evidence of harmful effects of WCR exposure. It is noteworthy, however, that studies employing real-life WCR exposures from commercially available devices have shown high consistency in revealing adverse effects [134].
WCR bioeffects depend on specific values of wave parameters including frequency, power density, polarization, exposure duration, modulation characteristics, as well as the cumulative history of exposure and background levels of electromagnetic, electric and magnetic fields. In laboratory studies, bioeffects observed also depend on genetic parameters and physiological parameters such as oxygen concentration [135]. The reproducibility of bioeffects of WCR exposure has sometimes been difficult due to failure to report and/or control all of these parameters. Similar to ionizing radiation, the bioeffects of WCR exposure can be subdivided into deterministic, that is, dose-dependent effects and stochastic effects that are seemingly random. Importantly, WCR bioeffects can also involve “response windows” of specific parameters whereby extremely low-level fields can have disproportionally detrimental effects [136]. This nonlinearity of WCR bioeffects can result in biphasic responses such as immune suppression from one range of parameters, and immune hyperactivation from another range of parameters, leading to variations that may appear inconsistent.
In gathering reports and examining existing data for this paper, we looked for outcomes providing evidence to support a proposed connection between the bioeffects of WCR exposure and COVID-19. We did not make an attempt to weigh the evidence. The radiofrequency radiation exposure literature is extensive and currently contains over 30,000 research reports dating back several decades. Inconsistencies in nomenclature, reporting of details, and cataloging of keywords make it difficult to navigate this enormous literature.
Another shortcoming of this paper is that we do not have access to experimental data on 5G exposures. In fact, little is known about population exposure from real-world WCR, which includes exposure to WCR infrastructure and the plethora of WCR emitting devices. In relation to this, it is difficult to accurately quantify the average power density at a given location, which varies greatly, depending on the time, specific location, time-averaging interval, frequency, and modulation scheme. For a specific municipality it depends on the antenna density, which network protocols are used, as, for example, 2G, 3G, 4G, 5G, Wi-Fi, WiMAX (Worldwide Interoperability for Microwave Access), DECT (Digitally Enhanced Cordless Telecommunications), and RADAR (Radio Detection and Ranging). There is also WCR from ubiquitous radio wave transmitters, including antennas, base stations, smart meters, mobile phones, routers, satellites, and other wireless devices currently in use. All of these signals superimpose to yield the total average power density at a given location that typically fluctuates greatly over time. No experimental studies on adverse health effects or safety issues of 5G have been reported, and none are currently planned by the industry, although this is sorely needed.
Finally, there is an inherent complexity to WCR that makes it very difficult to fully characterize wireless signals in the real world that may be associated with adverse bioeffects. Real world digital communication signals, even from single wireless devices, have highly variable signals: variable power density, frequency, modulation, phase, and other parameters changing constantly and unpredictably each moment, as associated with the short, rapid pulsations used in digital wireless communication [137]. For example, in using a mobile phone during a typical phone conversation, the intensity of emitted radiation varies significantly each moment depending on signal reception, number of subscribers sharing the frequency band, location within the wireless infrastructure, presence of objects and metallic surfaces, and “speaking” versus “non-speaking” mode, among others. Such variations may reach 100% of the average signal intensity. The carrier radiofrequency constantly changes between different values within the available frequency band. The greater the amount of information (text, speech, internet, video, etc.), the more complex the communication signals become. Therefore, we cannot estimate accurately the values of these signal parameters including ELF components or predict their variability over time. Thus, studies on the bioeffects of WCR in the laboratory can only be representative of real-world exposures [137].
This paper points to the need for further research on nonthermal WCR exposure and its potential role in COVID-19. Moreover, some of the WCR exposure bioeffects that we discuss here — oxidative stress, inflammation, and immune system disruption — are common to many chronic diseases, including autoimmune disease and diabetes. Thus, we hypothesize that WCR exposure may also be a potential contributing factor in many chronic diseases.
When a course of action raises threats of harm to human health, precautionary measures should be taken, even if clear causal relationships are not yet fully established. Therefore, we must apply the Precautionary Principle [138] regarding wireless 5G. The authors urge policymakers to execute an immediate worldwide moratorium on wireless 5G infrastructure until its safety can be assured.
Several unresolved safety issues should be addressed before wireless 5G is further implemented. Questions have been raised about 60 GHz, a key 5G frequency planned for extensive use, which is a resonant frequency of the oxygen molecule [139]. It is possible that adverse bioeffects might ensue from oxygen absorption of 60 GHz. In addition, water shows broad absorption in the GHz spectral region along with resonance peaks, for example, strong absorption at 2.45 GHz that is used in 4G Wi-Fi routers. This raises safety issues about GHz exposure of the biosphere, since organisms are comprised of mostly water, and changes in the structure of water due to GHz absorption have been reported that affect organisms [140]. Bioeffects from prolonged WCR exposure of the whole body need to be investigated in animal and human studies, and long-term exposure guidelines need to be considered. Independent scientists in particular should conduct concerted research to determine the biological effects of real-world exposure to WCR frequencies with digital modulation from the multiplicity of wireless communication devices. Testing could also include real-life exposures to multiple toxins (chemical and biological) [141], because multiple toxins may lead to synergistic effects. Environmental impact assessments are also needed. Once the long-term biological effects of wireless 5G are understood, we can set clear safety standards of public exposure limits and design an appropriate strategy for safe deployment.
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5. Conclusion​

There is a substantial overlap in pathobiology between COVID-19 and WCR exposure. The evidence presented here indicates that mechanisms involved in the clinical progression of COVID-19 could also be generated, according to experimental data, by WCR exposure. Therefore, we propose a link between adverse bioeffects of WCR exposure from wireless devices and COVID-19.
Specifically, evidence presented here supports a premise that WCR and, in particular, 5G, which involves densification of 4G, may have exacerbated the COVID-19 pandemic by weakening host immunity and increasing SARS-CoV-2 virulence by (1) causing morphologic changes in erythrocytes including echinocyte and rouleaux formation that may be contributing to hypercoagulation; (2) impairing microcirculation and reducing erythrocyte and hemoglobin levels exacerbating hypoxia; (3) amplifying immune dysfunction, including immunosuppression, autoimmunity, and hyperinflammation; (4) increasing cellular oxidative stress and the production of free radicals exacerbating vascular injury and organ damage; (5) increasing intracellular Ca2+ essential for viral entry, replication, and release, in addition to promoting pro-inflammatory pathways; and (6) worsening heart arrhythmias and cardiac disorders.
WCR exposure is a widespread, yet often neglected, environmental stressor that can produce a wide range of adverse bioeffects. For decades, independent research scientists worldwide have emphasized the health risks and cumulative damage caused by WCR [42,45]. The evidence presented here is consistent with a large body of established research. Healthcare workers and policymakers should consider WCR a potentially toxic environmental stressor. Methods for reducing WCR exposure should be provided to all patients and the general population.



This is a nice table of symptoms.

While it can be said that these are symptoms of COVID-19, it can also be said that these symptoms are not exclusive to COVID-19. While I am in agreement with WCR being very stressful on us as susceptible organisms, in itself it would not be able to cause enough stress to result in a putative pandemic. But it would be a significant stressor to put a sizeable portion of the population to tip over the edge, with the population already pushed to the edge by stressors that have built up over decades of intentional neglect and willful harm by the medical authoritarians of big pharma.

Even without having COVID, people who are extremely unhealthy would be exhibit the same symptoms. And that is why even without COVID, people do get deathly sick and hospital ICUs would always be filled with patients on their last legs who eventually die. If each of these patients is screened to see if the symptoms listed on the table are present, I would not be surprised to see most, if not all of them, exhibiting these symptoms.

So, if we were to disengage from the false reality of COVID-19, we can start to recognize that 5G is only one of many causes that together, create very compromised states in humans, in a subtle fashion that typifies death by a thousand cuts. Because people, as unintentional followers of the cult of medical orthodoxy, fail to recognize this, they are so readily given to believe in a direct relationship between a new threat to our health in 5G (while forgetting about a myriad of existing ones that are just as harmful) and a newly concocted pandemic called COVID-19 from the fictitious virus SARS-COV2.
 

Peater

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I just came to post this, have a bump.

What on earth do we do?
 
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Peater

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Interesting it STILL mentions a contagious "virus" called SARS-CoV-2. I think I read here that what could have happened is cells died and burst, and the "Virus" is actually ribosomes etc.
 

Peater

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I keep pondering this. If there is anything to this theory, is ivermectin therefore a good protection for EMF damage to cells?
 

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Radiation from wireless technology affects the blood, the heart, and the autonomic nervous system
The symptoms of electro-hypersensitivity (EHS), best described as rapid aging syndrome, experienced by adults and children resemble symptoms experienced by radar operators in the 1940s to the 1960s and are well described in the literature. An increasingly common response includes clumping (rouleau formation) of the red blood cells, heart palpitations, pain or pressure in the chest accompanied by anxiety, and an upregulation of the sympathetic nervous system coincident with a downregulation of the parasympathetic nervous system typical of the "fight-or-flight" response.

 

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