haidut

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Some more evidence on the role of PUFA as a big factor in CVD. While the evidence is not widely discussed on mainstream media, and a few saboteur attempt against coconut oil have recently been published, nonetheless a few "runaways" do make it to front page news and we have posted them on the forum before.
Eating PUFA Instead Of Butter Increases Overall Death Rates And CVD
Plant Diet Increases Risk Of Cancer And CVD Due To PUFA
PUFA increase CVD risk while saturated fats decrease it
Western Diet Or SFA Strikingly Protective Against Colon Cancer And Mortality

It now looks like even the hallowed BMJ is wising up to the fact that PUFA is no joke and may be the driving force of CVD. I know this topic has been discussed ad nausea on the forum but this is one of the few studies that places the blame squarely in PUFA's court while stating that MUFA and SFA are protective. It also has a nice bullet list of 29 points greatly summarizing the case for PUFA as perhaps THE main cause of CVD. So, it can be sent as a quick counterpoint summary to people (usually doctors) arguing in favor of PUFA and pushing statins plus complete avoidance of dietary cholesterol.
The study also mentions (under bullet 28) that PUFA is known to promote cell death and organ failure in otherwise healthy people. This could explain the kidney, heart and liver failures in (typically young) people as a result of acute stress, who do not have any signs of chronic disease. It can also explain the therapeutic effects of niacinamide and aspirin in such people.

EDIT: Sychronicity strikes again! About 2 hours after I posted this thread Peat's latest newsletter arrived in my Inbox. It is titled "Cholesterol in Context: Part I" and it has this statement in it:
"...Paul Cullen, et al. (1997, 2005) found that the foam cells found in atherosclerosis plaques contain “. . .cholesterol esters, principally cholesteryl eicosapentaenoate, cholesteryl docosahexaenoate, cholesteryl arachidonate, cholesteryl linoleate and cholesteryl oleate.” The oxidation of these fatty acids produces acrolein and related compounds which block the ability of cells to regulate cholesterol (Shao, et al., 2005)." Now, look at the quote from the study below, focusing on the part in red.


https://openheart.bmj.com/content/openhrt/5/2/e000898.full.pdf

"...However, oxidised cholesterol was also considered a culprit as it was contained in atherosclerotic plaque, which led to the demonisation of dietary cholesterol as a cause of coronary heart disease (CHD). However, cholesterol bound to saturated fat does not readily oxidise; this is not the case with linoleic acid.21 Moreover, lipids from human atherosclerotic plaques have been found to contain oxidised cholesteryl linoleate (cholesterol esters containing linoleic acid).21–24 Moreover, the severity of atherosclerosis is noted to increase with increasing oxidised cholesteryl linoleate.21 25 In other words, cholesterol was protected from oxidation if bound to saturated fat but susceptible to oxidation when bound to linoleic acid. Again, this suggests is that eating more linoleic acid increases the oxidation of cholesterol within LDL particles further increasing atherosclerosis formation and the risk of coronary heart disease."

"...
1. Greater amounts of linoleic acid oxidation products are found in LDL and plasma of patients with atherosclerosis.14

2. Greater amounts of linoleic acid oxidation products are found within atherosclerotic plaques and the degree of oxidation determines the severity of atherosclerosis.22

3. A diet higher in oleic acid or lower in linoleic acid decreases LDL susceptibility to oxidation.14

4. Endothelial cells oxidise LDL forming linoleic acid hydroperoxides.14

5. Linoleic acid is the most abundant fatty acid in LDL and is extremely vulnerable to oxidation being one of the very first fatty acids to oxidise.14

6. A meta-analysis of randomised controlled trials in humans found that when saturated fat plus trans-fat is replaced with omega-6 fat (high in linoleic acid), there is an increase in all-cause mortality, ischaemic heart disease mortality and cardiovascular mortality.41

7. The oxidation of linoleic acid in LDL leads to conjugated dienes (malondialdehyde and 4-hydroxynonenal), which covalently bind to apoB altering its structure creating oxidised LDL. oxLDL is no longer recognised by the LDL receptors on the liver but by scavenger receptors on macrophages causing monocyte infiltration into the subendothelium, foam cell formation and eventual atherosclerosis.14

8. Oxidation products of linoleic acid (including 9-HODE and 13- HODE) are found in infarcted tissue.44

9. Ultrasound of the carotid arteries in healthy patients who have high 9-HODE in LDL have signs of atherosclerosis.14

10. The increase in 9-HODE begins between 40 and 50 years old prior to the clinical manifestation of atherosclerosis.14

11. 9-HODE is a good indicator of oxLDL, especially if other causes of inflammation are excluded. An increased oxidised LDL, and hence levels of 9-HODE and 13-HODE in LDL, found in patients with rheumatoid arthritis may explain why they have an increased risk of heart disease.45

12. 9-HODE and 13-HODE stimulate the release of interleukin 1B from macrophages.45

13. The linoleic acid metabolite 9-HODE is a strong promoter of inflammation45 and hence may be both a marker and inducer of atherosclerosis.

14. Susceptibility of LDL to oxidation correlates independently with the extent of atherosclerosis.46

15. Linoleic acid free fatty acids and hydroxy acids (such as 13- HODE) can induce direct toxic effects to the endothelium causing an increase inflammation, reactive oxygen species and adhesion molecules.33 34

16. Exposure of the endothelium to linoleic acid has been found to increase LDL transfer across the endothelium, an essential step in the atherosclerosis process.35

17. Oxidised linoleic acid metabolites (OXLAMs) are recognised by immune cells and can recruit monocytes/neutrophils to atherosclerotic lesions.47 OXLAMs are considered a danger signal activating innate immune cells, which are involved in atherosclerosis formation.48 49

18. Linoleic acid is the most abundant fat found in atherosclerotic plaques, and this has been known since at least the 1960s.50

19. Oxidised linoleic acid but not oxidised oleic acid is found in atherosclerotic plaques.51

20. Consuming more linoleic acid increases the amount of linoleic acid in complicated aortic plaques.52

21. Linoleic acid in adipose tissue and platelets positively associates with CAD, whereas EPA and DHA in platelets are inversely correlated with CAD.3

22. Linoleic acid serum concentrations (as opposed to per cent of fatty acids) are higher in patients with CAD.4

23. Using the fat-1 transgenic mouse model, which converts omega-6 to omega-3 creating an omega-6:eek:mega-3 ratio of around 1:1 in tissues and organs, reduces atherosclerotic lesions by inhibiting systemic and vascular inflammation.53

24. Mice fed fish oil (high in omega-3) as compared with corn oil (high in omega-6) have a significant reduction in atherosclerotic plaque formation possibly due to an increase in antioxidant enzyme activity.54

25. There is more thin fibrous cap atheroma, less thick fibrous cap atheroma, less stable plaque and a greater percentage of plaque rupture in patients given sunflower oil (high in omega-6) versus control.55

26. An excess dietary intake of linoleic acid causes greater endothelial activation compared with an excess of saturated fat.56 Linoleic acid can activate vascular endothelial cells, a critical step for inducing atherosclerosis.57 58

27. Linoleic acid is inflammatory to the vascular endothelium.59

28. Linoleic acid metabolites promote cardiac arrhythmias, cell death, organ failure and cardiac arrest.60

29. Patients who have died from sudden cardiac death have more linoleic acid and less omega-3 polyunsaturated fats in their coronary arteries versus control patients who died mostly from traffic accidents.61 Box 2 summarises the opposing views for (1) why linoleic acid may reduce CHD and (2) why linoleic acid may increase the risk of CHD.

..."
 
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Well, plant oils are largely trash that should’ve never been pushed forward, a number of animal fats are by and large the main sources of arachidonic acid, plant based diets that consist of real foods are not French fries and vegan burgers and people live longer on them and doctors reverse disease on such diets, high saturated fat consumption isnt going to be any better than low saturated fat consumption.

I find it amazing how the pendulum consistently seems to swing between XYZ specific source of fat, at the expense of another one. We know people love to mix carbs and fats and that leads to disease.

All fats should be kept nice and low. Low fats low problems.
 
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Well, plant oils are largely trash that should’ve never been pushed forward, a number of animal fats are by and large the main sources of arachidonic acid, plant based diets that consist of real foods are not French fries and vegan burgers and people live longer on them and doctors reverse disease on such diets, high saturated fat consumption isnt going to be any better than low saturated fat consumption.

I find it amazing how the pendulum consistently seems to swing between XYZ specific source of fat, at the expense of another one. We know people love to mix carbs and fats and that leads to disease.

All fats should be kept nice and low. Low fats low problems.

Dr. Peat suggests mixing carbs and fat.
 

hmac

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Nice find, thanks.

It was done by the guy who wrote "The Salt Fix"!
 
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PUFA major cause of indigestion and heartburn. No doubt acid reflux too. I no longer have any problems with acid, since switching to lard and dripping for cooking. Told a friend who also has problems and now he don't! I thought I was lactose intolerant, but now can drink milk without any issues. Even drinking milk with tea and coffee now.
We never bought into margarine and all the BS butter substitutes, so have always had best butter.
I think you are hitting a nail on the head with precision here.
 

Mito

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Supplementation with linoleic acid-rich soybean oil stimulates macrophage foam cell formation via increased oxidative stress and diacylglycerol acyltransferase1-mediated triglyceride biosynthesis​

Abstract​

During the last decades there has been a staggering rise in human consumption of soybean oil (SO) and its major polyunsaturated fatty acid linoleic acid (LA). The role of SO or LA in cardiovascular diseases is highly controversial, and their impact on macrophage foam cell formation, the hallmark of early atherogenesis, is unclear. To investigate the effects of high SO or LA intake on macrophage lipid metabolism and the related mechanisms of action, C57BL/6 mice were orally supplemented with increasing levels of SO-based emulsion or equivalent levels of purified LA for 1 month, followed by analyses of lipid accumulation and peroxidation in aortas, serum and in peritoneal macrophages (MPM) of the mice. Lipid peroxidation and triglyceride mass in aortas from SO or LA supplemented mice were dose-dependently and significantly increased. In MPM from SO or LA supplemented mice, lipid peroxides were significantly increased and a marked accumulation of cellular triglycerides was found in accordance with enhanced triglyceride biosynthesis rate and overexpression of diacylglycerol acyltransferase1 (DGAT1), the key enzyme in triglyceride biosynthesis. In cultured J774A.1 macrophages treated with SO or LA, triglyceride accumulated via increased oxidative stress and a p38 mitogen-activated protein kinase (MAPK)-mediated overexpression of DGAT1. Accordingly, anti-oxidants (pomegranate polyphenols), inhibition of p38 MAPK (by SB202190) or DGAT1 (by oleanolic acid), all significantly attenuated SO or LA-induced macrophage triglyceride accumulation. These findings reveal novel mechanisms by which supplementation with SO or LA stimulate macrophage foam cell formation, suggesting a pro-atherogenic role for overconsumption of SO or LA. © 2016 BioFactors, 43(1):100–116, 2017

 

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