Research published this week from the Technical University of Munich explores how the degredation of myelin leaves a destructive cholesterol residue in the brain, which increases an inflammatory response and blocks myelin regeneration. It appears that with age, the process of transporting cholesterol out of the brain becomes less efficient. (Important to state that this research was done on a mouse model of MS.)
"Myelin contains a very high amount of cholesterol," explains Prof. Simons. "When myelin is destroyed, the cholesterol released has to be removed from the tissue." This is performed by microglia and macrophages, also referred to as phagocytes. They take up the damaged myelin, digest it and transport the non-digestible remainder, such as cholesterol, out of the cell by transport molecules. However, if too much cholesterol accumulates in the cell, cholesterol can forms needle-shaped crystals, which cause damage the cell. Using a mouse model, Simons and his team showed the devastating impact of the crystalline cholesterol: It activates the so-called inflammasome in phagocytes, which results in the release of inflammatory mediators, attracting even more immune cells. "Very similar problems occur in arteriosclerosis, however not in the brain tissue, but in blood vessels," says Simons.
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Although cholesterol synthesis in the brain is considered a different process than cholesterol synthesis in the rest of the body, lower plasma levels of HDL cholesterol have been found to be related to MS. Cardiovascular researchers have been looking at this fact, in relation to the heart brain connection.
HDL plasma levels have also been associated with other neurodegenerative diseases such as multiple sclerosis (MS).74 Patients in the acute phase MS have been reported to have lower HDL-C levels compared with those in the remission phase, and they show a higher probability of developing acute inflammatory lesions (assessed by MRI).74–768 Moreover, HDL inhibits cytokine-induced expression of adhesion molecules in endothelial cells.72
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Why are HDL levels important? Because HDL, also known as "good cholesterol", contains the transport protein ApoA1---needed to take cholesterol out of the blood and tissue.
Here's more research on low levels of ApoA1 found to be linked to MS severity. The lower HDL
ApoA1 plasma levels, the more severe the disease.
ApoA1 was reduced by approximately 25% in patients with relapsing-remitting MS, 50% in those with secondary progressive MS, and 75% in patients with primary progressive MS, the most severe form of the disease. link
Here's a whole blog post from 2013 on "Good" cholesterol and your brain
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While we wait for researchers to create their cholesterol transport block buster MS drug, or to repurpose things like statins (please, don't go there, so many side effects!)---there are things pwMS can do today, to encourage this process in their own bodies, by increasing your HDL levels with lifestyle.
1. Don't smoke. Quitting smoking will increase good cholesterol by 10%
2. Lose weight. Extra weight depletes HDL.
3. Exercise. Within 2 months of regular exercise, you can increase your HDL by 5%
4. Choose healthier fats for your diet. Avoid transfats and saturated animal fats. Choose omega 3s and monosaturated fats found in nuts, olive oil, and fish
5. Add fiber to your diet--lots of fresh fruits and vegetables, legumes and oats
6. Limit alcohol consumption.
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7. Check your vitamin D, magnesium, calcium and zinc levels--make sure they are in balance.
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7. Check your vitamin D, magnesium, calcium and zinc levels--make sure they are in balance.
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Keep an eye on the latest MS research.
It continues to affirm the heart-brain connection, and the importance of living a vascularly healthy life.
Be well,
Joan
Joan thank you always from me here in the UK for sharing lots of informative information as you always have done .
ReplyDeleteHi Joan!
ReplyDeleteMy question has nothing to do with this post (which is great given that people with 20ml+ a day of flaxseed oil have fewer relapses).
Do you have any scientific evidence of the lesions on the spinal cord?
There's an article that you mention about the 7T MRI where they see a blood vessel leaking in the center of a lesion.
Your research has a lot to do with BBB and I would like to know more about the spinal cord.
I look forward to your reply!
Thanks
Ricardo
Hi Ricardo---there were links found between azygos vein stenosis and spinal lesions in people with SPMS and PPMS in Dr. Zamboni's original CCSVI paper. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2647682/
DeleteYou are absolutely right--the majority of central vein sign/ microbleed imaging is done in the brain. 7Tesla imaging of the spine has only just begun--advances of imaging in the spine are at least 10 yrs. behind brain imaging. https://www.medpagetoday.com/resource-center/MS-Resource-Center/Advanced-Spinal-Cord-Imaging/a/62709
Perhaps the central vein sign will be found more in spinal lesions, as well. Here's a good paper:
https://www.nature.com/articles/nrneurol.2016.166
"Although most studies imaged the supratentorial brain only, central veins have also been demonstrated in lesions located in the thalamus, cerebellum and pons of patients with MS31,34. To our knowledge, no in vivo reports are available on central veins in MS lesions located in the spinal cord, although pathological evidence of this phenomenon exists35."
Thanks a lot for spending your time finding those references! I will go through them this weekend. Thanks again!
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