Reversing bacteria-induced vitamin D receptor dysfunction is key to autoimmune disease.

[beaverfury]

Abstract http://www.ncbi.nlm.nih.gov/pubmed/19758226
Vitamin D research is discussed in light of the hypothesis that the lower average levels of vitamin D frequently observed in autoimmune disease are not a sign of deficiency. Instead, it is proposed that the lower levels result from chronic infection with intracellular bacteria that dysregulate vitamin D metabolism by causing vitamin D receptor (VDR) dysfunction within phagocytes. The VDR dysfunction causes a decline in innate immune function that causes susceptibility to additional infections that contribute to disease progression. Evidence has been accumulating that indicates that a number of autoimmune diseases can be reversed by gradually restoring VDR function with the VDR agonist olmesartan and subinhibitory dosages of certain bacteriostatic antibiotics. Diseases showing favorable responses to treatment so far include systemic lupus erythematosis, rheumatoid arthritis, scleroderma, sarcoidosis, Sjogren's syndrome, autoimmune thyroid disease, psoriasis, ankylosing spondylitis, Reiter's syndrome, type I and II diabetes mellitus, and uveitis. Disease reversal using this approach requires limitation of vitamin D in order to avoid contributing to dysfunction of nuclear receptors and subsequent negative consequences for immune and endocrine function. Immunopathological reactions accompanying bacterial cell death require a gradual elimination of pathogens over several years. Practical and theoretical implications are discussed, along with the compatibility of this model with current research.


I find this really intriguing though i cant quite get my head around it.

They say, ' Disease reversal using this approach requires limitation of vitamin D in order to avoid contributing to dysfunction of nuclear receptors'.

I would have thought a VDR dysfunction would require more vitamin D supplementation, not less?

Though i realise there is not necessarily a linear relationship between supplementing vit D and getting VDReceptors to function properly.
Valentijn points this out in her thread http://forums.phoenixrising.me/index.php?threads/interesting-vdr-variations.24480/

Can anyone explain to me how excess Vitamin D might contribute to VDR dys-function?

Anyone tried Olmesartan ?

 

[Art Vandelay]

Hi Beaverfury, I've been using Olmesartan for years as part of the Marshall Protocol and it definitely reduces my inflammation, insomnia, brain fog and fatigue. Although it does reactivate your immune system, so many people find they have to deal with significant Herxheimer reactions and a huge increase in sensitivity to vitamin D.

I'm a bit brain fogged today so can't explain it all very well, but this site is a good place to start: http://bacteriality.com/about-the-mp/