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Ian Joris

Ian Joris, 20

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2-4 In the U.S., about 20% of White adults and 75% of Black adults have blood levels of vitamin D below 50 nmol/L. Worldwide, an estimated 1 billion people have inadequate levels of vitamin D in their blood, and deficiencies can be found in all ethnicities and age groups. NHANES data found that the median intake of vitamin D from food and supplements in women ages 51 to 71 years was 308 IU daily, but only 140 IU from food alone (including fortified products).
Instead, mast cell function, as determined by histamine release, may be regulated by androgens, as histamine levels at some peripheral sites are reduced after castration (61). Skin residing mast cells have been found to express the AR, however, neither numbers nor distribution of these cells are affected by altering levels of androgens (35, 41). Further support for androgen-induced granulopoiesis and neutrophil differentiation comes from studies of stanozolol, a testosterone analog, showing an increased prevalence of myelocytes and metamyelocytes as well as accelerated neutrophil maturation in treated female mice (50). The expression of AR in various immune organs and multiple immune cells provides some indication of the level at which androgens influence immunity (Table 1).
Vitamin D and calcium intakes from diet and supplements were assessed throughout the 20-year study. Vitamin D deficiency may negatively affect the biochemical pathways that lead to the development of Type 2 diabetes (T2DM), including impairment of beta cell function in the pancreas, insulin resistance, and inflammation. No association was found between taking the supplements and a lower risk of major cardiovascular events (heart attack, stroke, or death from cardiovascular causes) compared with the placebo.
So, what do we know about shilajit’s health benefits? And almost all of those studies are small and have methodologic problems," he explains. "There are only a few studies that assess shilajit’s impact on different medical conditions.
Finally, gonadectomy has been found to drive increased TLR4 expression by male murine macrophages leading to elevated pro-inflammatory responses during infection (58), suggesting that one mechanism by which androgens are immunosuppressive is by limiting myeloid cell responsiveness to pathogens. Together, these studies suggest that androgens drive neutrophil differentiation and/or survival in mice and humans. Similarly, androgen-deficient prostate cancer patients and gona-dectomized male mice also display neutropenia, prior to androgen-replacement therapy/DHT treatment (48, 49). As mentioned above, all myeloid progenitor cells express the classical AR (34, 35) and testosterone has been shown to affect early myelopoiesis (45–47).

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