[Lotus]

Interesting, this study claims Vitamin D increases aromatase activity.
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Sunday, May 29, 2011
Vitamin D and Testosterone. Sunshine Vitamin Not So Manly, After all? Vitamin D Increases Aromatase Activity in Sertoli Cells

Vitamin D is all the rave. Even mainstream nutritionists are now jumping on the vitamin D bandwagon and the hype is spilling over from the Internet to newspapers and TV stations. "Take your Vitamin D!" is what children and adults, men and women, couch-potatoes and top-level athletes are told. Recently discovered problems related to the accurate measurement of actual vitamin D levels aside (e.g. Shah. 2011), a recent investigation into the immediate effects of vitamin D on aromatase activity in Sertoli cells of rat testes, suggests that we have to reevaluate whether this advice, which is hitherto largely based on epidemiological data, is not overgeneralizing, to say the least.


After all, the results of the aforementioned study, which has been published in the Journal of Vertebrate Reproduktive Science & Technology (Zanatta. 2011), clearly indicate that, contrary to common believe, your testosterone levels will not benefit from high vitamin D levels. On the contrary, in their in-vitro study Zanatta et al. found that incubation of Sertoli cells with 100nm 1,25D "increased the amount of aromatase transcript [...] in [Sertoli cells of] 30-day-old rats". Additionally, the scientists were also able to show that the increased aromatase activity was not exclusively due to a genomic effect, but was mediated via a "non-genomic activation of the membrane-bound vitamin D receptor involving the PKA pathway". Whether this is a tissue-, rat- or even age-specific effect does yet still warrant further investigation.
The latter is especially true in view of conflicting data on the effects of vitamin D on aromatase activity in especially in view of previous studies such as Lundgvist 2011 et al. (Lundgvist. 2011) who found that
In breast cancer MCF-7 cells, aromatase gene expression and estradiol production were decreased, while production of androgens was markedly increased. In NCI-H295R cells, 1α,25-dihydroxyvitamin D(3) stimulated aromatase expression and decreased dihydrotestosterone production. In prostate cancer LNCaP cells, aromatase expression increased after the same treatment, as did production of testosterone and dihydrotestosterone. In summary, our data show that 1α,25-dihydroxyvitamin D(3) exerts tissue-specific effects on estrogen and androgen production and metabolism.
So, will taking supplemental Vitamin D3 (1,25D) transform you into a hermaphrodite? Will you get rid of gynecomastia (gyno), but develop testicular cancer? The answer to both questions is probably "NO" And I am by no means suggesting that you extrapolate the rat data from isolated sertoli cells to human beings, but In view of these findings, it is nevertheless becoming increasingly questionable whether the correlations between testosterone and vitamin D that have been observed in epidemiological studies have not been misinterpreted as causative, where in fact, both, higher testosterone, as well as vitamin D levels, are a mere results of confounding variables such as an overall healthier, more active lifestyle. After all, our previous understanding of the connection between vitamin D and testosterone could have been as misleading as the idea that firetrucks cause fire, because an "epidemiological" investigation of fires would show that they are present whenever ones breaks out.


http://suppversity.blogspot.com/2011/05/...shine.html

[Lotus]

Sooo, lots of new research to share, (maybe too much, lol)

Here's some interesting research collected,

• Progesterone inhibits prolactin, estrogen receptors and aromatase, also DHT (we already knew that though).
  
  
• 5 alpha reductase inhibits progesterone receptors.
  
  
• Synthetic hormones bind to the wrong receptors, those receptors may convey inaccurate signals, which throws the body off balance.
  (This is why BCP’s cause so many hormonal imbalances and side effects).
  
  
• Estradiol in part regulates progesterone production physiologically and blocks progesterone production in a pharmacological or pathological state in the human corpus luteum.
  
  
• Forskolin and dibutyryl-cyclic AMP-stimulates progesterone production.
  
  
• Omega-3 fats, a polyunsaturtated type of fat, is high in testosterone.
  (Omega-3 fatty acids contribute to testosterone conversion and production as well as muscle protein synthesis. Seeds such as flax seed, sunflower also provide healthy fats, including omega-3 fatty acids).
  
• Follicle granulosa cells have FSH-sensitive aromatase activity and proliferate in response to estrogens.
  
• Indole-3-carbinol selectively uncouples expression and activity of estrogen receptor subtypes in human breast cancer cells.
  

More to follow-

[Lotus]

♦ Genetic males produce progesterone, but about half the amount of females. Progesterone is made in men by the adrenal glands and testes. Progesterone is vital to good health in both women and men.

♦ During the aging process, progesterone levels fall in men, especially after age 60. Progesterone is the chief inhibitor of an enzyme called 5-alpha reductase that is responsible for converting testosterone to dihydrotestosterone (DHT).

♦ When the level of progesterone falls in genetic males, the amount of conversion from testosterone to DHT increases.

[Lotus]

♦ Studies demonstrate that ERβ-mediated estradiol actions are vital to FSH-induced granulosa cell differentiation.

♦ Protein interaction between ER alpha and ER beta was demonstrated in vitro by GST pull-down assay and in vivo by immunoprecipitation. Thus, this study indicates that ER alpha and ER beta can interact in vivo, cross-signaling each other.

♦ Studies on large doses of fenugreek on four target organs—the liver, stomach, kidney and small and large intestine—reveal that the liver is the only one affected by the high doses. (Although anything in high doses isn't a good idea to begin with, why take the risk).

Animal research on fenugreek toxicity reveals that very large doses of the herb can lead to mild hepatitis according to Aziza M. Hassan, lead author of a study published in the "African Journal of Biotechnology."


   

Clinical Studies on Fenugreek.
http://www.arthmender.com/clinical_studies/fenugreek

Fenugreek Benefits for Men
http://www.livestrong.com/article/513411...s-for-men/

Libido enhancement supplements produced from fenugreek claim to increase sexual desire and performance in men. In a study published in the February 2011 issue of “Phytotherapy Research,” researchers recruited 60 men between the ages of 25 and 52 years without a history of erectile dysfunction and supplemented them with either a placebo or 600 milligrams of fenugreek extract per day for six weeks. The participants self-evaluated their satisfaction with fenugreek and reported that the supplement had a positive effect on libido. The study found that fenugreek extract had a significant influence on sexual arousal, energy and stamina and helped participants maintain a normal testosterone level.




♦ If estradiol is around in high enough dosages, it can bind to progesterone receptors and androgen (male hormone) receptors as well as to estrogen receptors

[Lotus]

(From the earlier post on progesterone)

♦ Progesterone reduces the aromatization of testosterone to estrogen. More progesterone thus generally means less estrogen, especially in men.

♦ Yet less estrogen can also reduce the effects of progesterone itself, because estrogen and progesterone strongly interact via cross-talk at both the estrogen and the progesterone receptor sites.

[Lotus]

Circulating Androgens --► Estrogens

- Unlike the ovaries and testes, which can synthesize their own androgen precursors, these sites are totally dependent on circulating androgens for conversion to estrogens - such androgens are produced by the adrenal cortex, ovarian stroma (especially in post-menopausal women with endometrial cancer, possibly mediated by LH and insulin) and testis Leydig cells;




   

- Estrogen produced at peripheral sites is probably only biologically active in local tissue - where the aromatase enzyme is produced to convert circulating androgens (ANDROSTENEDIONE in women) to estrogen in tissues containing aromatase, which include:

√ Adipose tissue (mesenchymal cells) – this is a major source of estrogen in men (also the brain) and becomes the major source in post-menopausal women; thus the amount of body fat significantly determines the amount of estrogen produced and stored; the breasts contain significant amounts of adipose tissue;

http://healyourselfathome.com/SUPPORTING...ction.aspx

[Lotus]

Just an update,

[pom19]

Wow Lotus, I still don't understand how you go out as a male.

[Lotus]

Wow Lotus, I still don't understand how you go out as a male.

Hey POM,

Well ya know, I wait till there's a full moon out, then I can be seen lurking in the shadows lol. I dunno, I'm not fooling anybody, so it's on auto pilot now.

[pom19]

Wow Lotus, I still don't understand how you go out as a male.

Hey POM,

Well ya know, I wait till there's a full moon out, then I can be seen lurking in the shadows lol. I dunno, I'm not fooling anybody, so it's on auto pilot now.

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