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The conversion of pregnenolone to progesterone takes place in two steps.
The products range from sugar-free maple syrup to the steroid hormone pregnenolone.
The human placenta produces pregnenolone and progesterone from circulating cholesterol.
Like other steroids, pregnenolone consists of four interconnected cyclic hydrocarbons.
Progesterone is prepared by the Oppenauer oxidation of pregnenolone.
He had tested positive three times for DHEA and pregnenolone.
This vicinal diol is then further oxidized with loss of the side chain starting at position C-22 to produce pregnenolone (').
CYP17A1 functions in steroidogenesis, where it converts pregnenolone and progesterone to their 17-hydroxy forms.
The final step cleaves the bond between carbons 20 and 22, resulting in the production of pregnenolone and isocaproic acid.
It catalyzes hydroxylation of 17-hydroxyprogesterone to 11-deoxycortisol in the glucocorticoid pathway, which starts from pregnenolone and finishes with cortisol.
As you can see in Figure 3.2, the Steroid Family Tree begins with cholesterol, some of which is converted to the hormone pregnenolone.
TRPM3 was shown to be activated by the neurosteroid pregnenolone sulphate in pancreatic beta cell.
ACTH stimulates uptake of cholesterol and synthesis of pregnenolone.
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As such 17-OH-pregenolone represents an intermediary in the delta-5-pathway that leads from pregnenolone to DHEA.
In humans the reticularis layer does contain 17 alpha-hydroxylase; this hydroxylates pregnenolone, which is then converted to cortisol by a mixed function oxidase.
Pregnenolone sulfate is a derivative of pregnenolone.
Three times from October 2009 to January 2010, he tested positive for steroid derivatives called DHEA and pregnenolone.
It also catalyzes hydroxylation of progesterone to 11-deoxycorticosterone (DOC) in the mineralocorticoid pathway on its way from pregnenolone to aldosterone.
The diagnosis is usually confirmed by the distinctive pattern of adrenal steroids: elevated pregnenolone, 17-hydroxypregnenolone, DHEA, and renin.
Baulieu discovered that DHEA and pregnenolone are produced in the brain and introduced the term "neurosteroids" in 1981.
It has only weak glucocorticoid and mineralocorticoid potencies in humans and is important mainly as an intermediate in the steroidogenic pathway from pregnenolone to aldosterone.
It has been shown to have neuroprotective and cardioprotective effects and to stimulate steroidogenesis of pregnenolone in the brain, which may be linked to its neuroprotective action.
Accordingly, production of hormones in all three layers of the adrenal cortex is limited by the transportation of cholesterol into the mitochondria and by its conversion into pregnenolone.