Date published: 2025-9-17

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StARD5 Inhibitors

Regarding the chemical class of "StARD5 inhibitors," since there are no direct inhibitors known, the term is a bit of a misnomer. The focus is on compounds that can influence cholesterol metabolism and steroidogenesis, processes where StARD5 may play a role. The listed chemicals are inhibitors of various enzymes in the steroid biosynthesis pathway, which is tightly linked to cholesterol transport and homeostasis, both of which are critical to the function of StARD5. By inhibiting these enzymes, the compounds can indirectly affect the activity of StARD5 by altering the availability of cholesterol or the balance of steroid hormones within the cell.

The chemicals belong to different classes, including azoles (like Ketoconazole), spirolactones (like Spironolactone), imidazoles (like Metyrapone), and others, each with distinct mechanisms of action on enzymes involved in steroid biosynthesis. Aminoglutethimide, an older compound, was one of the first drugs found to inhibit the P450scc, which is crucial for the conversion of cholesterol to pregnenolone, the first step in the synthesis of all steroid hormones. Subsequent generations of inhibitors have been developed with increased specificity for various enzymes in the steroidogenesis pathway. Inhibiting these enzymes can alter the intracellular levels of cholesterol and steroids, thereby influencing the activity of StARD5, albeit indirectly.

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