Date published: 2025-11-8

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BBS1 Activators

In the case of BBS1, a gene implicated in Bardet-Biedl syndrome, identifying direct chemical activators is not straightforward due to its complex involvement in genetic pathways and the BBS protein complex. However, compounds that indirectly influence the cellular environment, signaling pathways, or processes related to ciliary function may offer avenues to modulate BBS1 function. Compounds such as Lithium Chloride and Forskolin, which impact the Wnt signaling pathway and cAMP levels respectively, might have indirect effects on ciliary biology, a key aspect of BBS1's role. Similarly, Retinoic Acid, with its broad effects on gene expression and development, could influence pathways associated with BBS1.

Metabolic modulators like Metformin and vitamins such as Vitamin D and Niacin (Vitamin B3) can also have an impact. While their primary roles are in metabolism, their secondary effects on cellular processes could extend to pathways relevant to BBS1. The involvement of BBS1 in a range of cellular processes, including those related to cilia, suggests that altering the general cellular environment could indirectly modulate its function. Additionally, natural compounds with various biological activities, such as Curcumin, Omega-3 Fatty Acids, Epigallocatechin Gallate (EGCG), and Resveratrol, might influence signaling pathways linked to BBS1. These compounds are known for their roles in modulating inflammation, oxidative stress, and cellular metabolism, all of which could intersect with the biological pathways in which BBS1 is involved. Through this indirect approach, these compounds offer a way to influence BBS1 function, especially in the context of research into Bardet-Biedl syndrome and related ciliary dysfunctions. This perspective is crucial in understanding the complex network of interactions and pathways associated with BBS1 and provides a starting point for exploring strategies for conditions related to BBS1 dysfunction.

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