Date published: 2025-9-16

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IIGP1B Activators

IIGP1B Activators encompass a diverse array of chemical compounds that indirectly enhance the functional activity of IIGP1B, a protein characterized by its GTPase function. Forskolin, by activating adenylate cyclase and subsequently increasing cAMP levels, triggers PKA activation, which can enhance IIGP1B's GTPase activity, integral to its role in immune response. Epigallocatechin gallate (EGCG), as a kinase inhibitor, alleviates competition in signaling pathways, potentially amplifying IIGP1B's activity. Ionomycin, increasing intracellular calcium, may also boost IIGP1B's activity by activating calcium-dependent pathways. Similarly, LY294002 and Wortmannin, both PI3K inhibitors, along with Rapamycin, an mTOR inhibitor, reshape cellular signaling, indirectly influencing IIGP1B's functionality in immune and growth-related processes. U0126 and PD98059, targeting the MAPK/ERK pathway, and SB203580, inhibiting p38 MAPK, redirect signaling in a manner that could enhance IIGP1B's role. Trichostatin A, by altering gene expression, might also upregulate pathways involving IIGP1B.

Sildenafil Citrate, through its PDE5 inhibitory action, raises cGMP levels, potentially affecting pathways that enhance IIGP1B's activity. Thapsigargin, a SERCA pump inhibitor, causes an increase in cytosolic calcium, which could indirectly enhance IIGP1B's GTPase activity. These activators, each affecting distinct signaling pathways or cellular processes, collectively contribute to the modulation of IIGP1B's activity. The convergence of these diverse mechanisms on IIGP1B highlights the intricate network of biochemical pathways that regulate protein function, underscoring the complex interplay between various signaling molecules and pathways in the regulation of protein activities.

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