Date published: 2025-12-22

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TMEM136 Inhibitors

Chemical inhibitors of TMEM136 encompass a diverse array of compounds that target various signaling pathways and kinases implicated in the regulation of its activity. Staurosporine and Bisindolylmaleimide I are broad-spectrum kinase inhibitors with high potency against protein kinases and protein kinase C (PKC), respectively. Their inhibition profile suggests that they can suppress TMEM136 activity by thwarting the phosphorylation events essential for its function. Wortmannin and LY294002 share a similar mechanism of action as phosphoinositide 3-kinases (PI3K) inhibitors. By obstructing the PI3K pathway, they can diminish the downstream signaling cascades that might otherwise culminate in the activation of TMEM136. This disruption can lead to a reduction in the biological processes that TMEM136 usually mediates.

Further, compounds such as SP600125 and AG490 specifically target the c-Jun N-terminal kinase (JNK) and the JAK/STAT signaling pathways, respectively. The inhibition by SP600125 implies that if TMEM136 activity is contingent upon JNK-mediated signaling, this kinase's suppression can attenuate TMEM136's role in the cellular context. AG490, by inhibiting JAK/STAT pathway, can similarly alter TMEM136's regulatory functions. Additionally, U0126, PD98059, and SB203580 are inhibitors of the mitogen-activated protein kinase (MAPK) pathway, with U0126 and PD98059 targeting MEK1/2 and SB203580 specifically inhibiting p38 MAP kinase. The inhibition of these kinases can result in a decrease in TMEM136 activity if it is dependent on the MAPK signaling pathway. Lastly, PP2 and Gö 6983 are selective inhibitors of Src family tyrosine kinases and PKC, respectively. PP2's action indicates that Src family kinases' inhibition can lead to a decrease in TMEM136 activity, while Gö 6983's ability to inhibit PKC suggests a similar potential effect on TMEM136 if PKC is involved in its regulation.

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