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초록
The Transient Receptor Potential, Canonical (TRPC) channels function as non-selective, Ca2+-permeable channels and mediate numerous cellular functions. It is commonly assumed that TRPC channels are activated by stimulation of Gaq coupled receptors. However, whether the Gaq-PLC pathway regulates the TRPC4/5 channels and how these channels are regulated by other Ga proteins is unknown. Here, we discovered that Gai subunits, rather than Gaq, are the primary and direct activators of TRPC4 and TRPC5. These channels were activated by the stimulation of Muscarinic receptor 2 that regulated by pertusis toxin sensitive manner in the activation process of channel.The expression of the constitutively active Gai mutants selectively activates TRPC4 and TRPC5 channels. TRPC4 is activated by several Gai subunits, most prominently by Gai2 and TRPC5 is activated primarily by Gai3. On the other hand, to investigate the effect of Gß? on the activation process of TRPC4/5, we used Gß mutants (Gß1 W99A and Gß1 I80A). The result from these mutants does not suggest the role of Gß? subunit as a key modulator for TRPC4/5 activation. Finally, to check out that the mechanism of TRPC4 activation by Gai2, we expressed TRPC4 C-terminus deletion and truncation mutants in HEK293 cells. When the region from 700 to 720 in C-terminal region of TRPC4 channel was deleted, electrophysiological activity did not elicited by Gai2 QL and infused GTP?S. Also co-IP between TRPC4 and Gai2 QL was altered by the deleted c-terminal region (700-720).These findings indicate an essential role of Gai proteins as novel activators for TRPC4/5 and reveal the molecular mechanism by which G proteins activate the channels. * This research was supported by the National Research Foundation of Korea (NRF) funded by the Korea government (MEST) (2008-2005948 and 2010-0019472).
- 제목
- SELECTIVE Gai SUBUNITS AS NOVEL DIRECT ACTIVATORS OF TRPC4
- 저자
- SUH, CHANG KOOK
- 학회명
- 56th Biophysical Society Annual Meeting
- 개최지
- San Diego, CA USA
- 학회 개최일
- 2012-02-25 ~ 2012-02-29