Epac1 mediates protein kinase A–independent mechanism of forskolin-activated intestinal chloride secretion

Anderson; Barrett; Barrett; Barrett; Barrett; Bos; Boucher; Cass; Chijiwa; Christensen; Chung-Ming Tse; Cliff; Conway; Cuppoletti; Damian B. van Rossum; Davies; de Rooij; Denning; Dharmsathaphorn; Doolen; Dyachok; Dyachok; Evans; Evellin; Factor; Fuller; George P.H. Leung; Gray; Gyömörey; Hartzell; Hartzell; Hidaka; Hidaka; Hillesheim; Holz; Hoque; Huang; Huflejt; Jentsch; Jordt; Kang; Kang; Kawasaki; Kazi Mirajul Hoque; Kidd; Kleppisch; Klöckner; Lewis; Linxi Chen; Lochner; Lorenowicz; Ma; Maly; Marty; McCarty; Merlin; Mohammad-Panah; Mun; Muroi; Nicholas C. Zachos; Owen M. Woodward; Pereira; Reenstra; Riordan; Sandra E. Guggino; Schmidt; Schultz; Schwiebert; Semrad; Sheppard; Thelin; Vajanaphanich; Verkman; Wang; William B. Guggino; Yang; Yip

Epac1 mediates protein kinase A–independent mechanism of forskolin-activated intestinal chloride secretion

Authors: Anderson
Barrett
Barrett
Barrett
Barrett
Bos
Boucher
Cass
Chijiwa
Christensen
Chung-Ming Tse
Cliff
Conway
Cuppoletti
Damian B. van Rossum
Davies
de Rooij
Denning
Dharmsathaphorn
Doolen
Dyachok
Dyachok
Evans
Evellin
Factor
Fuller
George P.H. Leung
Gray
Gyömörey
Hartzell
Hartzell
Hidaka
Hidaka
Hillesheim
Holz
Hoque
Huang
Huflejt
Jentsch
Jordt
Kang
Kang
Kawasaki
Kazi Mirajul Hoque
Kidd
Kleppisch
Klöckner
Lewis
Linxi Chen
Lochner
Lorenowicz
Ma
Maly
Marty
McCarty
Merlin
Mohammad-Panah
Mun
Muroi
Nicholas C. Zachos
Owen M. Woodward
Pereira
Reenstra
Riordan
Sandra E. Guggino
Schmidt
Schultz
Schwiebert
Semrad
Sheppard
Thelin
Vajanaphanich
Verkman
Wang
William B. Guggino
Yang
Yip
Publication date: 1 January 2010
Publisher: The Rockefeller University Press
Doi

Abstract

Intestinal Cl− secretion is stimulated by cyclic AMP (cAMP) and intracellular calcium ([Ca2+]i). Recent studies show that protein kinase A (PKA) and the exchange protein directly activated by cAMP (Epac) are downstream targets of cAMP. Therefore, we tested whether both PKA and Epac are involved in forskolin (FSK)/cAMP-stimulated Cl− secretion. Human intestinal T84 cells and mouse small intestine were used for short circuit current (Isc) measurement in response to agonist-stimulated Cl− secretion. FSK-stimulated Cl− secretion was completely inhibited by the additive effects of the PKA inhibitor, H89 (1 µM), and the [Ca2+]i chelator, 1,2-bis-(o-aminophenoxy)-ethane-N,N,N’,N’-tetraacetic acid, tetraacetoxymethyl ester (BAPTA-AM; 25 µM). Both FSK and the Epac activator 8-pCPT-2’-O-Me-cAMP (50 µM) elevated [Ca2+]i, activated Ras-related protein 2, and induced Cl− secretion in intact or basolateral membrane–permeabilized T84 cells and mouse ileal sheets. The effects of 8-pCPT-2’-O-Me-cAMP were completely abolished by BAPTA-AM, but not by H89. In contrast, T84 cells with silenced Epac1 had a reduced Isc response to FSK, and this response was completely inhibited by H89, but not by the phospholipase C inhibitor U73122 or BAPTA-AM. The stimulatory effect of 8-pCPT-2’-O-Me-cAMP on Cl− secretion was not abolished by cystic fibrosis transmembrane conductance (CFTR) inhibitor 172 or glibenclamide, suggesting that CFTR channels are not involved. This was confirmed by lack of effect of 8-pCPT-2’-O-Me-cAMP on whole cell patch clamp recordings of CFTR currents in Chinese hamster ovary cells transiently expressing the human CFTR channel. Furthermore, biophysical characterization of the Epac1-dependent Cl− conductance of T84 cells mounted in Ussing chambers suggested that this conductance was hyperpolarization activated, inwardly rectifying, and displayed a Cl−>Br−>I− permeability sequence. These results led us to conclude that the Epac-Rap-PLC-[Ca2+]i signaling pathway is involved in cAMP-stimulated Cl− secretion, which is carried by a novel, previously undescribed Cl− channel

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