cGMP‐dependent kinase 2, Na+/H+ exchanger NHE3, and PDZ‐adaptor NHERF2 co‐assemble in apical membrane microdomains

Author:

Luo Min12,Liu Yongjian13,Nikolovska Katerina1ORCID,Riederer Brigitte1,Patrucco Enrico45,Hofmann Franz4,Seidler Ursula1ORCID

Affiliation:

1. Department of Gastroenterology, Hepatology, Infectiology and Endocrinology Hannover Medical School Hannover Germany

2. Department of Infectious Diseases The Second Affiliated Hospital of Chongqing Medical University Chongqing China

3. Department of Endocrinology The Second Affiliated Hospital of Chongqing Medical University Chongqing China

4. Institut für Pharmakologie und Toxikologie TU München München Germany

5. Department of Molecular Biotechnology and Health Science University of Torino Torino Italy

Abstract

AbstractAimTrafficking, membrane retention, and signal‐specific regulation of the Na+/H+ exchanger 3 (NHE3) are modulated by the Na+/H+ Exchanger Regulatory Factor (NHERF) family of PDZ‐adapter proteins. This study explored the assembly of NHE3 and NHERF2 with the cGMP‐dependent kinase II (cGKII) within detergent‐resistant membrane microdomains (DRMs, “lipid rafts”) during in vivo guanylate cycle C receptor (Gucy2c) activation in murine small intestine.MethodsSmall intestinal brush border membranes (siBBMs) were isolated from wild type, NHE3‐deficient, cGMP‐kinase II‐deficient, and NHERF2‐deficient mice, after oral application of the heat‐stable Escherichia coli toxin (STa) analog linaclotide. Lipid raft and non‐raft fractions were separated by Optiprep density gradient centrifugation of Triton X‐solubilized siBBMs. Confocal microscopy was performed to study NHE3 redistribution after linaclotide application in vivo.ResultsIn the WT siBBM, NHE3, NHERF2, and cGKII were strongly raft associated. The raft association of NHE3, but not of cGKII, was NHERF2 dependent. After linaclotide application to WT mice, lipid raft association of NHE3 decreased, that of cGKII increased, while that of NHERF2 did not change. NHE3 expression in the BBM shifted from a microvillar to a terminal web region. The linaclotide‐induced decrease in NHE3 raft association and in microvillar abundance was abolished in cGKII‐deficient mice, and strongly reduced in NHERF2‐deficient mice.ConclusionNHE3, cGKII, and NHERF2 form a lipid raft‐associated signal complex in the siBBM, which mediates the inhibition of salt and water absorption by Gucy2c activation. NHERF2 enhances the raft association of NHE3, which is essential for its close interaction with the exclusively raft‐associated activated cGKII.

Publisher

Wiley

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