Proteomics

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Map of the Kir2.1 interactome using BioID


ABSTRACT: Kir2.1, an inward rectifier potassium channel, plays an important role in controlling membrane potential specially in cardiomyocytes. Here we explore its interactome via proximity biotin labeling and affinity purification approach (BioID). First, BioID membrane controls were generated with randomly selected transmembrane domains from yeast proteins, demonstrating the identification of membrane-associated proteins more than GFP or NLS controls. Using this control and a mutation from Andersen-Tawil syndrome which causes Kir2.1 Golgi accumulation, we have identified the most comprehensive Kir2.1 interactome and also found clues to its spatial information in subcellular levels. The interactome is showing that Kir2.1 in plasma membrane is surrounded by desmosome, integrin, cadherin and dystrophin-glycoprotein complex complexes, and supported by MAGUK family scaffold proteins. On the other hand, Kir2.1 mutant BioID revealed the COPII-mediated delivery of Kir2.1 from ER to Golgi and lysosome-mediated degradation of Golgi-accumulated and/or retrograde Kir2.1. Validating the interactome with co-immunoprecipitation, confocal microscope, and patch clamp analysis, we concluded that Kir2.1 is located in the defined membrane environment and is actively regulated by endosomal sorting for lysosome degradation.

INSTRUMENT(S): LTQ Orbitrap Velos

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Permanent Cell Line Cell, Kidney

SUBMITTER: Jean-Francois Rual  

LAB HEAD: Jean-Francois Rual

PROVIDER: PXD011004 | Pride | 2020-06-17

REPOSITORIES: Pride

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Publications

Kir2.1 Interactome Mapping Uncovers PKP4 as a Modulator of the Kir2.1-Regulated Inward Rectifier Potassium Currents.

Park Sung-Soo SS   Ponce-Balbuena Daniela D   Kuick Rork R   Guerrero-Serna Guadalupe G   Yoon Justin J   Mellacheruvu Dattatreya D   Conlon Kevin P KP   Basrur Venkatesha V   Nesvizhskii Alexey I AI   Jalife José J   Rual Jean-François JF  

Molecular & cellular proteomics : MCP 20200615 9


Kir2.1, a strong inward rectifier potassium channel encoded by the <i>KCNJ2</i> gene, is a key regulator of the resting membrane potential of the cardiomyocyte and plays an important role in controlling ventricular excitation and action potential duration in the human heart. Mutations in <i>KCNJ2</i> result in inheritable cardiac diseases in humans, <i>e.g.</i> the type-1 Andersen-Tawil syndrome (ATS1). Understanding the molecular mechanisms that govern the regulation of inward rectifier potassi  ...[more]

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