GIPC3 couples to MYO6 and PDZ domain proteins, and shapes the hair cell apical region

Author:

Chatterjee Paroma1,Morgan Clive P.1ORCID,Krey Jocelyn F.1,Benson Connor1ORCID,Goldsmith Jennifer1,Bateschell Michael1,Ricci Anthony J.2,Barr-Gillespie Peter G.1ORCID

Affiliation:

1. Oregon Hearing Research Center & Vollum Institute, Oregon Health & Science University 1 , Portland, OR 97239 , USA

2. Stanford University 2 Department of Otolaryngology—Head & Neck Surgery , , Stanford, CA 94305 , USA

Abstract

ABSTRACT GIPC3 has been implicated in auditory function. Here, we establish that GIPC3 is initially localized to the cytoplasm of inner and outer hair cells of the cochlea and then is increasingly concentrated in cuticular plates and at cell junctions during postnatal development. Early postnatal Gipc3KO/KO mice had mostly normal mechanotransduction currents, but had no auditory brainstem response at 1 month of age. Cuticular plates of Gipc3KO/KO hair cells did not flatten during development as did those of controls; moreover, hair bundles were squeezed along the cochlear axis in mutant hair cells. Junctions between inner hair cells and adjacent inner phalangeal cells were also severely disrupted in Gipc3KO/KO cochleas. GIPC3 bound directly to MYO6, and the loss of MYO6 led to altered distribution of GIPC3. Immunoaffinity purification of GIPC3 from chicken inner ear extracts identified co-precipitating proteins associated with adherens junctions, intermediate filament networks and the cuticular plate. Several of immunoprecipitated proteins contained GIPC family consensus PDZ-binding motifs (PBMs), including MYO18A, which bound directly to the PDZ domain of GIPC3. We propose that GIPC3 and MYO6 couple to PBMs of cytoskeletal and cell junction proteins to shape the cuticular plate.

Funder

National Institute on Deafness and Other Communication Disorders

Oregon Health & Science University

Publisher

The Company of Biologists

Subject

Cell Biology

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