Akt May Associate with Insulin-responsive Vesicles Via Interaction with Sortilin

Overview

Journal FEBS Lett

Specialty Biochemistry

Date 2023 Dec 17

PMID 38105115

Authors

Nava Zaarur

Anatoli B Meriin

Maneet Singh

Raghuveera K Goel

Joseph Zaia

Konstantin V Kandror

Affiliations

Soon will be listed here.

Abstract

Insulin-responsive vesicles (IRVs) deliver the glucose transporter Glut4 to the plasma membrane in response to activation of the insulin signaling cascade: insulin receptor-IRS-PI3 kinase-Akt-TBC1D4-Rab10. Previous studies have shown that Akt, TBC1D4, and Rab10 are compartmentalized on the IRVs. Although functionally significant, the mechanism of Akt association with the IRVs remains unknown. Using pull-down assays, immunofluorescence microscopy, and cross-linking, we have found that Akt may be recruited to the IRVs via the interaction with the juxtamembrane domain of the cytoplasmic C terminus of sortilin, a major IRV protein. Overexpression of full-length sortilin increases insulin-stimulated phosphorylation of TBC1D4 and glucose uptake in adipocytes, while overexpression of the cytoplasmic tail of sortilin has the opposite effect. Our findings demonstrate that the IRVs represent both a scaffold and a target of insulin signaling.

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