Chronic Fractalkine Administration Improves Glucose Tolerance and Pancreatic Endocrine Function

Overview

Journal J Clin Invest

Specialty General Medicine

Date 2018 Mar 6

PMID 29504946

Citations 18

Authors

Matthew Riopel

Jong Bae Seo

Gautam K Bandyopadhyay

Pingping Li

Joshua Wollam

Heekyung Chung

Seung-Ryoung Jung

Anne Murphy

Maria Wilson

Ron de Jong

Sanjay Patel

Deepika Balakrishna

James Bilakovics

Andrea Fanjul

Artur Plonowski

Duk-Su Koh

Christopher J Larson

Jerrold M Olefsky

Yun Sok Lee

Affiliations

Soon will be listed here.

Abstract

We have previously reported that the fractalkine (FKN)/CX3CR1 system represents a novel regulatory mechanism for insulin secretion and β cell function. Here, we demonstrate that chronic administration of a long-acting form of FKN, FKN-Fc, can exert durable effects to improve glucose tolerance with increased glucose-stimulated insulin secretion and decreased β cell apoptosis in obese rodent models. Unexpectedly, chronic FKN-Fc administration also led to decreased α cell glucagon secretion. In islet cells, FKN inhibited ATP-sensitive potassium channel conductance by an ERK-dependent mechanism, which triggered β cell action potential (AP) firing and decreased α cell AP amplitude. This results in increased glucose-stimulated insulin secretion and decreased glucagon secretion. Beyond its islet effects, FKN-Fc also exerted peripheral effects to enhance hepatic insulin sensitivity due to inhibition of glucagon action. In hepatocytes, FKN treatment reduced glucagon-stimulated cAMP production and CREB phosphorylation in a pertussis toxin-sensitive manner. Together, these results raise the possibility of use of FKN-based therapy to improve type 2 diabetes by increasing both insulin secretion and insulin sensitivity.

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