A Complex Relationship between Immunity and Metabolism in Drosophila Diet-Induced Insulin Resistance

生物 胰岛素抵抗 胰岛素受体 胰岛素 先天免疫系统 转录组 基因敲除 内分泌学 内科学 免疫系统 免疫学 基因表达 遗传学 基因 医学
作者
Laura Palanker Musselman,Jill L. Fink,Ana R. Grant,Jared A. Gatto,Bryon F. Tuthill,Thomas Baranski
出处
期刊:Molecular and Cellular Biology [Taylor & Francis]
卷期号:38 (2) 被引量:62
标识
DOI:10.1128/mcb.00259-17
摘要

Both systemic insulin resistance and tissue-specific insulin resistance have been described in Drosophila and are accompanied by many indicators of metabolic disease. The downstream mediators of insulin-resistant pathophysiology remain unclear. We analyzed insulin signaling in the fat body studying loss and gain of function. When expression of the sole Drosophila insulin receptor (InR) was reduced in larval fat bodies, animals exhibited developmental delay and reduced size in a diet-dependent manner. Fat body InR knockdown also led to reduced survival on high-sugar diets. To look downstream of InR at potential mediators of insulin resistance, transcriptome sequencing (RNA-seq) studies in insulin-resistant fat bodies revealed differential expression of genes, including those involved in innate immunity. Obesity-associated insulin resistance led to increased susceptibility of flies to infection, as in humans. Reduced innate immunity was dependent on fat body InR expression. The peptidoglycan recognition proteins (PGRPs) PGRP-SB2 and PGRP-SC2 were selected for further study based on differential expression studies. Downregulating PGRP-SB2 selectively in the fat body protected animals from the deleterious effects of overnutrition, whereas downregulating PGRP-SC2 produced InR-like phenotypes. These studies extend earlier work linking the immune and insulin signaling pathways and identify new targets of insulin signaling that could serve as potential drug targets to treat type 2 diabetes.

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