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The miR-23-27-24 clusters drive lipid-associated macrophage proliferation in obese adipose tissue.


ABSTRACT: Identifying molecular circuits that control adipose tissue macrophage (ATM) function is necessary to understand how ATMs contribute to tissue homeostasis and obesity-induced insulin resistance. In this study, we find that mice with a myeloid-specific knockout of the miR-23-27-24 clusters of microRNAs (miRNAs) gain less weight on a high-fat diet but exhibit worsened glucose and insulin tolerance. Analysis of ATMs from these mice shows selectively reduced numbers and proliferation of a recently reported subset of lipid-associated CD9+Trem2+ ATMs (lipid-associated macrophages [LAMs]). Leveraging the role of miRNAs to control networks of genes, we use RNA sequencing (RNA-seq), functional screens, and biochemical assays to identify candidate target transcripts that regulate proliferation-associated signaling. We determine that miR-23 directly targets the mRNA of Eif4ebp2, a gene that restricts protein synthesis and proliferation in macrophages. Altogether, our study demonstrates that control of proliferation of a protective subset of LAMs by noncoding RNAs contributes to protection against diet-induced obesity metabolic dysfunction.

SUBMITTER: Sprenkle NT 

PROVIDER: S-EPMC10712211 | biostudies-literature | 2023 Aug

REPOSITORIES: biostudies-literature

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The miR-23-27-24 clusters drive lipid-associated macrophage proliferation in obese adipose tissue.

Sprenkle Neil T NT   Winn Nathan C NC   Bunn Kaitlyn E KE   Zhao Yang Y   Park Deborah J DJ   Giese Brenna G BG   Karijolich John J JJ   Ansel K Mark KM   Serezani C Henrique CH   Hasty Alyssa H AH   Pua Heather H HH  

Cell reports 20230804 8


Identifying molecular circuits that control adipose tissue macrophage (ATM) function is necessary to understand how ATMs contribute to tissue homeostasis and obesity-induced insulin resistance. In this study, we find that mice with a myeloid-specific knockout of the miR-23-27-24 clusters of microRNAs (miRNAs) gain less weight on a high-fat diet but exhibit worsened glucose and insulin tolerance. Analysis of ATMs from these mice shows selectively reduced numbers and proliferation of a recently re  ...[more]

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