Deficient Mice Exhibit Premature Aging and Metabolic Perturbations in Adipocytes

Overview

Journal iScience

Publisher Cell Press

Date 2022 Oct 3

PMID 36185376

Authors

Aurore De Cauwer

Thomas Loustau

William Erne

Angelique Pichot

Anne Molitor

Tristan Stemmelen

Raphael Carapito

Gertraud Orend

Seiamak Bahram

Philippe Georgel

Affiliations

Soon will be listed here.

Abstract

Age-related diseases are major concern in developed countries. To avoid disabilities that accompany increased lifespan, pharmaceutical approaches are considered. Therefore, appropriate animal models are required for a better understanding of aging processes and potential assays to evaluate the impact of molecules that may delay the occurrence of age-related diseases. Few mouse models exhibiting pathological aging exist, but currently, none of them reproducibly mimics human diseases like osteoporosis, cognitive dysfunctions or sarcopenia that can be seen in some, but not all, elders. Here, we describe the premature aging phenotypes of Dicer-deficient mature animals, which exhibit an overall deterioration of many organs and tissues (skin, heart, and adipose tissue) ultimately leading to a significant reduction of their lifespan. Molecular characterization of transcriptional responses focused on the adipose tissue suggested that both canonical and non-canonical functions of DICER are involved in this process and highlight potential actionable pathways to revert it.

Citing Articles

MicroRNA biogenesis pathway alterations in aging.

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PMID: 39698023 PMC: 11648461. DOI: 10.20517/evcna.2023.29.

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