Targeting Dysregulated Phago-/auto-lysosomes in Sertoli Cells to Ameliorate Late-onset Hypogonadism

Overview

Journal Nat Aging

Specialty Geriatrics

Date 2024 Apr 22

PMID 38649614

Authors

Zhiwen Deng

Liangyu Zhao

Sha Li

Xiaoyang Chen

Xiaohan Ling

Jiajun Zheng

Kunkun Yu

Jing Xu

Chencheng Yao

Sha Han

Jiayi Liang

Huimin Feng

Lanlan Wu

Peng Li

Ruhui Tian

Tao Jing

Yuxin Tang

Yingbo Dai

Minbo Yan

Chenchen Wang

Zheng Li

Zhi Zhou

Affiliations

Soon will be listed here.

Abstract

Age-related changes in testicular function can impact health and well-being. The mechanisms underlying age-related testicular dysfunction, such as late-onset hypogonadism (LOH), remain incompletely understood. Using single-cell RNA sequencing on human testes with LOH, we delineated Sertoli cells (SCs) as pivotal metabolic coordinators within the testicular microenvironment. In particular, lysosomal acidity probing revealed compromised degradative capacity in aged SCs, hindering autophagy and phagocytic flux. Consequently, SCs accumulated metabolites, including cholesterol, and have increased inflammatory gene expression; thus, we termed these cells as phago-/auto-lysosomal deregulated SCs. Exposure to a high-fat diet-induced phago-/auto-lysosomal dysregulated-like SCs, recapitulating LOH features in mice. Notably, efferent ductular injection and systemic TRPML1 agonist administration restored lysosomal function, normalizing testosterone deficiency and associated abnormalities in high-fat diet-induced LOH mice. Our findings underscore the central role of SCs in testis aging, presenting a promising therapeutic avenue for LOH.

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