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miR‐125a‐5p increases cellular DNA damage of aging males and perturbs stage‐specific embryo development via Rbm38‐p53 signaling

Kuan Liang, Liangyu Yao, Shuxian Wang, Lu Zheng, Qian Zhang, Yi‐Feng Ge, Li Chen, Xi Cheng, Rujun Ma, Chuwei Li, Jun Jing, Yang Yang, Wanwan Yu, Tongmin Xue, Qiwei Chen, Siyuan Cao, Jinzhao Ma, Bing Yao

2021Aging Cell22 citationsDOIOpen Access PDF

Abstract

An increasing number of men are fathering children at an older age than in the past. While advanced maternal age has long been recognized as a risk factor for adverse reproductive outcomes, the influence of paternal age on reproduction is incompletely comprehended. Herein, we found that miR-125a-5p was upregulated in the sperm of aging males and was related to inferior sperm DNA integrity as an adverse predictor. Moreover, we demonstrated that miR-125a-5p suppressed mitochondrial function and increased cellular DNA damage in GC2 cells. We also found that miR-125a-5p perturbed embryo development at specific morula/blastocyst stages. Mechanistically, we confirmed that miR-125a-5p disturbed the mitochondrial function by targeting Rbm38 and activating the p53 damage response pathway, and induced a developmental delay in a p21-dependent manner. Our study revealed an important role of miR-125a-5p in sperm function and early embryo development of aging males, and provided a fresh view to comprehend the aging process in sperm.

Topics & Concepts

BiologyEmbryoSpermDNA damageCell biologyBlastocystMitochondrionSenescenceEmbryogenesisDownregulation and upregulationMitochondrial DNAAndrologyGeneticsDNAGeneMedicineMicroRNA in disease regulationReproductive Biology and FertilityRNA Research and Splicing
miR‐125a‐5p increases cellular DNA damage of aging males and perturbs stage‐specific embryo development via Rbm38‐p53 signaling | Litcius