| Literature DB >> 33232280 |
Yixuan Fang1,2,3,4, Yue Gu1,2, Lei Li1,2, Lingjiang Zhu1,2, Jiawei Qian1, Chen Zhao1,2, Li Xu1,2, Wen Wei1,2, Yanhua Du5, Na Yuan1,2,3,4, Suping Zhang1,2,3,4, Ye Yuan6, Youjia Xu6, Cizhong Jiang5, Jianrong Wang1,2,3,4.
Abstract
Atg7, a critical component of autophagy machinery, is essential for counteracting hematopoietic aging. However, the non-autophagic role of Atg7 on hematopoietic cells remains fundamentally unclear. In this study, we found that loss of Atg7, but not Atg5, another autophagy-essential gene, in the hematopoietic system reduces CD11b myeloid cellularity including CD11b+Ly6G+ and CD11b+Ly6G- populations in mouse bone marrow. Surprisingly, Atg7 deletion causes abnormally accumulated histone H3.1 to be overwhelmingly trapped in the cytoplasm in the CD11b+Ly6G-, but not the CD11b+Ly6G+ compartment. RNA profiling revealed extensively chaotic expression of the genes required in nucleosome assembly. Functional assays further indicated upregulated aging markers in the CD11b+Ly6G- population. Therefore, our study suggests that Atg7 is essential for maintaining proper nucleosome assembly and limiting aging in the bone marrow CD11b+Ly6G- population.Entities:
Keywords: Atg7; aging; histone H3.1; nucleosome assembly
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Year: 2020 PMID: 33232280 PMCID: PMC7803583 DOI: 10.18632/aging.104176
Source DB: PubMed Journal: Aging (Albany NY) ISSN: 1945-4589 Impact factor: 5.682