| Literature DB >> 33446552 |
Takehiro Yamanaka1, Satotaka Omori1, Teh-Wei Wang1, Yoshikazu Johmura2, Yuki Sugiura3, Masaki Matsumoto4, Narumi Suzuki1, Soichiro Kumamoto1, Kiyoshi Yamaguchi5, Seira Hatakeyama5, Tomoyo Takami4, Rui Yamaguchi6, Eigo Shimizu6, Kazutaka Ikeda7, Nobuyuki Okahashi7, Ryuta Mikawa8, Makoto Suematsu3, Makoto Arita7,9, Masataka Sugimoto8, Keiichi I Nakayama4, Yoichi Furukawa5, Seiya Imoto10, Makoto Nakanishi2.
Abstract
Removal of senescent cells (senolysis) has been proposed to be beneficial for improving age-associated pathologies, but the molecular pathways for such senolytic activity have not yet emerged. Here, we identified glutaminase 1 (GLS1) as an essential gene for the survival of human senescent cells. The intracellular pH in senescent cells was lowered by lysosomal membrane damage, and this lowered pH induced kidney-type glutaminase (KGA) expression. The resulting enhanced glutaminolysis induced ammonia production, which neutralized the lower pH and improved survival of the senescent cells. Inhibition of KGA-dependent glutaminolysis in aged mice eliminated senescent cells specifically and ameliorated age-associated organ dysfunction. Our results suggest that senescent cells rely on glutaminolysis, and its inhibition offers a promising strategy for inducing senolysis in vivo.Entities:
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Year: 2021 PMID: 33446552 DOI: 10.1126/science.abb5916
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728