Senolytic Combination of Dasatinib and Quercetin Alleviates Intestinal Senescence and Inflammation and Modulates the Gut Microbiome in Aged Mice

衰老 炎症 CXCL1型 生物 失调 微生物群 回肠 结肠炎 肠道菌群 免疫学 趋化因子 癌症研究 内分泌学 生物信息学 细胞生物学
作者
Tatiana D. Saccon,Ravinder Nagpal,Hariom Yadav,Marcelo Borges Cavalcante,Allancer Divino de Carvalho Nunes,Augusto Schneider,Adam Gesing,Brian M. Hughes,Matthew J. Yousefzadeh,Tamar Tchkonia,James L. Kirkland,Laura J. Niedernhofer,Paul D. Robbins,Michał M. Masternak
出处
期刊:The Journals of Gerontology [Oxford University Press]
卷期号:76 (11): 1895-1905 被引量:239
标识
DOI:10.1093/gerona/glab002
摘要

Cellular senescence contributes to age-related disorders including physical dysfunction, disabilities, and mortality caused by tissue inflammation and damage. Senescent cells accumulate in multiple tissues with aging and at etiological sites of multiple chronic disorders. The senolytic drug combination, Dasatinib plus Quercetin (D+Q), is known to reduce senescent cell abundance in aged mice. However, the effects of long-term D+Q treatment on intestinal senescent cell and inflammatory burden and microbiome composition in aged mice remain unknown. Here, we examine the effect of D+Q on senescence (p16Ink4a and p21Cip1) and inflammation (Cxcl1, Il1β, Il6, Mcp1, and Tnfα) markers in small (ileum) and large (caecum and colon) intestine in aged mice (n = 10) compared to age-matched placebo-treated mice (n = 10). Additionally, we examine microbial composition along the intestinal tract in these mice. D+Q-treated mice show significantly lower senescent cell (p16 and p21 expression) and inflammatory (Cxcl1, Il1β, Il6, Mcp1, and Tnfα expression) burden in small and large intestine compared with control mice. Further, we find specific microbial signatures in ileal, cecal, colonic, and fecal regions that are distinctly modulated by D+Q, with modulation being most prominent in small intestine. Further analyses reveal specific correlation of senescence and inflammation markers with specific microbial signatures. Together, these data demonstrate that the senolytic treatment reduces intestinal senescence and inflammation while altering specific microbiota signatures and suggest that the optimized senolytic regimens might improve health via reducing intestinal senescence, inflammation, and microbial dysbiosis in older subjects.
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