Single-cell transcriptomic atlas of taste papilla aging

IF 7.8 1区 医学 Q1 Biochemistry, Genetics and Molecular Biology
Aging Cell Pub Date : 2024-08-21 DOI:10.1111/acel.14308
Wenwen Ren, Weihao Li, Xudong Cha, Shenglei Wang, Boyu Cai, Tianyu Wang, Fengzhen Li, Tengfei Li, Yingqi Xie, Zengyi Xu, Zhe Wang, Huanhai Liu, Yiqun Yu
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Abstract

Taste perception is one of the important senses in mammals. Taste dysfunction causes significant inconvenience in daily life, leading to subhealth and even life-threatening condition. Aging is a major cause to taste dysfunction, while the underlying feature related to gustatory aging is still not known. Using single-cell RNA Sequencing, differentially expressed genes between aged and young taste papillae are identified, including upregulated mt-Nd4l and Xist, as well as downregulated Hsp90ab1 and Tmem59. In the Tmem59−/− circumvallate papillae (CVP), taste mature cell generation is impaired by reduction in the numbers of PLCβ2+ and Car4+ cells, as well as decreases in expression levels of taste transduction genes. Tmem59−/− mice showed deficits in sensitivities to tastants. Through screening by GenAge and DisGeNET databases, aging-dependent genes and oral disease-associated genes are identified in taste papillae. In the CVP, aging promotes intercellular communication reciprocally between (cycling) basal cell and mature taste cell by upregulated Crlf1/Lifr and Adam15/Itga5 signaling. By transcriptional network analysis, ribosome proteins, Anxa1, Prdx5, and Hmgb1/2 are identified as transcriptional hubs in the aged taste papillae. Chronological aging-associated transcriptional changes throughout taste cell maturation are revealed. Aged taste papillae contain more Muc5b+ cells that are not localized in gustatory gland. Collectively, this study shows molecular and cellular features associated with taste papilla aging.

Abstract Image

Abstract Image

味乳头老化的单细胞转录组图谱
味觉是哺乳动物的重要感官之一。味觉功能障碍会给日常生活带来极大不便,导致亚健康,甚至危及生命。衰老是味觉功能障碍的一个主要原因,而与味觉衰老相关的潜在特征仍不清楚。利用单细胞 RNA 测序技术,发现了老年和年轻味觉乳头之间的差异表达基因,包括上调的 mt-Nd4l 和 Xist,以及下调的 Hsp90ab1 和 Tmem59。在Tmem59-/-环卵乳头(CVP)中,由于PLCβ2+和Car4+细胞数量的减少以及味觉传导基因表达水平的下降,味觉成熟细胞的生成受到了影响。Tmem59-/- 小鼠对味觉刺激物的敏感性表现出缺陷。通过 GenAge 和 DisGeNET 数据库的筛选,在味觉乳头中发现了衰老依赖基因和口腔疾病相关基因。在CVP中,衰老通过上调Crlf1/Lifr和Adam15/Itga5信号,促进(循环)基底细胞和成熟味觉细胞之间的细胞间交流。通过转录网络分析,核糖体蛋白、Anxa1、Prdx5和Hmgb1/2被确定为老化味觉乳头的转录枢纽。研究揭示了整个味觉细胞成熟过程中与衰老相关的转录变化。衰老的味乳头含有更多的 Muc5b+ 细胞,而这些细胞在味腺中没有定位。总之,这项研究显示了与味乳头老化相关的分子和细胞特征。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Aging Cell
Aging Cell 生物-老年医学
CiteScore
14.40
自引率
2.60%
发文量
212
审稿时长
8 weeks
期刊介绍: Aging Cell, an Open Access journal, delves into fundamental aspects of aging biology. It comprehensively explores geroscience, emphasizing research on the mechanisms underlying the aging process and the connections between aging and age-related diseases.
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