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Single-Cell Transcriptomic Profiling of the Hypothalamic Median Eminence During Aging
Zhen-Hua Chen, Si Li, Mingrui Xu, Candace C. Liu, Hongying Ye, Ben Wang, Qing-Feng Wu
Journal of Genetics and Genomics
Abstract
Aging is a slow and progressive natural process that compromises the normal functions of cells, tissues, organs and systems. The aging of the hypothalamic median eminence (ME), a structural gate linking neural and endocrine systems, may impair hormone release, energy homeostasis and central sensing of circulating molecules, leading to systemic and reproductive aging. However, the molecular and cellular features of ME aging remain largely unknown. Here we describe the transcriptional landscape of young and middle-aged mouse ME at single-cell resolution, revealing the common and cell-type-specific transcriptional changes with age. The transcriptional changes in cell-intrinsic programs, cell-cell crosstalk and cell-extrinsic factors highlight five molecular features of ME aging and also implicate several potentially druggable targets at cellular, signaling and molecular levels.
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DOI:10.1016/j.jgg.2022.01.001 |
论文题目: |
Single-Cell Transcriptomic Profiling of the Hypothalamic Median Eminence During Aging |
英文论文题目: |
Single-Cell Transcriptomic Profiling of the Hypothalamic Median Eminence During Aging |
第一作者: |
Zhen-Hua Chen, Si Li, Mingrui Xu, Candace C. Liu, Hongying Ye, Ben Wang, Qing-Feng Wu |
英文第一作者: |
Zhen-Hua Chen, Si Li, Mingrui Xu, Candace C. Liu, Hongying Ye, Ben Wang, Qing-Feng Wu |
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2022-01-19 |
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Aging is a slow and progressive natural process that compromises the normal functions of cells, tissues, organs and systems. The aging of the hypothalamic median eminence (ME), a structural gate linking neural and endocrine systems, may impair hormone release, energy homeostasis and central sensing of circulating molecules, leading to systemic and reproductive aging. However, the molecular and cellular features of ME aging remain largely unknown. Here we describe the transcriptional landscape of young and middle-aged mouse ME at single-cell resolution, revealing the common and cell-type-specific transcriptional changes with age. The transcriptional changes in cell-intrinsic programs, cell-cell crosstalk and cell-extrinsic factors highlight five molecular features of ME aging and also implicate several potentially druggable targets at cellular, signaling and molecular levels. |
英文摘要: |
Aging is a slow and progressive natural process that compromises the normal functions of cells, tissues, organs and systems. The aging of the hypothalamic median eminence (ME), a structural gate linking neural and endocrine systems, may impair hormone release, energy homeostasis and central sensing of circulating molecules, leading to systemic and reproductive aging. However, the molecular and cellular features of ME aging remain largely unknown. Here we describe the transcriptional landscape of young and middle-aged mouse ME at single-cell resolution, revealing the common and cell-type-specific transcriptional changes with age. The transcriptional changes in cell-intrinsic programs, cell-cell crosstalk and cell-extrinsic factors highlight five molecular features of ME aging and also implicate several potentially druggable targets at cellular, signaling and molecular levels. |
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Journal of Genetics and Genomics |
英文刊物名称: |
Journal of Genetics and Genomics |
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Zhen-Hua Chen, Si Li, Mingrui Xu, Candace C. Liu, Hongying Ye, Ben Wang, Qing-Feng Wu. Single-Cell Transcriptomic Profiling of the Hypothalamic Median Eminence During Aging. Journal of Genetics and Genomics. DOI:10.1016/j.jgg.2022.01.001 |
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