| Literature DB >> 33238152 |
Zhiran Zou1, Xiao Long2, Qian Zhao3, Yandong Zheng4, Moshi Song5, Shuai Ma6, Yaobin Jing1, Si Wang7, Yifang He1, Concepcion Rodriguez Esteban8, Nanze Yu2, Jiuzuo Huang2, Piu Chan3, Ting Chen9, Juan Carlos Izpisua Belmonte8, Weiqi Zhang10, Jing Qu11, Guang-Hui Liu12.
Abstract
Skin undergoes constant self-renewal, and its functional decline is a visible consequence of aging. Understanding human skin aging requires in-depth knowledge of the molecular and functional properties of various skin cell types. We performed single-cell RNA sequencing of human eyelid skin from healthy individuals across different ages and identified eleven canonical cell types, as well as six subpopulations of basal cells. Further analysis revealed progressive accumulation of photoaging-related changes and increased chronic inflammation with age. Transcriptional factors involved in the developmental process underwent early-onset decline during aging. Furthermore, inhibition of key transcription factors HES1 in fibroblasts and KLF6 in keratinocytes not only compromised cell proliferation, but also increased inflammation and cellular senescence during aging. Lastly, we found that genetic activation of HES1 or pharmacological treatment with quercetin alleviated cellular senescence of dermal fibroblasts. These findings provide a single-cell molecular framework of human skin aging, providing a rich resource for developing therapeutic strategies against aging-related skin disorders.Entities:
Keywords: HES1; KLF6; aging; fibroblast; keratinocyte; quercetin; senescence; single-cell RNA sequencing; skin
Year: 2020 PMID: 33238152 DOI: 10.1016/j.devcel.2020.11.002
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270