A Glance into the Destiny of Transcriptomic Activity, Embodied by the HOX Genes, in Neonatal and Aging Dermal Cells

Hox基因 生物 转录组 基因 遗传学 人体皮肤 细胞生物学 皮肤老化 转录因子 基因表达 医学 皮肤病科
作者
Doyeong Ko,Seyoung Mun,Minji Kim,Youn Hwa Nho,Dong‐Geol Lee,Seunghyun Kang,Kyudong Han,Mi‐Sun Kim
出处
期刊:Advanced biology [Wiley]
卷期号:8 (4) 被引量:2
标识
DOI:10.1002/adbi.202300325
摘要

Abstract Skin is an organ having a crucial role in the protection of muscle, bone, and internal organs and undergoing continuous self‐renewal and aged. The growing interest in the prevention of skin aging and rejuvenation has sparked a surge of industrial and research studies focusing on the biological and transcriptional changes that occur during skin development and aging. In this study, the aim is to identify transcriptional differences between two main types of human skin cells: the human dermal fibroblasts (HDFs) and the human epidermis keratinocytes (HEKs) isolated from 30 neonatal and 30 adults (old) skin. Through differentially expressed gene (DEG) profiling using DEseq2, 604 up‐, and 769 down‐regulated genes are identified in the old group. A functional analysis using Metascape Gene Ontology and Reactome pathways revealed systematic transcriptomic shifts in key skin formation and maintenance markers, alongside a distinct difference in HOX gene families crucial for embryonic development and diverse biological processes. Among the 39 human HOX gene family, ten posterior HOX genes ( HOXA10 , 11 , 13 , HOXB13 , HOXC11 , and HOXD9 ‐ 13 ) are significantly downregulated, and anterior 25 genes ( HOXA2 ‐ 7 , HOXB1 ‐ 9 , HOXC4 ‐ 6 and 8 – 9 , and HOXD1 , 3 , 4 and 8 ) are upregulated, especially in the old HDFs. The study successfully demonstrates the correlation between HOX genes and the skin aging process, providing strong evidence that HOX genes are proposed as a new marker for skin aging assessment.
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