detalle del documento
IDENTIFICACIÓN

doi:10.1038/s41419-024-06637-2...

Autor
Li, Jiyong Ma, Rongze Wang, Xuebing Lu, Yunzhe Chen, Jing Feng, Deyi Zhou, Jiecan Xia, Kun Klein, Ophir Xie, Hao Lu, Pengfei
Langue
en
Editor

Nature

Categoría

Life Sciences

Año

2024

fecha de cotización

17/4/2024

Palabras clave
activated spry mammary development genes fibroblasts cancer
Métrico

Resumen

Stromal fibroblasts are a major stem cell niche component essential for organ formation and cancer development.

Fibroblast heterogeneity, as revealed by recent advances in single-cell techniques, has raised important questions about the origin, differentiation, and function of fibroblast subtypes.

In this study, we show in mammary stromal fibroblasts that loss of the receptor tyrosine kinase (RTK) negative feedback regulators encoded by Spry1 , Spry2 , and Spry4 causes upregulation of signaling in multiple RTK pathways and increased extracellular matrix remodeling, resulting in accelerated epithelial branching.

Single-cell transcriptomic analysis demonstrated that increased production of FGF10 due to Sprouty ( Spry ) loss results from expansion of a functionally distinct subgroup of fibroblasts with the most potent branching-promoting ability.

Compared to their three independent lineage precursors, fibroblasts in this subgroup are “activated,” as they are located immediately adjacent to the epithelium that is actively undergoing branching and invasion.

Spry genes are downregulated, and activated fibroblasts are expanded, in all three of the major human breast cancer subtypes.

Together, our data highlight the regulation of a functional subtype of mammary fibroblasts by Spry genes and their essential role in epithelial morphogenesis and cancer development.

Li, Jiyong,Ma, Rongze,Wang, Xuebing,Lu, Yunzhe,Chen, Jing,Feng, Deyi,Zhou, Jiecan,Xia, Kun,Klein, Ophir,Xie, Hao,Lu, Pengfei, 2024, Sprouty genes regulate activated fibroblasts in mammary epithelial development and breast cancer, Nature

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