Cancer-associated fibroblast subtypes modulate the tumor-immune microenvironment and are associated with skin cancer malignancy

癌症相关成纤维细胞亚型调节肿瘤免疫微环境,并与皮肤癌恶性程度相关。

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作者:Agnes Forsthuber #,Bertram Aschenbrenner #,Ana Korosec #,Tina Jacob,Karl Annusver,Natalia Krajic,Daria Kholodniuk,Sophie Frech,Shaohua Zhu,Kim Purkhauser,Katharina Lipp,Franziska Werner,Vy Nguyen,Johannes Griss,Wolfgang Bauer,Ana Soler Cardona,Benedikt Weber,Wolfgang Weninger,Bernhard Gesslbauer,Clement Staud,Jakob Nedomansky,Christine Radtke,Stephan N Wagner,Peter Petzelbauer,Maria Kasper,Beate M Lichtenberger

Abstract

Cancer-associated fibroblasts (CAFs) play a key role in cancer progression and treatment outcome. This study dissects the intra-tumoral diversity of CAFs in basal cell carcinoma, squamous cell carcinoma, and melanoma using molecular and spatial single-cell analysis. We identify three distinct CAF subtypes: myofibroblast-like RGS5+ CAFs, matrix CAFs (mCAFs), and immunomodulatory CAFs (iCAFs). Large-cohort tissue analysis reveals significant shifts in CAF subtype patterns with increasing malignancy. Two CAF subtypes exhibit immunomodulatory properties via different mechanisms. mCAFs sythesize extracellular matrix and may restrict T cell invasion in low-grade tumors via ensheathing tumor nests, while iCAFs are enriched in late-stage tumors, and express high levels of cytokines and chemokines to aid immune cell recruitment and activation. This is supported by the induction of an iCAF-like phenotype with immunomodulatory functions in primary healthy fibroblasts exposed to skin cancer cell secretomes. Thus, targeting CAF variants holds promise to enhance immunotherapy efficacy in skin cancers.

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