Astrocytic trans-Differentiation Completes a Multicellular Paracrine Feedback Loop Required for Medulloblastoma Tumor Growth

星形胶质细胞的跨分化完成了髓母细胞瘤肿瘤生长所需的多细胞旁分泌反馈回路

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作者:Maojin Yao, P Britten Ventura, Ying Jiang, Fausto J Rodriguez, Lixin Wang, Justin S A Perry, Yibo Yang, Kelsey Wahl, Rowena B Crittenden, Mariko L Bennett, Lin Qi, Cong-Cong Gong, Xiao-Nan Li, Ben A Barres, Timothy P Bender, Kodi S Ravichandran, Kevin A Janes, Charles G Eberhart, Hui Zong

Abstract

The tumor microenvironment (TME) is critical for tumor progression. However, the establishment and function of the TME remain obscure because of its complex cellular composition. Using a mouse genetic system called mosaic analysis with double markers (MADMs), we delineated TME evolution at single-cell resolution in sonic hedgehog (SHH)-activated medulloblastomas that originate from unipotent granule neuron progenitors in the brain. First, we found that astrocytes within the TME (TuAstrocytes) were trans-differentiated from tumor granule neuron precursors (GNPs), which normally never differentiate into astrocytes. Second, we identified that TME-derived IGF1 promotes tumor progression. Third, we uncovered that insulin-like growth factor 1 (IGF1) is produced by tumor-associated microglia in response to interleukin-4 (IL-4) stimulation. Finally, we found that IL-4 is secreted by TuAstrocytes. Collectively, our studies reveal an evolutionary process that produces a multi-lateral network within the TME of medulloblastoma: a fraction of tumor cells trans-differentiate into TuAstrocytes, which, in turn, produce IL-4 that stimulates microglia to produce IGF1 to promote tumor progression.

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