Discovery of Stromal Regulatory Networks that Suppress Ras-Sensitized Epithelial Cell Proliferation

发现抑制Ras敏感上皮细胞增殖的基质调控网络

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作者:Huayang Liu ,James A Dowdle ,Safiya Khurshid ,Nicholas J Sullivan ,Nicholas Bertos ,Komal Rambani ,Markus Mair ,Piotr Daniel ,Esther Wheeler ,Xing Tang ,Kyle Toth ,Michael Lause ,Markus E Harrigan ,Karl Eiring ,Connor Sullivan ,Matthew J Sullivan ,Serena W Chang ,Siddhant Srivastava ,Joseph S Conway ,Raleigh Kladney ,Joseph McElroy ,Sooin Bae ,Yuanzhi Lu ,Ali Tofigh ,Sadiq M I Saleh ,Soledad A Fernandez ,Jeffrey D Parvin ,Vincenzo Coppola ,Erin R Macrae ,Sarmila Majumder ,Charles L Shapiro ,Lisa D Yee ,Bhuvaneswari Ramaswamy ,Michael Hallett ,Michael C Ostrowski ,Morag Park ,Helen M Chamberlin ,Gustavo Leone

Abstract

Mesodermal cells signal to neighboring epithelial cells to modulate their proliferation in both normal and disease states. We adapted a Caenorhabditis elegans organogenesis model to enable a genome-wide mesodermal-specific RNAi screen and discovered 39 factors in mesodermal cells that suppress the proliferation of adjacent Ras pathway-sensitized epithelial cells. These candidates encode components of protein complexes and signaling pathways that converge on the control of chromatin dynamics, cytoplasmic polyadenylation, and translation. Stromal fibroblast-specific deletion of mouse orthologs of several candidates resulted in the hyper-proliferation of mammary gland epithelium. Furthermore, a 33-gene signature of human orthologs was selectively enriched in the tumor stroma of breast cancer patients, and depletion of these factors from normal human breast fibroblasts increased proliferation of co-cultured breast cancer cells. This cross-species approach identified unanticipated regulatory networks in mesodermal cells with growth-suppressive function, exposing the conserved and selective nature of mesodermal-epithelial communication in development and cancer. Keywords: Caenorhabditis elegans vulva development; Sympk; Tlk1/2; breast cancer; chromatin dynamics; cytoplasmic polyadenylation; mesodermal-epithelial communication; stromal regulatory networks; translation control; tumor microenvironment.

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