Comprehensive Molecular Characterization Identifies Distinct Genomic and Immune Hallmarks of Renal Medullary Carcinoma

Pavlos Msaouel,Hui Yao,Riyad N.H Seervai,Selvi Kunnimalaiyaan,Melinda Soeung,Katharina Schlacher,Jorge Blando,Ignacio I Wistuba,Asha S Multani,Priya Rao,Jianjun Gao,Sanjana Srinivasan,Federica Carbone,Alessandro Carugo,Timothy C Thompson,Patrick G Pilié,Daniel D Shapiro,Jose A Karam,Chad J Creighton,Christopher G Wood,Nizar M Tannir,Cristian Coarfa,Xiaoping Su,Virginia Giuliani,Padmanee Sharma,Rong He,Luigi Perelli,Ximing Tang,Irwin Davidson,Gabriel G Malouf,Menuka Karki,Timothy P Heffernan,Cheryl L Walker,Giannicola Genovese,Emily H Cheng,Durga Nand Tripathi ,Wei Lü ,Jean‐Philippe Bertocchio ,Bujamin Vokshi ,Dolores López‐Terrada

doi:10.1016/j.ccell.2020.04.002

Abstract

Renal medullary carcinoma (RMC) is a highly lethal malignancy that mainly afflicts young individuals of African descent and is resistant to all targeted agents used to treat other renal cell carcinomas. Comprehensive genomic and transcriptomic profiling of untreated primary RMC tissues was performed to elucidate the molecular landscape of these tumors. We found that RMC was characterized by high replication stress and an abundance of focal copy-number alterations associated with activation of the stimulator of the cyclic GMP-AMP synthase interferon genes (cGAS-STING) innate immune pathway. Replication stress conferred a therapeutic vulnerability to drugs targeting DNA-damage repair pathways. Elucidation of these previously unknown RMC hallmarks paves the way to new clinical trials for this rare but highly lethal malignancy.

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