Integrative molecular characterization of sarcomatoid and rhabdoid renal cell carcinoma
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Published:2021-02-05
Issue:1
Volume:12
Page:
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ISSN:2041-1723
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Container-title:Nature Communications
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language:en
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Short-container-title:Nat Commun
Author:
Bakouny ZiadORCID, Braun David A.ORCID, Shukla Sachet A.ORCID, Pan Wenting, Gao Xin, Hou Yue, Flaifel Abdallah, Tang StephenORCID, Bosma-Moody Alice, He Meng Xiao, Vokes NatalieORCID, Nyman Jackson, Xie Wanling, Nassar Amin H.ORCID, Abou Alaiwi SarahORCID, Flippot Ronan, Bouchard Gabrielle, Steinharter John A., Nuzzo Pier VitaleORCID, Ficial MiriamORCID, Sant’Angelo Miriam, Forman Juliet, Berchuck Jacob E.ORCID, Dudani Shaan, Bi Kevin, Park Jihye, Camp Sabrina, Sticco-Ivins Maura, Hirsch Laure, Baca Sylvan C., Wind-Rotolo Megan, Ross-Macdonald Petra, Sun Maxine, Lee Gwo-Shu Mary, Chang Steven L., Wei Xiao X., McGregor Bradley A., Harshman Lauren C., Genovese Giannicola, Ellis LeighORCID, Pomerantz Mark, Hirsch Michelle S., Freedman Matthew L., Atkins Michael B., Wu Catherine J.ORCID, Ho Thai H.ORCID, Linehan W. MarstonORCID, McDermott David F.ORCID, Heng Daniel Y. C., Viswanathan Srinivas R.ORCID, Signoretti Sabina, Van Allen Eliezer M.ORCID, Choueiri Toni K.ORCID
Abstract
AbstractSarcomatoid and rhabdoid (S/R) renal cell carcinoma (RCC) are highly aggressive tumors with limited molecular and clinical characterization. Emerging evidence suggests immune checkpoint inhibitors (ICI) are particularly effective for these tumors, although the biological basis for this property is largely unknown. Here, we evaluate multiple clinical trial and real-world cohorts of S/R RCC to characterize their molecular features, clinical outcomes, and immunologic characteristics. We find that S/R RCC tumors harbor distinctive molecular features that may account for their aggressive behavior, including BAP1 mutations, CDKN2A deletions, and increased expression of MYC transcriptional programs. We show that these tumors are highly responsive to ICI and that they exhibit an immune-inflamed phenotype characterized by immune activation, increased cytotoxic immune infiltration, upregulation of antigen presentation machinery genes, and PD-L1 expression. Our findings build on prior work and shed light on the molecular drivers of aggressivity and responsiveness to ICI of S/R RCC.
Funder
United States Department of Defense | United States Army | Army Medical Command | Congressionally Directed Medical Research Programs Bristol-Myers Squibb U.S. Department of Health & Human Services | NIH | National Cancer Institute Fondation ARC pour la Recherche sur le Cancer Kidney Cancer Association
Publisher
Springer Science and Business Media LLC
Subject
General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry
Reference78 articles.
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