Proteome Profiling Uncovers an Autoimmune Response Signature That Reflects Ovarian Cancer Pathogenesis

Author:

Kobayashi MakotoORCID,Katayama HiroyukiORCID,Irajizad Ehsan,Vykoukal Jody V.,Fahrmann Johannes F.,Kundnani Deepali L.ORCID,Yu Chuan-YihORCID,Cai Yining,Hsiao Fu Chung,Yang Wei-LeiORCID,Lu Zhen,Celestino Joseph,Long James P.,Do Kim-Ann,Lu Karen H.,Ladd Jon J.,Urban Nicole,Bast Jr. Robert C.ORCID,Hanash Samir M.

Abstract

Harnessing the immune response to tumor antigens in the form of autoantibodies, which occurs early during tumor development, has relevance to the detection of cancer at early stages. We conducted an initial screen of antigens associated with an autoantibody response in serous ovarian cancer using recombinant protein arrays. The top 25 recombinants that exhibited increased reactivity with cases compared to controls revealed TP53 and MYC, which are ovarian cancer driver genes, as major network nodes. A mass spectrometry based independent analysis of circulating immunoglobulin (Ig)-bound proteins in ovarian cancer and of ovarian cancer cell surface MHC-II bound peptides also revealed a TP53–MYC related network of antigens. Our findings support the occurrence of a humoral immune response to antigens linked to ovarian cancer driver genes that may have utility for early detection applications.

Funder

Cancer Prevention and Research Institute of Texas

University of Texas MD Anderson Cancer Center

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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