A mutational process signature and genomic alterations associated with outcome and immunogenicity in cancers with brain metastasis
Wanli Sun, Xueying Wang, Yixin Xu, Yanfeng Ren, Wenjing Zhang, Qinghua Wang, Yingzhi Chong

TL;DR
This study identifies genetic markers linked to survival and immunotherapy response in cancer patients with brain metastasis.
Contribution
The study introduces a mutational process signature and genomic alterations associated with prognosis and immunogenicity in brain metastasis.
Findings
A C > T mutation signature linked to DNA damage repair correlates with worse outcomes and lower tumor mutation burden.
PTPRT mutation is associated with improved prognosis and better immunotherapy response in brain metastasis patients.
PTEN deletion is linked to poorer outcomes, while DUSP4 deletion is associated with better outcomes in BM patients.
Abstract
Brain metastasis (BM) is one of the common ways of tumor metastasis and has a poor prognosis. This study aims to identify potential biomarkers from the perspective of somatic mutations, providing a basis for the prognosis evaluation and immunogenicity prediction of BM patients. This study collected the somatic mutation profiles and clinical information of a total of 421 patients with BM in Memorial Sloan Kettering Cancer Center (MSKCC). Non-negative matrix factorization was employed to extract the mutational process signatures operating in the genome. Consensus clustering analysis was utilized to identify mutation-related molecular subtypes. Through a comprehensive analysis of genomic mutations and copy number variations (CNV), biomarkers associated with outcomes and tumor immunogenicity were screened. Non-small cell lung cancer, melanoma, and breast cancer were common primary tumors…
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Taxonomy
TopicsBrain Metastases and Treatment · Lung Cancer Treatments and Mutations · Cancer Immunotherapy and Biomarkers
