Frequent Mutation of <i>BAP1</i> in Metastasizing Uveal Melanomas

J. William Harbour; Michael D. Onken; Elisha Roberson; Shenghui Duan; Li Cao; Lori A. Worley; Katie A. Matatall; Cynthia Helms; A. Bowcock

doi:10.1126/science.1194472

Frequent Mutation of <i>BAP1</i> in Metastasizing Uveal Melanomas

J. William Harbour(Washington University in St. Louis), Michael D. Onken, Elisha Roberson(Washington University in St. Louis), Shenghui Duan(Washington University in St. Louis), Li Cao(Washington University in St. Louis), Lori A. Worley, Katie A. Matatall(Washington University in St. Louis), Cynthia Helms(Washington University in St. Louis), A. Bowcock(Washington University in St. Louis)

Science

November 4, 2010

10.1126/science.1194472

Cited by 1,487Open Access

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Abstract

Metastasis is a defining feature of malignant tumors and is the most common cause of cancer-related death, yet the genetics of metastasis are poorly understood. We used exome capture coupled with massively parallel sequencing to search for metastasis-related mutations in highly metastatic uveal melanomas of the eye. Inactivating somatic mutations were identified in the gene encoding BRCA1-associated protein 1 (BAP1) on chromosome 3p21.1 in 26 of 31 (84%) metastasizing tumors, including 15 mutations causing premature protein termination and 5 affecting its ubiquitin carboxyl-terminal hydrolase domain. One tumor harbored a frameshift mutation that was germline in origin, thus representing a susceptibility allele. These findings implicate loss of BAP1 in uveal melanoma metastasis and suggest that the BAP1 pathway may be a valuable therapeutic target.

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