Data from Exome Sequencing Reveals a Sparse Genomic Landscape in Kaposi Sarcoma

外显子组测序 外显子组 计算生物学 肉瘤 生物 医学 遗传学 基因 突变 病理
作者
Warren Phipps,Bhavneet Bhinder,Andrea Towlerton,Peter Mooka,James Kafeero,Matthew Fitzgibbon,Olivier Elemento,Ethel Cesarman
标识
DOI:10.1158/1541-7786.c.7798958
摘要

<div>Abstract<p>Kaposi sarcoma is a frequently aggressive malignancy caused by Kaposi sarcoma herpesvirus. People with immunodeficiencies, including human immunodeficiency virus (HIV), are at increased risk for developing Kaposi sarcoma, but our understanding of the contributions of the cellular genome to Kaposi sarcoma pathogenesis remains limited. To determine if there are cellular genetic alterations in Kaposi sarcoma that might provide biological or therapeutic insights, we performed whole-exome sequencing on 78 Kaposi sarcoma tumors and matched normal control skin from 59 adults with Kaposi sarcoma (46 with HIV-associated Kaposi sarcoma and 13 with HIV-negative Kaposi sarcoma) receiving treatment at the Uganda Cancer Institute in Kampala, Uganda. We found a very low mutational burden in all but one specimen (median = 11 mutations), which is the lowest number of mutations among all 33 tumor types in The Cancer Genome Atlas. No recurrent mutations were seen, and the most commonly affected oncogenic pathway was RTK/RAS. Mutational signatures included defective DNA mismatch repair and smoking. There was no evidence suggesting that multiple tumors from the same patient originated from the same original clone. The number of genome copy alterations per genome was higher in tumors from those without HIV infection and in tumors from participants with advanced stage disease, suggesting that lesions that take longer to develop may accumulate more alterations, although the number of alterations remains low compared with other cancers.</p><p><b>Implications:</b> Our findings indicate that the pathogenesis of Kaposi sarcoma differs from other malignancies and that the primary driver of carcinogenesis is Kaposi sarcoma–associated herpesvirus infection and expression of viral oncogenes, rather than clonal oncogenic transformation.</p></div>

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