Identification of Novel FAM134B (JK1) Mutations in Oesophageal Squamous Cell Carcinoma

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作者
Md. Hakimul Haque
Vinod Gopalan
Kwok-wah Chan
Muhammad J. A. Shiddiky
Robert Anthony Smith
Alfred King-yin Lam
机构
[1] Cancer Molecular Pathology in Menzies Health Institute Queensland,Department of Pathology
[2] Griffith University,undefined
[3] Li Ka Shing Faculty of Medicine,undefined
[4] The University of Hong Kong,undefined
[5] School of Natural Sciences,undefined
[6] Griffith University,undefined
[7] Genomics Research Centre,undefined
[8] Institute of Health and Biomedical Innovation,undefined
[9] Faculty of Health,undefined
[10] Queensland University of Technology,undefined
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Mutation of FAM134B (Family with Sequence Similarity 134, Member B) leading to loss of function of its encoded Golgi protein and has been reported induce apoptosis in neurological disorders. FAM134B mutation is still unexplored in cancer. Herein, we studied the DNA copy number variation and novel mutation sites of FAM134B in a large cohort of freshly collected oesophageal squamous cell carcinoma (ESCC) tissue samples. In ESCC tissues, 37% (38/102) showed increased FAM134B DNA copies whereas 35% (36/102) showed loss of FAM134B copies relative to matched non-cancer tissues. Novel mutations were detected in exons 4, 5, 7, 9 as well as introns 2, 4-8 of FAM134B via HRM (High-Resolution Melt) and Sanger sequencing analysis. Overall, thirty-seven FAM134B mutations were noted in which most (31/37) mutations were homozygous. FAM134B mutations were detected in all the cases with metastatic ESCC in the lymph node tested and in 14% (8/57) of the primary ESCC. Genetic alteration of FAM134B is a frequent event in the progression of ESCCs. These findings imply that mutation might be the major driving source of FAM134B genetic modulation in ESCCs.
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