Abstract
The molecular drivers of thymoma are poorly understood. Outside of the identification of rarely occurring epidermal growth factor receptor and v-kit Hardy-Zuckerman 4 feline sarcoma viral oncogene homolog mutations via candidate gene sequencing, mutations in common cancer genes have yet to be observed. Only a single thymoma genome sequence has been previously reported, with no mutations in known cancer genes identified. Thus, we attempted to identify somatic driver mutations in a cytogenetically normal thymoma. A stage IVB type B3 thymoma from a 47-year-old male of Asian descent with no history of myasthenia gravis or other autoimmune condition was genomically evaluated. Exome sequencing and low-pass whole-genome sequencing was performed to identify somatic point mutations, copy number changes and structural variants. Mutations in known tumor suppressors DNMT3A (p.G728D) and ASXL1 (p.E657fs), consistent with mutations of known consequence in acute myeloid leukemia, were identified. Contrary to a previous report, this finding suggests the genetic etiology of thymomas may not be fundamentally distinct from other tumor types. Rather, these findings suggest that further sequencing of cytogenetically normal thymoma samples should reveal the specific molecular drivers of thymoma.
Highlights
Thymomas are rare tumors arising from the epithelial cells of the thymus, commonly associated with myasthenia gravis or other autoimmune disorders.[1]
Our results show that mutations in DNMT3A and additional sex comblike 1 (ASXL1) have a role in the development of thymoma
The previously reported thymoma displayed cytogenetic abnormalities commonly observed in B3 thymomas, whereas this tumor displayed largely normal cytogenetics
Summary
Thymomas are rare tumors arising from the epithelial cells of the thymus, commonly associated with myasthenia gravis or other autoimmune disorders.[1] The WHO classification system categorizes thymomas (type A, B1, B2, B3 and AB) and thymic carcinoma (type C) according to morphology, degree of atypia, histological similarity to normal thymic cells and degree of lymphocyte infiltration.[2] Thymomas are staged (stage I, IIA, IIB, III, IVA and IVB) according to degree of encapsulation and anatomic extent of disease with encapsulation decreasing and dispersion from the thymus increasing with stage.[3] Late stage thymomas are very rare and tend to locally recur rather than metastasize. Type B3 thymomas are the most aggressive of the thymomas. Surgical resection is the favored treatment for thymoma
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