Oh Joowon, Kim Yu Ri, Kim Yoonjung, Kim Boyeon, Park Kyung Sun, Nam Seong-Hyeuk, Lee Kyung-A
Department of Laboratory Medicine, Sheikh Khalifa Specialty Hospital, Ras Al Khaimah, United Arab Emirates.
Division of hematology, Department of internal medicine, Yonsei University College of Medicine, Seoul, Korea.
J Cancer. 2021 May 19;12(14):4288-4294. doi: 10.7150/jca.54169. eCollection 2021.
As the number of long-term survivors of solid cancers keeps increasing, risk assessment of secondary hematologic malignancies is important for the prognosis of the patient. Germline genetic predisposition to secondary hematologic malignancy has been studied widely in myeloid neoplasms and rarely in lymphoid neoplasms. This study aimed to profile the mutational spectrums of patients with subsequent lymphoid tissue neoplasm to shed some light on the understudied area. In total, 39 patients who had primary solid cancer and subsequent hematologic malignancies were enrolled. We performed two next-generation sequencing (NGS) panel tests encompassing hereditary cancer predisposition genes and genes related to clonal hematopoiesis of indeterminate potential (CHIP). All statistical analyses were performed using R 3.5.1. We found 8 of 39 patients with germline mutations in cancer predisposition genes; 4 of 18 patients had therapy-related myeloid neoplasms (22.2%); and 4 of 15 patients had secondary lymphoid malignancies (26.7%). Notably, of 14 patients who initially suffered from thyroid cancer, 5 patients (35.7%) had germline mutations. Malignancy of lymphoid tissue showed no association with radioactive iodine therapy but was observed to a greater extent in germline mutation-positive thyroid cancer patients regardless of their history of treatment. We observed that 24 of 39 patients (61.5%) were CHIP carriers. Patients who had secondary lymphoid malignancy were less likely to have CHIP than those who had myeloid malignancy. In patients with primary solid cancer who are planning to undergo cytotoxic chemotherapy, radiotherapy, or radioactive iodine therapy, an initial assessment with germline mutation testing using an expanded NGS panel, including low, moderate, and high-risk cancer-associated genes, and somatic CHIP mutation testing can screen the patients who are at risk of developing therapy-related myeloid and lymphoid malignancies. Through careful screening and monitoring throughout the treatment process, patients can benefit from the early detection of secondary malignancies and receive proper treatment.
随着实体癌长期存活者数量不断增加,继发性血液系统恶性肿瘤的风险评估对患者预后至关重要。在髓系肿瘤中,对继发性血液系统恶性肿瘤的种系遗传易感性已进行了广泛研究,而在淋巴系肿瘤中研究较少。本研究旨在剖析后续发生淋巴组织肿瘤患者的突变谱,以阐明这一研究不足的领域。总共纳入了39例患有原发性实体癌并继发血液系统恶性肿瘤的患者。我们进行了两项二代测序(NGS)panel检测,涵盖遗传性癌症易感基因和与潜在意义未明的克隆性造血(CHIP)相关的基因。所有统计分析均使用R 3.5.1进行。我们发现39例患者中有8例存在癌症易感基因的种系突变;18例患者中有4例发生了与治疗相关的髓系肿瘤(22.2%);15例患者中有4例发生了继发性淋巴系恶性肿瘤(26.7%)。值得注意的是,在最初患有甲状腺癌的14例患者中,有5例(35.7%)存在种系突变。淋巴组织恶性肿瘤与放射性碘治疗无关,但在种系突变阳性的甲状腺癌患者中更为常见,无论其治疗史如何。我们观察到39例患者中有24例(61.5%)是CHIP携带者。发生继发性淋巴系恶性肿瘤的患者比发生髓系恶性肿瘤的患者携带CHIP的可能性更小。对于计划接受细胞毒性化疗、放疗或放射性碘治疗的原发性实体癌患者,使用包括低、中、高风险癌症相关基因的扩展NGS panel进行种系突变检测和体细胞CHIP突变检测的初始评估,可以筛查出有发生与治疗相关的髓系和淋巴系恶性肿瘤风险的患者。通过在整个治疗过程中进行仔细的筛查和监测,患者可以从继发性恶性肿瘤的早期发现中获益并接受适当的治疗。
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