在携带BAP1和其他种系突变的患者中出现的一组生存期有所改善的间皮瘤。
A Subset of Mesotheliomas With Improved Survival Occurring in Carriers of BAP1 and Other Germline Mutations.
作者信息
Pastorino Sandra, Yoshikawa Yoshie, Pass Harvey I, Emi Mitsuru, Nasu Masaki, Pagano Ian, Takinishi Yasutaka, Yamamoto Ryuji, Minaai Michael, Hashimoto-Tamaoki Tomoko, Ohmuraya Masaki, Goto Keisuke, Goparaju Chandra, Sarin Kavita Y, Tanji Mika, Bononi Angela, Napolitano Andrea, Gaudino Giovanni, Hesdorffer Mary, Yang Haining, Carbone Michele
机构信息
Sandra Pastorino, Mitsuru Emi, Masaki Nasu, Ian Pagano, Yasutaka Takinishi, Ryuji Yamamoto, Michael Minaai, Keisuke Goto, Mika Tanji, Angela Bononi, Andrea Napolitano, Giovanni Gaudino, Haining Yang, and Michele Carbone, University of Hawaii Cancer Center, Honolulu, HI; Yoshie Yoshikawa, Mitsuru Emi, Tomoko Hashimoto-Tamaoki, and Masaki Ohmuraya, Hyogo College of Medicine, Hyogo, Japan; Mary Hesdorffer, Mesothelioma Applied Research Foundation, Washington DC; Harvey I. Pass and Chandra Goparaju, New York University Langone Medical Center, New York, NY; Andrea Neopolitano, University Campus Bio-Medico, Rome, Italy; and Kavita Y. Sarin, Stanford University, Stanford, CA.
出版信息
J Clin Oncol. 2018 Oct 30;36(35):JCO2018790352. doi: 10.1200/JCO.2018.79.0352.
PURPOSE
We hypothesized that four criteria could help identify malignant mesotheliomas (MMs) most likely linked to germline mutations of BAP1 or of other genes: family history of MM, BAP1-associated cancers, or multiple malignancies; or age younger than 50 years.
PATIENTS AND METHODS
Over the course of 7 years, 79 patients with MM met the four criteria; 22 of the 79 (28%) reported possible asbestos exposure. They were screened for germline BAP1 mutations by Sanger sequencing and by targeted next-generation sequencing (tNGS) for germline mutations in 55 additional cancer-linked genes. Deleterious mutations detected by tNGS were validated by Sanger sequencing.
RESULTS
Of the 79 patients, 43 (16 probands and 27 relatives) had deleterious germline BAP1 mutations. The median age at diagnosis was 54 years and median survival was 5 years. Among the remaining 36 patients with no BAP1 mutation, median age at diagnosis was 45 years, median survival was 9 years, and 12 had deleterious mutations of additional genes linked to cancer. When compared with patients with MMs in the SEER cohort, median age at diagnosis (72 years), median survival for all MM stages (8 months), and stage I (11 months) were significantly different from the 79 patients with MM in the current study ( P < .0001).
CONCLUSION
We provide criteria that help identify a subset of patients with MM who had significantly improved survival. Most of these patients were not aware of asbestos exposure and carried either pathogenic germline mutations of BAP1 or of additional genes linked to cancer, some of which may have targeted-therapy options. These patients and their relatives are susceptible to development of additional cancers; therefore, genetic counseling and cancer screening should be considered.
目的
我们假设四个标准有助于识别最有可能与BAP1或其他基因的种系突变相关的恶性间皮瘤(MM):MM家族史、BAP1相关癌症或多种恶性肿瘤;或年龄小于50岁。
患者和方法
在7年的时间里,79例MM患者符合这四个标准;79例中的22例(28%)报告可能接触过石棉。通过Sanger测序对他们进行种系BAP1突变筛查,并通过靶向二代测序(tNGS)检测另外55个癌症相关基因的种系突变。通过tNGS检测到的有害突变通过Sanger测序进行验证。
结果
79例患者中,43例(16例先证者和27例亲属)有种系BAP1有害突变。诊断时的中位年龄为54岁,中位生存期为5年。其余36例无BAP1突变的患者中,诊断时的中位年龄为45岁,中位生存期为9年,12例有与癌症相关的其他基因的有害突变。与监测、流行病学和最终结果(SEER)队列中的MM患者相比,诊断时的中位年龄(72岁)、所有MM分期的中位生存期(8个月)和I期(11个月)与本研究中的79例MM患者有显著差异(P <.0001)。
结论
我们提供了有助于识别生存期显著改善的MM患者亚组的标准。这些患者中的大多数不知道接触过石棉,并且携带BAP1或与癌症相关的其他基因的致病种系突变,其中一些可能有靶向治疗选择。这些患者及其亲属易患其他癌症;因此,应考虑进行遗传咨询和癌症筛查。
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