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胚系 BAP1 突变的间皮瘤患者的长期生存率提高了 7 倍。

Mesothelioma patients with germline BAP1 mutations have 7-fold improved long-term survival.

机构信息

University of Hawaii Cancer Center, Honolulu, HI 96813, USA,

University of Hawaii Cancer Center, Honolulu, HI 96813, USA.

出版信息

Carcinogenesis. 2015 Jan;36(1):76-81. doi: 10.1093/carcin/bgu227. Epub 2014 Nov 7.

Abstract

BRCA1-associated protein-1 (BAP1) mutations cause a new cancer syndrome, with a high rate of malignant mesothelioma (MM). Here, we tested the hypothesis that MM associated with germline BAP1 mutations has a better prognosis compared with sporadic MM. We compared survival among germline BAP1 mutation MM patients with that of all MM (N = 10 556) recorded in the United States Surveillance, Epidemiology, and End Results (SEER) data from 1973 to 2010. We identified 23 MM patients--11 alive--with germline BAP1 mutations and available data on survival. Ten patients had peritoneal MM, ten pleural MM and three MM in both locations. Thirteen patients had one or more malignancies in addition to MM. Actuarial median survival for the MM patients with germline BAP1 mutations was 5 years, as compared with <1 year for the median survival in the United States SEER MM group. Five-year survival was 47%, 95% confidence interval (24-67%), as compared with 6.7% (6.2-7.3%) in the control SEER group. Analysis of the pooled cohort of germline BAP1 mutation MM showed that patients with peritoneal MM (median survival of 10 years, P = 0.0571), or with a second malignancy in addition to MM (median survival of 10 years, P = 0.0716), survived for a longer time compared with patients who only had pleural MM, or MM patients without a second malignancy, respectively. In conclusion, we found that MM patients with germline BAP1 mutations have an overall 7-fold increased long-term survival, independently of sex and age. Appropriate genetic counseling and clinical management should be considered for MM patients who are also BAP1 mutation carriers.

摘要

BRCA1 相关蛋白-1(BAP1)突变导致一种新的癌症综合征,其中恶性间皮瘤(MM)的发生率很高。在这里,我们检验了这样一个假设,即与胚系 BAP1 突变相关的 MM 与散发性 MM 相比具有更好的预后。我们比较了美国监测、流行病学和最终结果(SEER)数据库中 1973 年至 2010 年间记录的胚系 BAP1 突变 MM 患者与所有 MM 患者的生存情况(N=10556)。我们鉴定了 23 名 MM 患者,其中 11 名仍存活,且可获得生存数据。其中 10 名患者为腹膜 MM,10 名患者为胸膜 MM,3 名患者为腹膜和胸膜 MM 均有。13 名患者除 MM 外还有一种或多种恶性肿瘤。胚系 BAP1 突变 MM 患者的 MM 中位生存时间为 5 年,而美国 SEER MM 组的中位生存时间不到 1 年。5 年生存率为 47%(95%CI:24%-67%),而对照组 SEER 组为 6.7%(6.2%-7.3%)。对胚系 BAP1 突变 MM 患者的汇总队列分析显示,与仅患有胸膜 MM 患者(中位生存时间 10 年,P=0.0571)或除 MM 之外还有第二种恶性肿瘤的患者(中位生存时间 10 年,P=0.0716)相比,患有腹膜 MM 的患者生存时间更长。总之,我们发现,与仅患有胸膜 MM 的患者或没有第二种恶性肿瘤的 MM 患者相比,胚系 BAP1 突变 MM 患者的总生存期延长了 7 倍,与性别和年龄无关。对于同时为 BAP1 突变携带者的 MM 患者,应考虑进行适当的遗传咨询和临床管理。

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