Vis D J, Lewin J, Liao R G, Mao M, Andre F, Ward R L, Calvo F, Teh B T, Camargo A A, Knoppers B M, Sawyers C L, Wessels L F A, Lawler M, Siu L L, Voest E
Netherlands Cancer Institute, Amsterdam, The Netherlands.
Princess Margaret Cancer Centre, Toronto, Canada.
Ann Oncol. 2017 May 1;28(5):1145-1151. doi: 10.1093/annonc/mdx037.
While next generation sequencing has enhanced our understanding of the biological basis of malignancy, current knowledge on global practices for sequencing cancer samples is limited. To address this deficiency, we developed a survey to provide a snapshot of current sequencing activities globally, identify barriers to data sharing and use this information to develop sustainable solutions for the cancer research community.
A multi-item survey was conducted assessing demographics, clinical data collection, genomic platforms, privacy/ethics concerns, funding sources and data sharing barriers for sequencing initiatives globally. Additionally, respondents were asked as to provide the primary intent of their initiative (clinical diagnostic, research or combination).
Of 107 initiatives invited to participate, 59 responded (response rate = 55%). Whole exome sequencing (P = 0.03) and whole genome sequencing (P = 0.01) were utilized less frequently in clinical diagnostic than in research initiatives. Procedures to identify cancer-specific variants were heterogeneous, with bioinformatics pipelines employing different mutation calling/variant annotation algorithms. Measurement of treatment efficacy varied amongst initiatives, with time on treatment (57%) and RECIST (53%) being the most common; however, other parameters were also employed. Whilst 72% of initiatives indicated data sharing, its scope varied, with a number of restrictions in place (e.g. transfer of raw data). The largest perceived barriers to data harmonization were the lack of financial support (P < 0.01) and bioinformatics concerns (e.g. lack of interoperability) (P = 0.02). Capturing clinical data was more likely to be perceived as a barrier to data sharing by larger initiatives than by smaller initiatives (P = 0.01).
These results identify the main barriers, as perceived by the cancer sequencing community, to effective sharing of cancer genomic and clinical data. They highlight the need for greater harmonization of technical, ethical and data capture processes in cancer sample sequencing worldwide, in order to support effective and responsible data sharing for the benefit of patients.
虽然下一代测序技术增进了我们对恶性肿瘤生物学基础的理解,但目前关于全球癌症样本测序实践的知识有限。为解决这一不足,我们开展了一项调查,以呈现全球当前测序活动的概况,识别数据共享的障碍,并利用这些信息为癌症研究界制定可持续的解决方案。
进行了一项多项调查,评估全球测序计划的人口统计学、临床数据收集、基因组平台、隐私/伦理问题、资金来源和数据共享障碍。此外,还要求受访者提供其计划的主要意图(临床诊断、研究或两者结合)。
在受邀参与的107项计划中,59项作出回应(回应率 = 55%)。与研究计划相比,全外显子组测序(P = 0.03)和全基因组测序(P = 0.01)在临床诊断中的使用频率较低。识别癌症特异性变异的程序各不相同,生物信息学流程采用了不同的突变检测/变异注释算法。各计划对治疗效果的衡量方法各异,治疗时间(57%)和实体瘤疗效评价标准(RECIST)(53%)是最常用的;不过,也采用了其他参数。虽然72%的计划表示会进行数据共享,但其范围各不相同,存在一些限制(如原始数据的转移)。数据协调方面最大的障碍被认为是缺乏资金支持(P < 0.01)和生物信息学问题(如缺乏互操作性)(P = 0.02)。与较小的计划相比,较大的计划更有可能将收集临床数据视为数据共享的障碍(P = 0.01)。
这些结果确定了癌症测序界认为的癌症基因组和临床数据有效共享的主要障碍。它们凸显了全球癌症样本测序在技术、伦理和数据收集过程中需要更大程度的协调,以支持有效且负责的数据共享,从而造福患者。
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