家族病史评估在基因组学时代极大地促进了精准医学的发展。
Family history assessment significantly enhances delivery of precision medicine in the genomics era.
机构信息
SingHealth Duke-NUS Institute of Precision Medicine, Singapore Health Services, Singapore, Singapore.
Cancer and Stem Cell Biology, Duke-NUS Medical School, Singapore, Singapore.
出版信息
Genome Med. 2021 Jan 7;13(1):3. doi: 10.1186/s13073-020-00819-1.
BACKGROUND
Family history has traditionally been an essential part of clinical care to assess health risks. However, declining sequencing costs have precipitated a shift towards genomics-first approaches in population screening programs rendering the value of family history unknown. We evaluated the utility of incorporating family history information for genomic sequencing selection.
METHODS
To ascertain the relationship between family histories on such population-level initiatives, we analysed whole genome sequences of 1750 research participants with no known pre-existing conditions, of which half received comprehensive family history assessment of up to four generations, focusing on 95 cancer genes.
RESULTS
Amongst the 1750 participants, 866 (49.5%) had high-quality standardised family history available. Within this group, 73 (8.4%) participants had an increased family history risk of cancer (increased FH risk cohort) and 1 in 7 participants (n = 10/73) carried a clinically actionable variant inferring a sixfold increase compared with 1 in 47 participants (n = 17/793) assessed at average family history cancer risk (average FH risk cohort) (p = 0.00001) and a sevenfold increase compared to 1 in 52 participants (n = 17/884) where family history was not available (FH not available cohort) (p = 0.00001). The enrichment was further pronounced (up to 18-fold) when assessing only the 25 cancer genes in the American College of Medical Genetics (ACMG) Secondary Findings (SF) genes. Furthermore, 63 (7.3%) participants had an increased family history cancer risk in the absence of an apparent clinically actionable variant.
CONCLUSIONS
These findings demonstrate that the collection and analysis of comprehensive family history and genomic data are complementary and in combination can prioritise individuals for genomic analysis. Thus, family history remains a critical component of health risk assessment, providing important actionable data when implementing genomics screening programs.
TRIAL REGISTRATION
ClinicalTrials.gov NCT02791152 . Retrospectively registered on May 31, 2016.
背景
家族史一直是临床评估健康风险的重要组成部分。然而,测序成本的下降促使人群筛查项目转向以基因组学为基础的方法,使得家族史的价值变得未知。我们评估了将家族史信息纳入基因组测序选择的效用。
方法
为了确定此类人群级计划中家族史之间的关系,我们分析了 1750 名无已知既往疾病的研究参与者的全基因组序列,其中一半接受了最多四代的全面家族史评估,重点关注 95 个癌症基因。
结果
在 1750 名参与者中,866 名(49.5%)有高质量的标准化家族史可用。在这一组中,73 名(8.4%)参与者有增加的癌症家族史风险(增加的 FH 风险队列),每 7 名参与者中就有 1 名(n=10/73)携带可临床操作的变异,与每 47 名参与者中 1 名(n=17/793)评估的平均 FH 风险队列(平均 FH 风险队列)相比增加了六倍(p=0.00001),与每 52 名参与者中 1 名(n=17/884)相比增加了七倍,其中家族史不可用(FH 不可用队列)(p=0.00001)。当仅评估美国医学遗传学学院(ACMG)次要发现(SF)基因中的 25 个癌症基因时,这种富集更为明显(高达 18 倍)。此外,63 名(7.3%)参与者在没有明显可临床操作的变异的情况下有增加的家族史癌症风险。
结论
这些发现表明,全面家族史和基因组数据的收集和分析是互补的,并且可以结合起来优先对个体进行基因组分析。因此,家族史仍然是健康风险评估的关键组成部分,在实施基因组筛查计划时提供重要的可操作数据。
试验注册
ClinicalTrials.gov NCT02791152。于 2016 年 5 月 31 日回顾性注册。
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