Clinical Genetics Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA.
Clinical Genetics Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA.
Lancet Oncol. 2021 Dec;22(12):1787-1798. doi: 10.1016/S1470-2045(21)00580-5. Epub 2021 Nov 12.
Li-Fraumeni syndrome, caused primarily by pathogenic or likely pathogenic germline TP53 variants, is a rare, variably penetrant, cancer predisposition syndrome with very high risks of cancer starting in childhood, including the risk of multiple primary malignancies over an individual's lifespan. We aimed to characterise and quantify cancer incidence, patterns, and genotype-phenotype associations in individuals with pathogenic or likely pathogenic germline TP53 variants.
This observational cohort study was done in 480 carriers of pathogenic or likely pathogenic germline TP53 variants enrolled in the National Cancer Institute's referral-based longitudinal Li-Fraumeni syndrome study between Aug 1, 2011, and March 24, 2020. Data on personal and family history of cancer were obtained through study questionnaires and validated by medical records. Variants were categorised on the basis of both loss-of-function (LOF) and dominant-negative effect (DNE) properties. Cancer incidence associated with Li-Fraumeni syndrome was compared with that of the general population using the Surveillance, Epidemiology, and End Results (SEER) 1975-2017 registry. Cancer incidence was evaluated with family-clustered Cox regression models and competing risk methods. This study is registered with ClinicalTrials.gov, NCT01443468.
Individuals with Li-Fraumeni syndrome had a nearly 24 times higher incidence of any cancer than the general population (standardised incidence ratio 23·9; 95% CI 21·9-26·0), with the highest comparative incidence from childhood to 30 years of age. The overall cancer incidence remained 10·3 (95% CI 7·9-13·2) times higher than that of the general population after age 50 years. In women, when considering breast cancer as a competing risk, the probability of a first diagnosis of a non-breast cancer malignancy was substantially lower than that of any first cancer (24·4% [95% CI 19·6-30·5] vs 50·4% [43·5-56·5] by age 33·7 years). Overall, DNE_LOF and notDNE_LOF variants were associated with earlier age at first and second cancer compared with notDNE_notLOF and DNE_notLOF variants. The time interval from first to second cancer was shorter among carriers whose first cancer diagnoses were later in life. Multiple cancers were diagnosed within a short timeframe in some individuals, regardless of the order of cancer occurrence.
This study adds granularity to the understanding of cancer incidence and patterns in individuals with pathogenic or likely pathogenic germline TP53 variants. Integration of age range-specific cancer incidence estimates, cancer-free survival by functional variant group, the potential impact of risk-reducing mastectomy on female cancer incidence, and data on subsequent malignancies will be important for the development of strategies to optimise cancer screening and management for these individuals.
Intramural Research Program, Division of Cancer Epidemiology and Genetics, National Institutes of Health.
李-佛美尼综合征主要由致病性或可能致病性种系 TP53 变异引起,是一种罕见的、表现度可变的、易患癌症的综合征,儿童期开始即具有极高的癌症风险,包括个体一生中发生多种原发性恶性肿瘤的风险。我们旨在描述和量化具有致病性或可能致病性种系 TP53 变异的个体的癌症发病率、模式和基因型-表型相关性。
本观察性队列研究纳入了 2011 年 8 月 1 日至 2020 年 3 月 24 日期间在国家癌症研究所基于转诊的纵向李-佛美尼综合征研究中入组的 480 名致病性或可能致病性种系 TP53 变异携带者。通过研究问卷和病历验证获取个人和家族癌症史数据。根据失活功能(LOF)和显性负效应(DNE)特性对变异进行分类。使用监测、流行病学和最终结果(SEER)1975-2017 登记处,将李-佛美尼综合征相关的癌症发病率与一般人群进行比较。使用家族聚类 Cox 回归模型和竞争风险方法评估癌症发病率。本研究在 ClinicalTrials.gov 注册,NCT01443468。
李-佛美尼综合征患者的癌症总发病率比一般人群高近 24 倍(标准化发病比 23.9;95%CI 21.9-26.0),儿童至 30 岁时的相对发病率最高。50 岁以后,癌症总发病率仍比一般人群高 10.3 倍(95%CI 7.9-13.2)。在女性中,当将乳腺癌视为竞争风险时,首次诊断为非乳腺癌恶性肿瘤的概率明显低于首次任何癌症的概率(24.4%[95%CI 19.6-30.5]vs 50.4%[43.5-56.5],至 33.7 岁)。总体而言,与 notDNE_notLOF 和 DNE_notLOF 变异相比,DNE_LOF 和 notDNE_LOF 变异与首次和第二次癌症的发病年龄更早相关。首次癌症诊断年龄较大的携带者的首次癌症至第二次癌症的时间间隔较短。无论癌症发生的顺序如何,一些个体的多种癌症都在短时间内被诊断出来。
本研究为了解具有致病性或可能致病性种系 TP53 变异的个体的癌症发病率和模式提供了更详细的信息。整合特定年龄范围的癌症发病率估计值、按功能变异组的无癌生存情况、降低风险的乳房切除术对女性癌症发病率的潜在影响以及随后发生的恶性肿瘤数据,将有助于制定策略来优化这些个体的癌症筛查和管理。
美国国立卫生研究院癌症流行病学和遗传学分部内部研究计划。
