基于生活方式、环境和遗传因素确定结直肠癌风险和筛查起始年龄。
Determining Risk of Colorectal Cancer and Starting Age of Screening Based on Lifestyle, Environmental, and Genetic Factors.
机构信息
Department of Epidemiology, University of Michigan, Ann Arbor, Michigan.
Memorial Sloan Kettering, New York, New York.
出版信息
Gastroenterology. 2018 Jun;154(8):2152-2164.e19. doi: 10.1053/j.gastro.2018.02.021. Epub 2018 Feb 17.
BACKGROUND & AIMS: Guidelines for initiating colorectal cancer (CRC) screening are based on family history but do not consider lifestyle, environmental, or genetic risk factors. We developed models to determine risk of CRC, based on lifestyle and environmental factors and genetic variants, and to identify an optimal age to begin screening.
METHODS
We collected data from 9748 CRC cases and 10,590 controls in the Genetics and Epidemiology of Colorectal Cancer Consortium and the Colorectal Transdisciplinary study, from 1992 through 2005. Half of the participants were used to develop the risk determination model and the other half were used to evaluate the discriminatory accuracy (validation set). Models of CRC risk were created based on family history, 19 lifestyle and environmental factors (E-score), and 63 CRC-associated single-nucleotide polymorphisms identified in genome-wide association studies (G-score). We evaluated the discriminatory accuracy of the models by calculating area under the receiver operating characteristic curve values, adjusting for study, age, and endoscopy history for the validation set. We used the models to project the 10-year absolute risk of CRC for a given risk profile and recommend ages to begin screening in comparison to CRC risk for an average individual at 50 years of age, using external population incidence rates for non-Hispanic whites from the Surveillance, Epidemiology, and End Results program registry.
RESULTS
In our models, E-score and G-score each determined risk of CRC with greater accuracy than family history. A model that combined both scores and family history estimated CRC risk with an area under the receiver operating characteristic curve value of 0.63 (95% confidence interval, 0.62-0.64) for men and 0.62 (95% confidence interval, 0.61-0.63) for women; area under the receiver operating characteristic curve values based on only family history ranged from 0.53 to 0.54 and those based only E-score or G-score ranged from 0.59 to 0.60. Although screening is recommended to begin at age 50 years for individuals with no family history of CRC, starting ages calculated based on combined E-score and G-score differed by 12 years for men and 14 for women, for individuals with the highest vs the lowest 10% of risk.
CONCLUSIONS
We used data from 2 large international consortia to develop CRC risk calculation models that included genetic and environmental factors along with family history. These determine risk of CRC and starting ages for screening with greater accuracy than the family history only model, which is based on the current screening guideline. These scoring systems might serve as a first step toward developing individualized CRC prevention strategies.
背景与目的
结直肠癌(CRC)筛查指南基于家族史,但不考虑生活方式、环境或遗传风险因素。我们开发了基于生活方式和环境因素以及遗传变异来确定 CRC 风险的模型,并确定开始筛查的最佳年龄。
方法
我们从 1992 年至 2005 年期间收集了遗传与结直肠癌流行病学研究联盟和结直肠跨学科研究中 9748 例 CRC 病例和 10590 例对照的数据。参与者的一半用于开发风险确定模型,另一半用于评估鉴别准确性(验证集)。基于家族史、19 种生活方式和环境因素(E 评分)以及全基因组关联研究中确定的 63 个 CRC 相关单核苷酸多态性(G 评分),建立 CRC 风险模型。我们通过计算验证集中调整研究、年龄和内镜史后的受试者工作特征曲线下面积值来评估模型的鉴别准确性。我们使用这些模型为给定的风险特征预测特定年龄的 CRC 10 年绝对风险,并与 50 岁时平均个体的 CRC 风险进行比较,使用非西班牙裔白人的外部人群发病率来自监测、流行病学和最终结果计划登记处。
结果
在我们的模型中,E 评分和 G 评分各自比家族史更准确地确定 CRC 的风险。一个结合了这两个评分和家族史的模型,男性的受试者工作特征曲线下面积值为 0.63(95%置信区间,0.62-0.64),女性为 0.62(95%置信区间,0.61-0.63);仅基于家族史的受试者工作特征曲线下面积值范围为 0.53 至 0.54,仅基于 E 评分或 G 评分的受试者工作特征曲线下面积值范围为 0.59 至 0.60。虽然对于没有 CRC 家族史的个体,建议从 50 岁开始筛查,但根据 E 评分和 G 评分的综合计算得出的起始年龄,男性相差 12 岁,女性相差 14 岁,最高和最低 10%的风险个体之间。
结论
我们使用来自两个大型国际联盟的数据,开发了包括遗传和环境因素以及家族史的 CRC 风险计算模型。这些模型比仅基于家族史的模型更准确地确定 CRC 风险和筛查开始年龄,该模型基于当前的筛查指南。这些评分系统可能成为制定个体化 CRC 预防策略的第一步。
Zotero 插件