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针对风险因素以减轻乳腺癌的种族差异负担。

Targeting risk factors for reducing the racially disparate burden in breast cancer.

作者信息

Wright Nikita, Akinyemiju Tomi, Subhedar Preeti, Rida Padmashree, Aneja Ritu

机构信息

Georgia State University, Atlanta, GA 30303.

University of Kentucky, Lexington, KY 40504.

出版信息

Front Biosci (Schol Ed). 2019 Mar 1;11(1):136-160. doi: 10.2741/S531.

Abstract

African-American (AA) women are more likely to die from breast cancer (BC), at any age, compared to European-American women. Although breakthroughs in pre-clinical studies have resulted in potentially actionable targets in AA BC, drugs that were rationally designed for these targets have performed poorly in clinical trials. Challenges with interpatient and intratumoral heterogeneity, lack of drug sensitivity and specificity, suboptimal biomarker cut-offs, lack of drug response predictive biomarkers, drug side effects, high costs of drug development, and under-representation of AAs in clinical trials complicate the development of targeted therapies for AA BC patients. Accumulating evidence suggests that racial disparities exist in non-genetic risk factors that can alter genetic and epigenetic programs to promote breast tumorigenesis. Herein, we present a "roadmap" that addresses non-genetic risk factors that are suspected to contribute to the racial disparity in BC mortality. Increased targeting of these non-genetic risk factors may proffer a safer and more economical route to alleviating the racially disparate burden in BC.

摘要

与欧美女性相比,非裔美国(AA)女性在任何年龄段死于乳腺癌(BC)的可能性都更高。尽管临床前研究取得了突破,在AA BC中产生了潜在可操作的靶点,但针对这些靶点合理设计的药物在临床试验中的表现却很差。患者间和肿瘤内异质性、缺乏药物敏感性和特异性、生物标志物临界值不理想、缺乏药物反应预测生物标志物、药物副作用、药物开发成本高昂以及AA人群在临床试验中的代表性不足等问题,使AA BC患者靶向治疗的开发变得复杂。越来越多的证据表明,在非遗传风险因素方面存在种族差异,这些因素可改变基因和表观遗传程序,促进乳腺肿瘤发生。在此,我们提出一个“路线图”,以解决那些被怀疑导致BC死亡率种族差异的非遗传风险因素。增加对这些非遗传风险因素的针对性,可能会为减轻BC的种族差异负担提供一条更安全、更经济的途径。

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