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白血病和多发性骨髓瘤药物的关键性临床试验是否能代表风险人群?

Are Pivotal Clinical Trials for Drugs Approved for Leukemias and Multiple Myeloma Representative of the Population at Risk?

机构信息

Internal Medicine, Medical College of Georgia at Augusta University, Augusta, GA.

Institute of Public Health and Preventive Health, Augusta University, Augusta, GA.

出版信息

J Clin Oncol. 2022 Nov 10;40(32):3719-3729. doi: 10.1200/JCO.22.00504. Epub 2022 Aug 9.

Abstract

PURPOSE

There are significant disparities in care and outcomes for patients with leukemias and multiple myeloma (MM). To evaluate the extent to which clinical trials (CTs) match the demographic and geographic diversity of populations affected by leukemias and MM.

METHODS

CTs leading to drug approval were identified from the US Food and Drug Administration databases. Demographic and geographic data were collected from ClinicalTrials.gov and primary manuscripts. Standard descriptive statistics were used to summarize the data in frequencies and proportions, including 95% CIs, by race, ethnicity, sex, and malignancy subtypes.

RESULTS

A total of 41 (67.2%) trials leading to drug approval reported data on race and 20 (48.8%) on ethnicity. These trials included 13,731 patients, of whom 11,209 (81.6%) were White. Among minorities, Asian-Pacific Islanders and Blacks had the highest representation in chronic myeloid leukemia, 147 (12.7%) and 61 (5.3%), and lowest in chronic lymphocytic leukemia, 55 (3%) and 20 (1.1%), respectively. Proportions for Blacks, Native Americans, and Hispanics were significantly low, reflecting under-representation in trials compared with the proportion in the general population. Females were also under-represented in acute myeloid leukemia (44.7% 60.5%, < .0001), and males in MM (55.3% 60.2%, < .0001) and chronic myeloid leukemia (55.2% 62.9%, < .0001). The geographic distribution of trials showed inadequate regional and state participation compared with mortality for all malignancies except MM.

CONCLUSION

There are significant demographic and geographic under-representation and imbalances in pivotal CTs leading to drug approvals for leukemias and MM compared with the population affected. These disparities need to be addressed to make results applicable to all relevant populations.

摘要

目的

白血病和多发性骨髓瘤(MM)患者的治疗和结局存在显著差异。本研究旨在评估临床试验(CTs)在多大程度上与受白血病和 MM 影响的人群的人口统计学和地理多样性相匹配。

方法

从美国食品和药物管理局数据库中确定了导致药物批准的 CTs。从 ClinicalTrials.gov 和主要手稿中收集了人口统计学和地理数据。使用标准描述性统计数据以频率和比例(包括 95%置信区间)总结数据,按种族、族裔、性别和恶性肿瘤亚型进行分类。

结果

总共 41 项(67.2%)导致药物批准的试验报告了种族数据,20 项(48.8%)报告了族裔数据。这些试验共纳入了 13731 名患者,其中 11209 名(81.6%)为白人。在少数族裔中,亚洲-太平洋岛民和黑人在慢性髓性白血病中的代表性最高,分别为 147 例(12.7%)和 61 例(5.3%),而在慢性淋巴细胞白血病中则最低,分别为 55 例(3%)和 20 例(1.1%)。黑人、美国原住民和西班牙裔的比例明显较低,这反映了他们在试验中的代表性不足,与普通人群中的比例相比存在差距。女性在急性髓性白血病中的代表性也不足(44.7% 60.5%,<.0001),男性在 MM(55.3% 60.2%,<.0001)和慢性髓性白血病(55.2% 62.9%,<.0001)中的代表性也不足。与除 MM 外的所有恶性肿瘤的死亡率相比,试验的地理分布在区域和州参与方面存在明显不足。

结论

与受影响人群相比,白血病和 MM 的关键 CT 导致药物批准的人群在人口统计学和地理分布方面存在显著的代表性不足和不平衡。需要解决这些差异,以使结果适用于所有相关人群。

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