Methodologic Approach to Defining Comorbidities in a Cohort of Patients With Cancer: An Example in the Optimal Breast Cancer Chemotherapy Dosing Study.

IF 3.3 Q2 ONCOLOGY

JCO Clinical Cancer Informatics Pub Date : 2025-02-01 Epub Date: 2025-02-14 DOI:10.1200/CCI-24-00231

Peng Wang, Kelli O'Connell, Jenna Bhimani, Victoria Blinder, Rachael Burganowski, Isaac J Ergas, Grace B Gallagher, Jennifer J Griggs, Narre Heon, Tatjana Kolevska, Yuriy Kotsurovskyy, Candyce H Kroenke, Cecile A Laurent, Raymond Liu, Kanichi G Nakata, Sonia Persaud, Donna R Rivera, Janise M Roh, Sara Tabatabai, Emily Valice, Elisa V Bandera, Lawrence H Kushi, Erin J Aiello Bowles, Elizabeth D Kantor

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引用次数: 0

Abstract

Purpose: We evaluated the definitions of five comorbidities (renal and hepatic impairments, anemia, neutropenia, and thrombocytopenia) in women with breast cancer using data from electronic health records.

Methods: In 11,097 women receiving adjuvant chemotherapy for stage I-IIIA breast cancer at Kaiser Permanente Northern California or Kaiser Permanente Washington, we assessed comorbidity definitions in two commonly used lookback windows (1 year before diagnosis, T1; and extending until chemotherapy initiation, T1-2). Within each, we assessed data availability and agreement between International Classification of Diseases (ICD)-defined and lab-defined comorbidities of varying severity. To assess how different pieces of information may affect providers in making treatment decisions, we used multivariable logistic regression to evaluate four-category (with comorbidity indicated by both ICD and lab, ICD-only, lab-only, or neither) and collapsed binary (comorbidity indicated by either ICD or lab v neither) definitions in relation to first cycle chemotherapy dose reduction (FCDR).

Results: Extending the lookback period to chemotherapy initiation increased laboratory data availability (missingness ≤4.1% in T1-2 v >40% in T1). Assessment of agreement guided selection of laboratory cutpoints. In both time periods, the four-category and binary comorbidity variables were associated with use of FCDR, but binary variables had larger cell sizes and more stability of regression models. Ultimately, the comorbidity variables in T1 were defined by a combination of either ICD/qualifying laboratory values. Results were similar in T1-2, except laboratory data alone outperformed the combination variable for renal and hepatic comorbidity.

Conclusion: Leveraging both ICD and lab data and extending the lookback period to include postdiagnosis but prechemotherapy initiation may provide better capture of comorbidity. Future studies may consider validating our findings with a gold-standard comorbidity status and in other community health care settings.

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在癌症患者队列中定义合并症的方法学方法：以最佳乳腺癌化疗剂量研究为例。

目的：我们利用电子健康记录的数据评估乳腺癌女性患者的五种合并症（肾和肝损害、贫血、中性粒细胞减少症和血小板减少症）的定义。方法：在北加州Kaiser Permanente或华盛顿Kaiser Permanente接受I-IIIA期乳腺癌辅助化疗的11097名女性中，我们通过两种常用的回顾窗口(诊断前1年，T1；并持续到化疗开始，T1-2)。在每一项研究中，我们评估了数据的可用性以及国际疾病分类（ICD）定义的不同严重程度的合并症和实验室定义的合并症之间的一致性。为了评估不同的信息如何影响提供者做出治疗决策，我们使用多变量逻辑回归来评估与第一周期化疗剂量减少（FCDR）相关的四类定义（ICD和实验室显示的合并症，仅ICD，仅实验室，或两者都没有）和折叠二元定义（ICD或实验室显示的合并症或两者都没有）。结果：延长化疗开始的回顾期增加了实验室数据的可获得性（T1-2 v的缺失≤4.1%，T1的缺失≤40%）。协议评估指导了实验室切入点的选择。在这两个时间段，四类和二元共病变量与FCDR的使用有关，但二元变量具有更大的细胞大小和更稳定的回归模型。最终，T1中的合并症变量由ICD/合格实验室值的组合来定义。T1-2的结果相似，除了实验室数据单独优于肾脏和肝脏合并症的联合变量。结论：利用ICD和实验室数据，延长回顾期，包括诊断后和化疗前开始，可以更好地捕捉合并症。未来的研究可能会考虑用金标准的合并症状态和其他社区卫生保健机构来验证我们的发现。

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来源期刊

JCO Clinical Cancer Informatics ONCOLOGY-

CiteScore

6.20

自引率

4.80%

发文量

190