非小细胞肺癌分子诊断使用率的种族和社会经济差异。

Stephanie Tuminello,Wiley M Turner,Matthew Untalan,Tara Ivic-Pavlicic,Raja Flores,Emanuela Taioli
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引用次数: 0

摘要

背景靶向疗法和免疫疗法等精准疗法大大改变了晚期非小细胞肺癌(NSCLC)的治疗现状。方法我们从监测、流行病学和最终结果(SEER)-医疗保险(Medicare)关联数据中提取了一组 NSCLC 患者。主要结果是根据理赔数据接受分子诊断检测。主要预测因素是种族和社会经济地位。结果 在 28,511 名 NSCLC 患者中,11,209 人(39.3%)接受了分子诊断检测。与白人患者相比,接受分子诊断检测的黑人患者较少(40.4% vs 27.9%; p < .001)。经调整后,黑人患者(ORadj[几率比]:0.64;95% CI[置信区间]:0.58-0.71)和生活在较贫困地区的患者(ORadj:0.85;95% CI:0.80-0.89)接受分子诊断检测的可能性在统计学上显著降低。接受检测的患者的死亡风险在统计学上显著降低(HRadj [危险比]:0.74;95% CI:0.72-0.76)。这些结果在对 IV 期 NSCLC 患者进行分层分析时也得到了证实。解决分子检测的障碍有助于缩小癌症治疗的差距并改善患者的预后。
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Racial and socioeconomic disparities in NSCLC molecular diagnostics uptake.
BACKGROUND Precision therapies, such as targeted and immunotherapies, have substantially changed the landscape of late-stage non-small cell lung cancer (NSCLC). Yet utilization of these therapies is disproportionate across strata defined by race and socioeconomic status (SES), possibly due to disparities in molecular diagnostic testing (or "biomarker testing"), which is a prerequisite to treatment. METHODS We extracted a cohort of NSCLC patients from the Surveillance, Epidemiology and End Results (SEER)-Medicare linked data. The primary outcome was receipt of a molecular diagnostic test, based on claims data. The primary predictors were race and SES. Likelihood of receiving a molecular diagnostic test, and overall survival (OS), were investigated using logistic and Cox proportional hazards regression, adjusted for sex, age, residence, histology, marital status, and comorbidity. RESULTS Of the 28,511 NSCLC patients, 11,209 (39.3%) received molecular diagnostic testing. Compared to White patients, fewer Black patients received a molecular diagnostic test (40.4% vs 27.9%; p < .001). After adjustment, Black patients (ORadj [odds ratio]: 0.64; 95% CI [confidence interval]: 0.58-0.71) and those living in areas with greater poverty (ORadj: 0.85; 95% CI: 0.80-0.89) had statistically significant decreased likelihood of molecular diagnostic testing. Patients who did receive testing had a statistically significant decreased risk of death (HRadj [hazards ratio]: 0.74; 95% CI: 0.72-0.76). These results held in the stratified analysis of stage IV NSCLC patients. CONCLUSION Disparities exist in comprehensive molecular diagnostics, which is critical for clinical decision making. Addressing barriers to molecular testing could help close gaps in cancer care and improve patient outcomes.
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