外周血 T 细胞受体库作为 PD-1 抑制剂治疗胃肠道癌患者临床结局的预测指标。
Peripheral blood T-cell receptor repertoire as a predictor of clinical outcomes in gastrointestinal cancer patients treated with PD-1 inhibitor.
机构信息
Academy of Military Medical Sciences, Academy of Military Sciences, Beijing, China.
Department of Gastrointestinal Oncology, The Fifth Medical Centre, Chinese PLA General Hospital, No. 8 East Street, Fengtai District, Beijing, 100071, China.
出版信息
Clin Transl Oncol. 2021 Aug;23(8):1646-1656. doi: 10.1007/s12094-021-02562-4. Epub 2021 Feb 13.
BACKGROUND
Identifying valid biomarkers for patient selection impressively promotes the success of anti-PD-1 therapy. However, the unmet need for biomarkers in gastrointestinal (GI) cancers remains significant. We aimed to explore the predictive value of the circulating T-cell receptor (TCR) repertoire for clinical outcomes in GI cancers who received anti-PD-1 therapy.
METHODS
137 pre- and 79 post-treated peripheral blood samples were included. The TCR repertoire was evaluated by sequencing of complementarity-determining region 3 (CDR3) in the TRB gene. The Shannon index was used to measure the diversity of the TCR repertoire, and Morisita's overlap index was used to determine TCR repertoire similarities between pre- and post-treated samples.
RESULTS
Among all enrolled patients, 76 received anti-PD-1 monotherapy and 61 received anti-PD-1 combination therapy. In the anti-PD-1 monotherapy cohort, patients with higher baseline TCR diversity exhibited a significantly higher disease control rate (77.8% vs. 47.2%; hazard ratio [HR] 3.92; 95% confidence interval [CI] 1.14-13.48; P = 0.030) and a longer progression-free survival (PFS) (median: 6.47 months vs. 2.77 months; HR 2.10; 95% CI 1.16-3.79; P = 0.014) and overall survival (OS) (median: NA vs. 8.97 months; HR 3.53; 95% CI 1.49-8.38; P = 0.004) than those with lower diversity. Moreover, patients with a higher TCR repertoire similarity still showed a superior PFS (4.43 months vs. 1.84 months; HR 13.98; 95% CI 4.37-44.68; P < 0.001) and OS (13.40 months vs. 6.12 months; HR 2.93; 95% CI 1.22-7.03; P = 0.016) even in the cohort with lower baseline diversity. However, neither biomarker showed predictive value in the anti-PD-1 combination therapy cohort. Interestingly, the combination of TCR diversity and PD-L1 expression can facilitate patient stratification in a pooled cohort.
CONCLUSION
The circulating TCR repertoire can serve as a predictor of clinical outcomes in anti-PD-1 therapy in GI cancers.
背景
识别有效的生物标志物来选择患者可以显著提高抗 PD-1 治疗的成功率。然而,胃肠道(GI)癌症对生物标志物的需求仍未得到满足。我们旨在探索循环 T 细胞受体(TCR)谱对抗 PD-1 治疗的 GI 癌症患者临床结局的预测价值。
方法
纳入了 137 例治疗前和 79 例治疗后外周血样本。通过 TRB 基因中互补决定区 3(CDR3)的测序来评估 TCR 谱。Shannon 指数用于测量 TCR 谱的多样性,Morisita 的重叠指数用于确定治疗前和治疗后样本之间 TCR 谱的相似性。
结果
在所有入组患者中,76 例接受了抗 PD-1 单药治疗,61 例接受了抗 PD-1 联合治疗。在抗 PD-1 单药治疗队列中,基线 TCR 多样性较高的患者疾病控制率显著更高(77.8% vs. 47.2%;风险比[HR]3.92;95%置信区间[CI]1.14-13.48;P=0.030),无进展生存期(PFS)更长(中位数:6.47 个月 vs. 2.77 个月;HR 2.10;95%CI 1.16-3.79;P=0.014)和总生存期(OS)更长(中位数:NA vs. 8.97 个月;HR 3.53;95%CI 1.49-8.38;P=0.004)。此外,TCR 谱相似性较高的患者仍表现出更优的 PFS(4.43 个月 vs. 1.84 个月;HR 13.98;95%CI 4.37-44.68;P<0.001)和 OS(13.40 个月 vs. 6.12 个月;HR 2.93;95%CI 1.22-7.03;P=0.016),即使在基线多样性较低的队列中也是如此。然而,这两种生物标志物在抗 PD-1 联合治疗队列中均没有预测价值。有趣的是,TCR 多样性和 PD-L1 表达的组合可以促进汇总队列中患者的分层。
结论
循环 TCR 谱可作为 GI 癌症抗 PD-1 治疗临床结局的预测指标。
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