转移性黑色素瘤患者对伊匹单抗的敏感性不能通过肿瘤特征来预测。

IF 0.3 Q4 ONCOLOGY
Kara Rossfeld, Erinn M Hade, Alexandra Gangi, Matthew Perez, Emily N Kinsey, Joanna Grabska, Ashley Ederle, Jonathan Zager, April K Salama, Thomas E Olencki, Georgia M Beasley
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引用次数: 4

摘要

免疫检查点抑制剂极大地改变了转移性黑色素瘤患者的预后。然而,并非所有患者对治疗都有反应,毒性可能很严重,因此需要可靠的临床预测指标。方法:我们检查了随后发展为IV期疾病并在3家机构接受伊匹单抗治疗的患者的原发肿瘤特征,包括溃疡、BRAF突变状态和brreslow深度。本研究的患者未进行临床试验。为了研究患者诊断时的特征与黑色素瘤诊断后的生存之间的关系,我们使用Cox比例风险模型,考虑到延迟进入研究队列。Cox模型估计年龄和机构调整后的死亡风险风险比。结果:在接受ipilimumab治疗IV期黑色素瘤的患者(n=385)中,302例符合纳入标准。伊匹单抗完全缓解率为5%,部分缓解率为13%,疾病稳定率为18%,疾病进展率为62%,未知率为5%。中位总生存率为2.03年[95%可信区间(CI): 0.13, 3.05]。原发肿瘤brreslow深度、淋巴血管浸润、BRAF状态和溃疡不能预测对伊匹单抗的敏感性。在本研究患者队列中,BRAF突变(校正风险比:1.43,95% CI: 0.98, 2.07)和溃疡的存在(校正风险比:1.47,95% CI: 0.95, 2.26)导致死亡风险增加。结论:溃疡的存在与对伊匹单抗的敏感性无关。易普利姆单抗治疗的转移性黑色素瘤患者,原发肿瘤溃疡和BRAF突变与较差的生存率中度相关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Metastatic melanoma patients' sensitivity to ipilimumab cannot be predicted by tumor characteristics.

Metastatic melanoma patients' sensitivity to ipilimumab cannot be predicted by tumor characteristics.

Metastatic melanoma patients' sensitivity to ipilimumab cannot be predicted by tumor characteristics.

Metastatic melanoma patients' sensitivity to ipilimumab cannot be predicted by tumor characteristics.

Immune checkpoint inhibitors have dramatically changed the prognosis for patients with metastatic melanoma. However, not all patients respond to therapy and toxicities can be severe leaving need for reliable clinical predictive markers.

Methods: We examined primary tumor characteristics including ulceration, BRAF mutation status, and Breslow depth in patients who subsequently developed stage IV disease and were treated with ipilimumab at 3 institutions. Patients in this study were not treated on clinical trials. To investigate the relationship between patient characteristics at the time of diagnosis and survival following melanoma diagnosis we utilized Cox proportional hazards models, accounting for delayed entry into the study cohort. Cox models estimate the age and institution adjusted hazard ratios for risk of death.

Results: Of patients (n=385) treated with ipilimumab for stage IV melanoma, 302 met inclusion criteria. The complete response to ipilimumab was 5%, partial response was 13%, 18% had stable disease, 62% had progressive disease, and 5 unknown. The median overall survival rate was 2.03 years [95% confidence interval (CI): 0.13, 3.05]. Primary tumor Breslow depth, lymphovascular invasion, BRAF status, and ulceration did not predict sensitivity to ipilimumab. In this study patient cohort, BRAF mutation (adjusted hazard ratio: 1.43, 95% CI: 0.98, 2.07) and presence of ulceration (adjusted hazard ratio: 1.47, 95% CI: 0.95, 2.26) contributed to an increased risk of death.

Conclusions: The presence of ulceration did not correlate with sensitivity to ipilimumab. Ulceration of the primary tumor and a BRAF mutation were moderately associated with worse survival in patients with metastatic melanoma treated with ipilimumab.

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