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在接受免疫检查点抑制剂治疗的转移性恶性黑色素瘤患者中,使用Xa因子抑制剂进行抗凝治疗与总体缓解率提高和无进展生存期延长相关——一项回顾性真实世界队列研究。

Anticoagulation with Factor Xa Inhibitors Is Associated with Improved Overall Response and Progression-Free Survival in Patients with Metastatic Malignant Melanoma Receiving Immune Checkpoint Inhibitors-A Retrospective, Real-World Cohort Study.

作者信息

Haist Maximilian, Stege Henner, Pemler Saskia, Heinz Jaqueline, Fleischer Maria Isabel, Graf Claudine, Ruf Wolfram, Loquai Carmen, Grabbe Stephan

机构信息

Department of Dermatology, University Medical Center of the Johannes-Gutenberg University Mainz, 55131 Mainz, Germany.

Center for Thrombosis and Hemostasis, University Medical Center of the Johannes-Gutenberg University Mainz, 55131 Mainz, Germany.

出版信息

Cancers (Basel). 2021 Oct 12;13(20):5103. doi: 10.3390/cancers13205103.

Abstract

Immune checkpoint inhibitors (ICI) significantly improved the prognosis of advanced melanoma patients. However, many patients do not derive long-term benefit from ICI therapy due to primary and acquired resistance. In this regard, it has been shown that coagulation factors contribute to cancer immune evasion and might therefore promote resistance to ICI. In particular, recent observations in murine systems demonstrated that myeloid-derived factor Xa (FXa) impedes anti-tumor immunity in the tumor microenvironment and that the oral FXa inhibitor (FXa-i) rivaroxaban synergizes with ICI. The synergistic effect of FXa inhibitors with clinical ICI therapy is unknown. We performed a retrospective study of 280 metastatic melanoma patients who were treated with ICI and stratified them for concomitant anticoagulation (AC) by medical chart review. Data on baseline patient characteristics, specific AC treatment, ICI therapy, other tumor-targeting therapies, and clinical outcomes were analyzed. Of 280 patients who received ICI, 76 received concomitant AC during initial ICI therapy. Patients on AC were treated either with heparins ( = 29), vitamin K antagonists (VKA) ( = 20), or FXa-i ( = 27). Patients requiring AC during ICI therapy showed no significantly reduced objective response rate (ORR) ( = 0.27), or progression-free (PFS; median PFS 4 vs. 4 months; = 0.71) or overall survival (OS; median OS: 39 vs. 51 months; = 0.31). Furthermore, patients who underwent AC did not show significantly more bleeding complications ( = 0.605) than those who were not anticoagulated. Remarkably, stratification of patients by the class of AC revealed that patients receiving FXa-i were more likely to obtain CR (26.9 vs. 12.6%, = 0.037), and showed better ORR (69.2 vs. 36.4%, = 0.005), PFS (median PFS: 12 months vs. 3 months; = 0.006), and OS (median OS not reached vs. 42 months; = 0.09) compared to patients not receiving FXa-i. Patient demographics and tumor characteristics in this patient subcohort did not significantly differ from patients not on FXa-i. In summary, our study provides first clinical evidence that the clinical application of FXa-i may enhance the efficacy of ICI therapy via the restoration of anti-tumor immunity, while patients who received FXa-i were not more likely to encounter bleeding complications.

摘要

免疫检查点抑制剂(ICI)显著改善了晚期黑色素瘤患者的预后。然而,由于原发性和获得性耐药,许多患者无法从ICI治疗中获得长期益处。在这方面,已有研究表明凝血因子有助于癌症免疫逃逸,因此可能促进对ICI的耐药性。特别是,最近在小鼠模型中的观察表明,髓系衍生的因子Xa(FXa)会阻碍肿瘤微环境中的抗肿瘤免疫,而口服FXa抑制剂(FXa-i)利伐沙班可与ICI协同作用。FXa抑制剂与临床ICI治疗的协同效应尚不清楚。我们对280例接受ICI治疗的转移性黑色素瘤患者进行了一项回顾性研究,并通过病历审查对他们是否同时接受抗凝治疗(AC)进行了分层。分析了患者的基线特征、特定的AC治疗、ICI治疗、其他肿瘤靶向治疗以及临床结局的数据。在280例接受ICI治疗的患者中,76例在初始ICI治疗期间同时接受了AC。接受AC治疗的患者分别使用肝素(n = 29)、维生素K拮抗剂(VKA)(n = 20)或FXa-i(n = 27)进行治疗。在ICI治疗期间需要AC的患者,其客观缓解率(ORR)没有显著降低(P = 0.27),无进展生存期(PFS;中位PFS分别为4个月和4个月;P = 0.71)或总生存期(OS;中位OS分别为39个月和51个月;P = 0.31)。此外,接受AC治疗的患者与未接受抗凝治疗的患者相比,出血并发症并没有显著增加(P = 0.605)。值得注意的是,根据AC类别对患者进行分层后发现,接受FXa-i治疗的患者更有可能获得完全缓解(CR)(26.9%对12.6%,P = 0.037),并且与未接受FXa-i治疗的患者相比,表现出更好的ORR(69.2%对36.4%,P = 0.005)、PFS(中位PFS:12个月对3个月;P = 0.006)和OS(中位OS未达到对42个月;P = 0.09)。该亚组患者的人口统计学特征和肿瘤特征与未接受FXa-i治疗的患者没有显著差异。总之,我们的研究提供了首个临床证据,即FXa-i的临床应用可能通过恢复抗肿瘤免疫来增强ICI治疗的疗效,同时接受FXa-i治疗的患者发生出血并发症的可能性并不更高。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/07d4/8534137/c8890adbdd28/cancers-13-05103-g001.jpg

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