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治疗性抗体在肿瘤和肿瘤引流淋巴结中的药代动力学和药效学。

Pharmacokinetics and pharmacodynamics of therapeutic antibodies in tumors and tumor-draining lymph nodes.

机构信息

Division of Pharmacotherapy and Experimental Therapeutics, UNC Eshelman School of Pharmacy, University of North Carolina, Chapel Hill, NC, USA.

Lineberger Comprehensive Cancer Center, School of Medicine, University of North Carolina at Chapel Hill, NC, USA.

出版信息

Math Biosci Eng. 2020 Nov 19;18(1):112-131. doi: 10.3934/mbe.2021006.

Abstract

The signaling axis from the primary tumor to the tumor-draining lymph node (TDLN) has emerged as a crucial mediator for the efficacy of immunotherapies in neoadjuvant settings, challenging the primary use of immunotherapy in adjuvant settings. TDLNs are regarded as highly opportunistic sites for cancer cell dissemination and promote further spread via several primary tumor-dependent mechanisms. Lesion-level mixed responses to antibody immunotherapy have been traced to local immune signatures present in the TDLN and the organ-specific primary tumors that they drain. However, the pharmacokinetics (PK) and biodistribution gradients of antibodies in primary tumors and TDLNs have not been systemically evaluated. These concentration gradients are critical in ensuring adequate antibody pharmacodynamic (PD) T-cell activation and/or anti-tumor response. The current work reviews the knowledge for developing physiologically-based PK and pharmacodynamic (PBPK/PD) models to quantify antibody biodistribution gradients in anatomically distinct primary tumors and TDLNs as a means to characterize the clinically observed heterogeneous responses to antibody therapies. Several clinical and pathophysiological considerations in modeling the primary tumor-TDLN axis, as well as a summary of both preclinical and clinical PK/PD lymphatic antibody disposition studies, will be provided.

摘要

原发肿瘤到引流淋巴结(TDLN)的信号轴已成为新辅助治疗中免疫治疗疗效的重要介导因素,这对免疫治疗在辅助治疗中的主要应用提出了挑战。TDLN 被认为是癌细胞扩散的高度机会性部位,并通过几种依赖原发肿瘤的机制促进进一步扩散。抗体免疫治疗的病变水平混合反应可追溯到 TDLN 和它们引流的器官特异性原发肿瘤中存在的局部免疫特征。然而,抗体在原发肿瘤和 TDLN 中的药代动力学(PK)和生物分布梯度尚未得到系统评估。这些浓度梯度对于确保足够的抗体药效学(PD)T 细胞激活和/或抗肿瘤反应至关重要。目前的工作综述了开发基于生理的 PK 和药效学(PBPK/PD)模型的知识,以定量分析解剖上不同的原发肿瘤和 TDLN 中抗体的生物分布梯度,作为一种表征临床观察到的抗体治疗异质性反应的方法。将提供在建模原发肿瘤-TDLN 轴时的一些临床和病理生理学考虑因素,以及对临床前和临床 PK/PD 淋巴抗体处置研究的总结。

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