Evaluating Anticoagulant and Antiplatelet Therapies in Rhesus and Cynomolgus Macaques for Predictive Modeling in Humans

Surgeries Pub Date : 2024-05-17 DOI:10.3390/surgeries5020035
Sydney N. Phu, David J. Leishman, Sierra D. Palmer, S. Oppler, Melanie N. Niewinski, Lucas A. Mutch, Jill S. Faustich, Andrew B. Adams, Robert T. Tranquillo, Melanie L. Graham
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Abstract

Anticoagulant and antiplatelet therapies are used to prevent life-threatening complications associated with thrombosis. While there are numerous clinical guidelines for antithrombotic medications, there is an incomplete understanding of whether these interventions yield similar effects in preclinical models, potentially impacting their predictive value for translational studies on the development of medical devices, therapies, and surgical techniques. Due to their close physiologic similarities to humans, we employed nonhuman primates (NHPs) using a reverse translational approach to analyze the response to clinical regimens of unfractionated heparin, low-molecular-weight heparin (LMWH) and aspirin to assess concordance with typical human responses and evaluate the predictive validity of this model. We evaluate activated clotting time (ACT) in nine rhesus and six cynomolgus macaques following the intraoperative administration of intravenous unfractionated heparin (100–300 U/kg) reflecting the clinical dose range. We observed a significant dose-dependent effect of heparin on ACT (low-dose average = 114.1 s; high-dose average = 148.3 s; p = 0.0011). LMWH and aspirin, common clinical antithrombotic prophylactics, were evaluated in three rhesus macaques. NHPs achieved therapeutic Anti-Xa levels (mean = 0.64 U/mL) and ARU (mean = 459) via VerifyNow, adhering to clinical guidance using 1.0 mg/kg enoxaparin and 81 mg aspirin. Clinical dosing strategies for unfractionated heparin, LMWH, and aspirin were safe and effective in NHPs, with no development of thrombosis or bleeding complications intraoperatively, postoperatively, or for prophylaxis. Our findings suggest that coagulation studies, performed as an integrative part of studies on biologics, bioengineered devices, or transplantation in NHPs, can be extrapolated to the clinical situation with high predictive validity.
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评估恒河猴和猕猴的抗凝剂和抗血小板疗法,为人类建立预测模型
抗凝剂和抗血小板疗法用于预防与血栓形成有关的危及生命的并发症。虽然抗血栓药物有许多临床指南,但人们对这些干预措施是否在临床前模型中产生类似效果的了解并不全面,这可能会影响它们对医疗设备、疗法和手术技术开发转化研究的预测价值。由于非人灵长类动物(NHPs)在生理上与人类非常相似,因此我们采用反向转化的方法来分析它们对非减量肝素、低分子量肝素(LMWH)和阿司匹林的临床治疗方案的反应,以评估它们与人类典型反应的一致性,并评估该模型的预测有效性。我们评估了 9 只恒河猴和 6 只猕猴在术中静脉注射反映临床剂量范围的非减量肝素(100-300 U/kg)后的活化凝血时间(ACT)。我们观察到肝素对 ACT 有明显的剂量依赖效应(低剂量平均 = 114.1 秒;高剂量平均 = 148.3 秒;p = 0.0011)。临床常用的抗血栓预防药物 LMWH 和阿司匹林在三只猕猴身上进行了评估。根据临床指导,使用 1.0 毫克/千克依诺肝素和 81 毫克阿司匹林,NHP 通过 VerifyNow 达到了治疗性 Anti-Xa 水平(平均 = 0.64 U/mL)和 ARU(平均 = 459)。非分叶肝素、LMWH 和阿司匹林的临床给药策略对 NHP 安全有效,术中、术后或预防性用药均未出现血栓或出血并发症。我们的研究结果表明,凝血研究是生物制剂、生物工程设备或移植研究的重要组成部分,可以将其应用于临床,并具有很高的预测效力。
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