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抗凝血因子 XI 反义寡核苷酸抑制物延长 APTT 而不增加食蟹猴出血风险。

Antisense inhibition of coagulation factor XI prolongs APTT without increased bleeding risk in cynomolgus monkeys.

机构信息

Preclinical Development, ISIS Pharmaceuticals, Carlsbad, CA, USA.

出版信息

Blood. 2012 Mar 8;119(10):2401-8. doi: 10.1182/blood-2011-10-387134. Epub 2012 Jan 13.

DOI:10.1182/blood-2011-10-387134
PMID:22246038
Abstract

A strategy to produce sufficient anticoagulant properties with reduced risk of bleeding may be possible through inhibition of factor XI (FXI), a component of the intrinsic coagulation cascade. The objective of this work was to determine the safety profile of ISIS 416858, a 2'-methoxyethoxy (2'-MOE) antisense oligonucleotide inhibitor of FXI, with focus on assessment of bleeding risk. Cynomolgus monkeys administered ISIS 416858 (4, 8, 12, and 40 mg/kg/wk, subcutaneous) for up to 13 weeks produced a dose-dependent reduction in FXI (mRNA in liver and plasma activity) and a concomitant increase in activated partial thromboplastin time (APTT). ISIS 416858 (20 or 40 mg/kg/wk) reduced plasma FXI activity by 80% at 4 weeks of treatment that resulted in a 33% increase in APTT by 13 weeks with no effects on PT, platelets, or increased bleeding following partial tail amputation or gum and skin laceration. The dose-dependent presence of basophilic granules in multiple tissues in ISIS 416858-treated animals was an expected histologic change for a 2'-MOE antisense oligonucleotide, and no toxicity was attributed to hepatic FXI reduction. Basophilic granules reflect cellular drug uptake and subsequent visualization on hematoxylin staining. These results suggest that ISIS 416858 has an acceptable preclinical safety profile and is a promising clinical candidate to treat thrombotic disease.

摘要

通过抑制因子 XI(FXI),一种内在凝血级联的组成部分,可能会产生具有降低出血风险的足够抗凝特性的策略。这项工作的目的是确定 ISIS 416858 的安全性概况,ISIS 416858 是一种 FXI 的 2'-甲氧基乙氧基(2'-MOE)反义寡核苷酸抑制剂,重点评估出血风险。接受 ISIS 416858(4、8、12 和 40 mg/kg/周,皮下)治疗长达 13 周的食蟹猴导致 FXI(肝和血浆活性中的 mRNA)剂量依赖性降低,同时激活部分凝血活酶时间(APTT)增加。ISIS 416858(20 或 40 mg/kg/周)在治疗 4 周时将血浆 FXI 活性降低 80%,导致 APTT 在 13 周时增加 33%,而对 PT、血小板或部分尾巴截肢或牙龈和皮肤裂伤后无出血增加无影响。在 ISIS 416858 治疗动物的多种组织中出现的嗜碱性颗粒是 2'-MOE 反义寡核苷酸的预期组织学变化,并且没有将肝 FXI 减少归因于毒性。嗜碱性颗粒反映了细胞摄取药物,随后在苏木精染色上可视化。这些结果表明,ISIS 416858具有可接受的临床前安全性概况,是治疗血栓性疾病的有前途的临床候选药物。

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