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评价重组凝血因子 IX Fc 融合蛋白在动物体内的毒理学、药代动力学和局部耐受性。

Evaluation of the toxicology, pharmacokinetics, and local tolerance of recombinant factor IX Fc fusion protein in animals.

机构信息

Biogen Idec, Cambridge, MA, USA.

出版信息

Thromb Res. 2015 Aug;136(2):371-8. doi: 10.1016/j.thromres.2015.01.020. Epub 2015 Jan 23.

DOI:10.1016/j.thromres.2015.01.020
PMID:25840744
Abstract

INTRODUCTION

Recombinant factor IX Fc fusion protein (rFIXFc) is a recombinant coagulation factor composed of a single molecule of recombinant factor IX (rFIX) covalently fused to the Fc domain of human immunoglobulin G1 (IgG1) with no intervening sequence. An extensive nonclinical program was performed to support the clinical development of rFIXFc for treatment of people with hemophilia B.

MATERIALS AND METHODS

Repeat-dose toxicology studies of rFIXFc were performed in 2 relevant species: Sprague Dawley rats (4-week study) and cynomolgus monkeys (5- and 27-week studies). Assessments included in-life observations, electrocardiograms (monkeys only), laboratory evaluations (including hematology and blood chemistry), postmortem analyses, local tolerance, and pharmacokinetics (PK). Allometric scaling was performed with PK data from multiple species, including humans. Local tolerance (single-dose study) and thrombogenic potential (Wessler stasis model) of rFIXFc were tested in New Zealand White rabbits.

RESULTS

There were no significant local or systemic toxicity findings in the repeat-dose studies. Allometric scaling data suggested that animal rFIXFc PK results are predictive of human PK parameters. There were no findings from the local tolerance study in rabbits; thrombogenic activity was less than that elicited by rFIX and a prothrombin complex concentrate, and similar to vehicle control.

CONCLUSIONS

rFIXFc was well tolerated in toxicology studies and demonstrated a low thrombogenic potential. These results are consistent with phase 1/2a and phase 3 clinical studies of rFIXFc in people with hemophilia B.

摘要

简介

重组凝血因子 IX Fc 融合蛋白(rFIXFc)是一种由单个重组凝血因子 IX(rFIX)分子与人类免疫球蛋白 G1(IgG1)的 Fc 结构域通过无间隔序列共价融合而成的重组凝血因子。为了支持 rFIXFc 治疗乙型血友病患者的临床开发,进行了广泛的非临床研究计划。

材料和方法

在 2 种相关物种中进行了 rFIXFc 的重复剂量毒性研究:Sprague Dawley 大鼠(4 周研究)和食蟹猴(5 周和 27 周研究)。评估包括在体观察、心电图(仅猴子)、实验室评估(包括血液学和血液化学)、尸检、局部耐受性和药代动力学(PK)。使用来自多个物种(包括人类)的 PK 数据进行了同种异体缩放。在新西兰白兔中测试了 rFIXFc 的局部耐受性(单次剂量研究)和血栓形成潜力(Wessler 停滞模型)。

结果

在重复剂量研究中,没有发现明显的局部或全身毒性。同种异体缩放数据表明,动物 rFIXFc PK 结果可预测人类 PK 参数。在兔子的局部耐受性研究中没有发现任何发现;血栓形成活性低于 rFIX 和凝血酶原复合物浓缩物引起的活性,与载体对照相似。

结论

rFIXFc 在毒理学研究中耐受性良好,血栓形成潜力低。这些结果与乙型血友病患者的 rFIXFc 1/2a 期和 3 期临床研究一致。

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