用重组人骨形态发生蛋白7治疗可在一部分患者中短暂诱导中和性自身抗体

Andrea Schuette , Arash Moghaddam , Petra Seemann , Georg N. Duda , Gerhard Schmidmaier , Lutz Schomburg
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引用次数: 6

摘要

背景:重组人骨形态发生蛋白7 (rhBMP7)被用于治疗骨折,尤其是胫骨骨不连。其应用可能诱导自身抗体(aAB)影响靶向和内源性信号通路,进而对治疗效果产生负面影响。方法建立新的、灵敏的BMP7-aAB和BMP2-aAB定量检测方法,并对健康对照(男性100例,女性100例)和未使用rhBMP7治疗或未使用rhBMP7治疗的长骨骨折患者(265例)血清进行分析。每位患者可获得3至9个时间点的血清,并可在长达一年的时间过程中评估aAB。BMP-aAB的功能活性通过bmp应答细胞报告试验进行检测。评估BMP7-aAB可能影响骨折巩固的临床结果。结果BMP7-aAB和BMP2-aAB在未治疗患者和健康对照中阳性率为1-2.5%。在一部分患者中,rhBMP7治疗导致BMP7-aAB短暂升高,并在6个月内恢复到无法检测到的水平。来自BMP7-aAB阳性血清的IgG对bmp7报告基因活性的抑制呈剂量依赖性,而对照血清对bmp7报告基因活性无影响。在大多数aab阳性和aab阴性患者中均观察到骨折的成功巩固。我们得出结论,BMP7-aAB可以在健康受试者中作为天然aAB检测到,并且在一部分患者中通过rhBMP7治疗可短暂诱导。aAB能够在体外拮抗BMP7信号,但不妨碍患者的治疗成功。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Treatment with recombinant human bone morphogenetic protein 7 leads to a transient induction of neutralizing autoantibodies in a subset of patients

Treatment with recombinant human bone morphogenetic protein 7 leads to a transient induction of neutralizing autoantibodies in a subset of patients

Background

Recombinant human bone morphogenetic protein 7 (rhBMP7) is applied for treatment of bone fractures, especially tibial non-unions. Its application may induce autoantibodies (aAB) affecting the targeted and endogenous signaling pathways and in turn negatively impact treatment efficacy.

Methods

Novel and sensitive assays for the quantification of BMP7-aAB and BMP2-aAB were established and used to analyze serum samples from healthy controls (n = 100 men, n = 100 women) and patients with long bone fracture (n = 265) treated or not with rhBMP7. Sera from three to nine time points per patient were available and enabled the evaluation of aAB over a time course of up to one year. Functional activity of the BMP-aAB was tested with a BMP-responsive cell-based reporter assay. Consolidation of the fracture was evaluated as clinical outcome potentially affected by BMP7-aAB.

Results

Prevalence of BMP7-aAB and BMP2-aAB was 1–2.5% in non-treated patients or healthy controls. The rhBMP7 treatment induced a transient increase in BMP7-aAB in a subset of patients, returning to non-detectable levels within six months. IgG from BMP7-aAB positive sera inhibited dose dependently the BMP7-reporter gene activity, whereas control sera were without effect. Successful consolidation of the fracture was observed in the majority of both aAB-positive and aAB-negative patients.

General significance

We conclude that BMP7-aAB can be detected as natural aAB in healthy subjects, and are transiently induced by rhBMP7 therapy in a subset of patients. The aAB are capable of antagonizing BMP7 signaling in vitro, but do not preclude treatment success in patients.

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