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Recombinant Production of MFHR1 A Novel Synthetic Multitarget Complement Inhibitor in Moss Bioreactors

机译:在苔藓生物反应器中重组生产MFHR1一种新型的合成多靶补体抑制剂

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摘要

The human complement system is an important part of the immune system responsible for lysis and elimination of invading microorganisms and apoptotic body cells. Improper activation of the system due to deficiency, mutations, or autoantibodies of complement regulators, mainly factor H (FH) and FH-related proteins (FHRs), causes severe kidney and eye diseases. However, there is no recombinant FH therapeutic available on the market. The first successful recombinant production of FH was accomplished with the moss bioreactor, Physcomitrella patens. Recently, a synthetic regulator, MFHR1, was designed to generate a multitarget complement inhibitor that combines the activities of FH and the FH-related protein 1 (FHR1). The potential of MFHR1 was demonstrated in a proof-of-concept study with transiently transfected insect cells. Here, we present the stable production of recombinant glyco-engineered MFHR1 in the moss bioreactor. The key features of this system are precise genome engineering via homologous recombination, Good Manufacturing Practice-compliant production in photobioreactors, high batch-to-batch reproducibility, and product stability. Several potential biopharmaceuticals are being produced in this system. In some cases, these are even biobetters, i.e., the recombinant proteins produced in moss have a superior quality compared to their counterparts from mammalian systems as for example moss-made aGal, which successfully passed phase I clinical trials. Via mass spectrometry-based analysis of moss-produced MFHR1, we now prove the correct synthesis and modification of this glycoprotein with predominantly complex-type N-glycan attachment. Moss-produced MFHR1 exhibits cofactor and decay acceleration activities comparable to FH, and its mechanism of action on multiple levels within the alternative pathway of complement activation led to a strong inhibitory activity on the whole alternative pathway, which was higher than with the physiological regulator FH.
机译:人补体系统是免疫系统的重要组成部分,负责溶解和消除入侵的微生物和凋亡的体细胞。由于补体调节因子(主要是因子H(FH)和FH相关蛋白(FHRs))的缺乏,突变或自身抗体引起的系统激活不当,会导致严重的肾脏和眼睛疾病。但是,市场上没有重组FH治疗剂。 FH的首次成功重组生产是通过苔藓生物反应器Physcomitrella patens完成的。最近,设计了一种合成调节剂MFHR1,以产生结合了FH和FH相关蛋白1(FHR1)活性的多靶补体抑制剂。瞬时转染昆虫细胞的概念验证研究证明了MFHR1的潜力。在这里,我们介绍了在苔藓生物反应器中重组糖工程化MFHR1的稳定生产。该系统的关键功能是通过同源重组进行精确的基因组工程,在光生物反应器中进行符合Good Manufacturing Practice要求的生产,批次间的高可重复性以及产品稳定性。该系统正在生产几种潜在的生物药物。在某些情况下,它们甚至是生物促进剂,即,与通过哺乳动物系统生产的重组蛋白(例如通过苔藓制造的aGal)成功通过I期临床试验的结果相比,在苔藓中产生的重组蛋白具有更高的质量。通过基于质谱的苔藓生产MFHR1的分析,我们现在证明这种糖蛋白的合成和修饰正确,且主要具有复杂的N型聚糖连接。苔藓产生的MFHR1具有与FH相当的辅因子和衰变加速活性,其在补体激活的替代途径内在多个水平上的作用机理导致了对整个替代途径的强烈抑制活性,高于生理调节剂FH 。

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