优化igg降解酶治疗方案,增强腺相关病毒转导存在中和抗体

IF 4.6 2区 医学 Q2 IMMUNOLOGY Clinical & Translational Immunology Pub Date : 2022-02-24 DOI:10.1002/cti2.1375
Irene Ros-Ga?án, Mirja Hommel, Laia Trigueros-Motos, Blanche Tamarit, Estefanía Rodríguez-García, David Salas, Guiomar Pérez, Anne Douar, Jean Philippe Combal, Bernard Benichou, Veronica Ferrer, Gloria González-Aseguinolaza
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引用次数: 10

摘要

针对腺相关病毒(aav)的预先存在的中和抗体(nab)仍然是许多患者系统给予aav介导的基因治疗的障碍,各种策略正在研究中以克服这一限制。本研究测试了从链球菌属细菌中提取的IgG降解酶(Ides)切割人IgG的能力,并在已有nab的个体中允许aav介导的转导。方法测定3种ide在不同物种血清中的体外裂解活性。采用具有天然抗aav抗体的被动免疫小鼠或非人灵长类动物(NHP)来确定AAVAnc80和AAV8载体在小鼠体内和AAV3B在NHPs体内的最佳ide剂量和给药窗口。结果选择的IdeS对人IgG的裂解效率高,对NHP IgG的裂解效率低,对小鼠IgG的裂解效率低。在体内,我们观察到在nab存在的情况下,ide如何影响肝转导取决于AAV血清型的差异。对于AAVAnc80和AAV3B,当IgG消化产物从循环中清除后给予载体时,达到最佳转导水平。然而,对于AAV8,我们只观察到IdeS切割产物对转导的适度和短暂的抑制。结论:对于因循环抗aav NAb水平升高而被排除在基因治疗临床试验之外的患者,ide预处理是一种独特的治疗机会。然而,仔细确定每种AAV血清型的最佳ide剂量和给药时间对于最佳转导至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Optimising the IgG-degrading enzyme treatment regimen for enhanced adeno-associated virus transduction in the presence of neutralising antibodies

Objective

Pre-existing neutralising antibodies (NAbs) to adeno-associated viruses (AAVs) remain an impediment for systemically administered AAV-mediated gene therapy treatment in many patients, and various strategies are under investigation to overcome this limitation. Here, IgG-degrading enzymes (Ides) derived from bacteria of the genus Streptococcus were tested for their ability to cleave human IgG and allow AAV-mediated transduction in individuals with pre-existing NAbs.

Methods

Cleavage activity of three different Ides was evaluated in vitro in serum from different species. Passively immunised mice or non-human primates (NHP) with naturally occurring anti-AAV NAbs were used to define the optimal IdeS dose and administration window for AAVAnc80 and AAV8 vectors in mice and AAV3B in NHPs.

Results

The selected candidate, IdeS, was found to be highly efficient at cleaving human IgG, less efficient against NHP IgG and inefficient against mouse IgG. In vivo, we observed differences in how IdeS affected liver transduction in the presence of NAbs depending on the AAV serotype. For AAVAnc80 and AAV3B, the best transduction levels were achieved when the vector was administered after IgG digestion products were cleared from circulation. However, for AAV8 we only observed a modest and transient inhibition of transduction by IdeS cleavage products.

Conclusion

Preconditioning with IdeS represents a unique treatment opportunity for patients primarily excluded from participation in gene therapy clinical trials because of elevated circulating anti-AAV NAb levels. However, careful determination of the optimal IdeS dose and timing for the administration of each AAV serotype is essential for optimal transduction.

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来源期刊
Clinical & Translational Immunology
Clinical & Translational Immunology Medicine-Immunology and Allergy
CiteScore
12.00
自引率
1.70%
发文量
77
审稿时长
13 weeks
期刊介绍: Clinical & Translational Immunology is an open access, fully peer-reviewed journal devoted to publishing cutting-edge advances in biomedical research for scientists and physicians. The Journal covers fields including cancer biology, cardiovascular research, gene therapy, immunology, vaccine development and disease pathogenesis and therapy at the earliest phases of investigation.
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