Inclusion of a degron reduces levelsof undesired inteins after AAV-mediated proteintrans-splicing in the retina.

Molecular Therapy. Methods & Clinical Development Pub Date : 2021-10-19 eCollection Date: 2021-12-10 DOI:10.1016/j.omtm.2021.10.004

Patrizia Tornabene, Ivana Trapani, Miriam Centrulo, Elena Marrocco, Renato Minopoli, Mariangela Lupo, Carolina Iodice, Carlo Gesualdo, Francesca Simonelli, Enrico M Surace, Alberto Auricchio

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引用次数: 9

Abstract

Split intein-mediated protein trans-splicing expands AAV transfer capacity, thus overcoming the limited AAV cargo. However, non-mammalian inteins persist as trans-splicing by-products, and this could raise safety concerns for AAV intein clinical applications. In this study, we tested the ability of several degrons to selectively decrease levels of inteins after protein trans-splicing and found that a version of E. coli dihydrofolate reductase, which we have shortened to better fit into the AAV vector, is the most effective. We show that subretinal administration of AAV intein armed with this short degron is both safe and effective in a mouse model of Stargardt disease (STGD1), which is the most common form of inherited macular degeneration in humans. This supports the use of optimized AAV intein for gene therapy of both STGD1 and other conditions that require transfer of large genes.

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在aav介导的视网膜蛋白反式剪接后，degron的包含降低了不需要的蛋白水平。

分裂间质介导的蛋白质反式剪接扩大了AAV的转运能力，从而克服了AAV载货量有限的问题。然而，非哺乳动物肠道蛋白仍然是反式剪接的副产物，这可能会引起AAV在临床应用中的安全性问题。在这项研究中，我们测试了几个degrons在蛋白质反式剪接后选择性降低干扰素水平的能力，发现大肠杆菌二氢叶酸还原酶的一个版本是最有效的，我们已经缩短了它，以更好地适应AAV载体。我们发现，在Stargardt病(STGD1)小鼠模型中，视网膜下给药带有这种短degron的AAV既安全又有效，STGD1是人类遗传性黄斑变性最常见的形式。这支持将优化的AAV蛋白用于STGD1和其他需要转移大基因的疾病的基因治疗。

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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Molecular Therapy. Methods & Clinical Development

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