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去除循环抗体的衣壳特异性腺相关病毒载体。

Capsid-specific removal of circulating antibodies to adeno-associated virus vectors.

机构信息

Genethon and INSERM U951, 1 rue de l'internationale, 91000, Evry, France.

Atlantic Gene Therapies, Centre de Boisbonne, ONIRIS, La Chantrerie, BP 40706, 44307, Nantes, France.

出版信息

Sci Rep. 2020 Jan 21;10(1):864. doi: 10.1038/s41598-020-57893-z.

Abstract

Neutralizing antibodies directed against adeno-associated virus (AAV) are commonly found in humans. In seropositive subjects, vector administration is not feasible as antibodies neutralize AAV vectors even at low titers. Consequently, a relatively large proportion of humans is excluded from enrollment in clinical trials and, similarly, vector redosing is not feasible because of development of high-titer antibodies following AAV vector administration. Plasmapheresis has been proposed as strategy to remove anti-AAV antibodies from the bloodstream. Although safe and relatively effective, the technology has some limitations mainly related to the nonspecific removal of all circulating IgG. Here we developed an AAV-specific plasmapheresis column which was shown to efficiently and selectively deplete anti-AAV antibodies without depleting the total immunoglobulin pool from plasma. We showed the nearly complete removal of anti-AAV antibodies from high titer purified human IgG pools and plasma samples, decreasing titers to levels that allow AAV vector administration in mice. These results provide proof-of-concept of a method for the AAV-specific depletion of neutralizing antibodies in the setting of in vivo gene transfer.

摘要

针对腺相关病毒 (AAV) 的中和抗体在人类中很常见。在血清阳性的受试者中,由于抗体甚至在低滴度时就能中和 AAV 载体,因此载体给药是不可行的。因此,相当一部分人被排除在临床试验之外,同样,由于 AAV 载体给药后会产生高滴度的抗体,因此也不可能进行载体再给药。已经提出了血浆置换作为从血液中去除抗 AAV 抗体的策略。尽管该技术安全且相对有效,但也存在一些限制,主要与非特异性去除所有循环 IgG 有关。在这里,我们开发了一种 AAV 特异性血浆置换柱,该柱被证明能够有效地、选择性地去除抗 AAV 抗体,而不会从血浆中耗尽总免疫球蛋白池。我们表明,从高滴度纯化的人 IgG 池和血浆样本中几乎完全去除了抗 AAV 抗体,将滴度降低到允许在小鼠中给予 AAV 载体的水平。这些结果为在体内基因转移的情况下针对中和抗体的 AAV 特异性耗尽提供了概念验证。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/15f0/6972890/583e904d3483/41598_2020_57893_Fig1_HTML.jpg

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