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解析:这段英文文本中,出现了专业词汇,“Characterization”,意思是“特性描述”;“Adeno-Associated Virus”,意思是“腺相关病毒”;“Capsid”,意思是“衣壳”;“Receptor”,意思是“受体”;“Antigenicity”,意思是“抗原性”。 因此,译文为: 蛇形腺相关病毒(SAAV)衣壳结构的特征描述:受体相互作用和抗原性。

Characterization of the Serpentine Adeno-Associated Virus (SAAV) Capsid Structure: Receptor Interactions and Antigenicity.

机构信息

University of Floridagrid.15276.37, Department of Biochemistry & Molecular Biology, Gainesville, Florida, USA.

NRS-Institut Armand Frappier, Université du Québec, Laval, Quebec, Canada.

出版信息

J Virol. 2022 Jun 8;96(11):e0033522. doi: 10.1128/jvi.00335-22. Epub 2022 May 9.

Abstract

Adeno-associated viruses (AAVs) are being developed as clinical gene therapy vectors. One issue undermining their broad use in the clinical setting is the high prevalence of circulating antibodies in the general population capable of neutralizing AAV vectors. Hence, there is a need for AAV vectors that can evade the preexisting immune response. One possible source of human naive vectors are AAVs that do not disseminate in the primate population, and one such example is serpentine AAV (SAAV). This study characterizes the structural and biophysical properties of the SAAV capsid and its receptor interactions and antigenicity. Single particle cryo-electron microscopy (cryo-EM) and thermal stability studies were conducted to characterize the SAAV capsid structure at pH 7.4, 6.0, 5.5, and 4.0, conditions experienced during cellular trafficking. Cell binding assays using Chinese hamster ovary (CHO) cell lines identified terminal sialic acid as the primary attachment receptor for SAAV similar to AAV1, 4, 5, and 6. The binding site of sialic acid to the SAAV capsid was mapped near the 2-fold axis toward the 2/5-fold wall, in a different location than AAV1, 4, 5, and 6. Towards determining the SAAV capsid antigenicity native immunodot blots showed that SAAV evades AAV serotype-specific mouse monoclonal antibodies. However, despite its reptilian origin, it was recognized by ~25% of 50 human sera tested, likely due to the presence of cross-reactive antibodies. These findings will inform future gene delivery applications using SAAV-based vectors and further aid the structural characterization and annotation of the repertoire of available AAV capsids. AAVs are widely studied therapeutic gene delivery vectors. However, preexisting antibodies and their detrimental effect on therapeutic efficacy are a primary challenge encountered during clinical trials. In order to circumvent preexisting neutralizing antibodies targeting mammalian AAV capsids, serpentine AAV (SAAV) was evaluated as a potential alternative to existing mammalian therapeutic vectors. The SAAV capsid was found to be thermostable at a wide range of environmental pH conditions, and its structure showed conservation of the core capsid topology but displays high structural variability on the surface. At the same time, it binds to a common receptor, sialic acid, that is also utilized by other AAVs already being utilized in gene therapy trials. Contrary to the initial hypothesis, SAAV capsids were recognized by one in four human sera tested, pointing to conserved amino acids around the 5-fold region as epitopes for cross-reacting antibodies.

摘要

腺相关病毒 (AAV) 正被开发为临床基因治疗载体。在临床环境中广泛应用的一个问题是,普通人群中存在大量能够中和 AAV 载体的循环抗体。因此,需要能够逃避固有免疫反应的 AAV 载体。人类原始载体的一个可能来源是不在灵长类动物中传播的 AAV,其中一个例子是蛇形 AAV (SAAV)。本研究描述了 SAAV 衣壳的结构和生物物理特性及其受体相互作用和抗原性。进行了单颗粒冷冻电子显微镜 (cryo-EM) 和热稳定性研究,以表征 pH 值为 7.4、6.0、5.5 和 4.0 时 SAAV 衣壳的结构,这些条件是在细胞运输过程中经历的。使用中国仓鼠卵巢 (CHO) 细胞系进行的细胞结合测定鉴定出末端唾液酸是 SAAV 的主要附着受体,类似于 AAV1、4、5 和 6。唾液酸与 SAAV 衣壳的结合位点被映射到 2 倍轴附近的 2/5 倍壁,位于与 AAV1、4、5 和 6 不同的位置。为了确定 SAAV 衣壳的抗原性,天然免疫印迹显示 SAAV 逃避 AAV 血清型特异性小鼠单克隆抗体。然而,尽管它起源于爬行动物,但它被测试的 50 个人血清中的约 25%识别,可能是由于存在交叉反应性抗体。这些发现将为使用基于 SAAV 的载体的未来基因传递应用提供信息,并进一步帮助对现有 AAV 衣壳的结构特征和注释。AAV 是广泛研究的治疗性基因传递载体。然而,在临床试验中,预先存在的抗体及其对治疗效果的不利影响是主要挑战。为了规避针对哺乳动物 AAV 衣壳的预先存在的中和抗体,评估了蛇形 AAV (SAAV) 作为现有哺乳动物治疗性载体的潜在替代物。研究发现 SAAV 衣壳在广泛的环境 pH 条件下具有热稳定性,其结构显示核心衣壳拓扑结构的保守性,但在表面显示出高度的结构变异性。同时,它与一种常见的受体——唾液酸结合,该受体也被其他已用于基因治疗试验的 AAV 利用。与最初的假设相反,SAAV 衣壳被测试的四分之一人类血清识别,表明 5 倍区周围的保守氨基酸是交叉反应抗体的表位。

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