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跨物种宽容性:山羊腺相关病毒的结构及其与人受体 AAVR 的复合物。

Cross-Species Permissivity: Structure of a Goat Adeno-Associated Virus and Its Complex with the Human Receptor AAVR.

机构信息

Department of Biochemistry, University of Missourigrid.134936.a, Columbia, Missouri, USA.

出版信息

J Virol. 2022 Dec 21;96(24):e0148422. doi: 10.1128/jvi.01484-22. Epub 2022 Dec 1.

Abstract

Adeno-associated virus (AAV) is a small ssDNA satellite virus of high interest (in recombinant form) as a safe and effective gene therapy vector. AAV's human cell entry receptor (AAVR) contains polycystic kidney disease (PKD) domains bound by AAV. Seeking understanding of the spectrum of interactions, goat AAVGo.1 is investigated, because its host is the species most distant from human with reciprocal cross-species cell susceptibility. The structure of AAVGo.1, solved by cryo-EM to 2.9 Å resolution, is most similar to AAV5. Through ELISA (enzyme-linked immunosorbent assay) studies, it is shown that AAVGo.1 binds to human AAVR more strongly than do AAV2 or AAV5, and that it joins AAV5 in a class that binds exclusively to PKD domain 1 (PKD1), in contrast to other AAVs that interact primarily with PKD2. The AAVGo.1 cryo-EM structure of a complex with a PKD12 fragment of AAVR at 2.4 Å resolution shows PKD1 bound with minimal change in virus structure. There are only minor conformational adaptations in AAVR, but there is a near-rigid rotation of PKD1 with maximal displacement of the receptor domain by ~1 Å compared to PKD1 bound to AAV5. AAVGo.1 joins AAV5 as the second member of an emerging class of AAVs whose mode of receptor-binding is completely different from other AAVs, typified by AAV2. Adeno-associated virus (AAV) is a small ssDNA satellite parvovirus. As a recombinant vector with a protein shell encapsidating a transgene, recombinant AAV (rAAV) is a leading delivery vehicle for gene therapy, with two FDA-approved treatments and 150 clinical trials for 30 diseases. The human entry receptor AAVR has five PKD domains. To date, all serotypes, except AAV5, have interacted primarily with the second PKD domain, PKD2. Goat is the AAV host most distant from human with cross-species cell infectivity. AAVGo.1 is similar in structure to AAV5, the two forming a class with a distinct mode of receptor-binding. Within the two classes, binding interactions are mostly conserved, giving an indication of the latitude available in modulating delivery vectors.

摘要

腺相关病毒 (AAV) 是一种小型 ssDNA 卫星微小病毒,具有很高的研究价值(以重组形式存在),可用作安全有效的基因治疗载体。AAV 的人细胞进入受体 (AAVR) 包含多毛囊性肾病 (PKD) 结构域,这些结构域与 AAV 结合。为了寻求对相互作用范围的理解,研究了山羊 AAVGo.1,因为它的宿主是与人类亲缘关系最远的物种,具有交叉物种细胞易感性。通过 cryo-EM 解析到 2.9 Å 分辨率,确定了 AAVGo.1 的结构,它与 AAV5 最为相似。通过 ELISA(酶联免疫吸附试验)研究表明,AAVGo.1 与人 AAVR 的结合比 AAV2 或 AAV5 更强,并且它与 AAV5 一起属于仅与 PKD1 结构域 1 (PKD1) 结合的一类,而其他 AAV 则主要与 PKD2 相互作用。在 2.4 Å 分辨率下,与 AAVR 的 PKD12 片段的复合物的 AAVGo.1 cryo-EM 结构显示,PKD1 结合时病毒结构几乎没有变化。AAVR 只有微小的构象适应,但 PKD1 发生近乎刚性的旋转,与 AAV5 结合的受体结构域最大位移约 1 Å。AAVGo.1 与 AAV5 一起成为新兴 AAV 类别的第二个成员,该类别与 AAV2 等其他 AAV 的受体结合模式完全不同。腺相关病毒 (AAV) 是一种小型 ssDNA 卫星微小病毒。作为一种带有蛋白外壳包裹转基因的重组载体,重组腺相关病毒 (rAAV) 是基因治疗的主要载体,已有两种 FDA 批准的治疗方法和 150 种针对 30 种疾病的临床试验。人类进入受体 AAVR 有五个 PKD 结构域。迄今为止,除了 AAV5 之外,所有血清型都主要与第二个 PKD 结构域 PKD2 相互作用。山羊是与人类亲缘关系最远的 AAV 宿主,具有跨物种细胞感染性。AAVGo.1 与 AAV5 在结构上相似,两者形成一个具有独特受体结合模式的类别。在这两个类别中,结合相互作用大多是保守的,这表明在调节载体时可提供一定的灵活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9e03/9769368/0569b4997c9d/jvi.01484-22-f001.jpg

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