Divergent engagements between adeno-associated viruses with their cellular receptor AAVR

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作者
Ran Zhang
Guangxue Xu
Lin Cao
Zixian Sun
Yong He
Mengtian Cui
Yuna Sun
Shentao Li
Huapeng Li
Lan Qin
Mingxu Hu
Zhengjia Yuan
Zipei Rao
Wei Ding
Zihe Rao
Zhiyong Lou
机构
[1] Tsinghua University,MOE Key Laboratory of Protein Science & Collaborative Innovation Center of Biotherapy, School of Medicine
[2] Tsinghua University,School of Life Sciences
[3] Nankai University,State Key Laboratory of Medicinal Chemical Biology, College of Life Science and College of Pharmacy
[4] Capital Medical University,Department of Biochemistry and Molecular Biology, School of Basic Medical Sciences
[5] Chinese Academy of Science,National Laboratory of Macromolecules, Institute of Biophysics
[6] PackGene Biotech,undefined
[7] DIAN Diagnostics,undefined
[8] High School Attached to Capital Normal University,undefined
[9] No. 4 High School,undefined
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摘要
Adeno-associated virus (AAV) receptor (AAVR) is an essential receptor for the entry of multiple AAV serotypes with divergent rules; however, the mechanism remains unclear. Here, we determine the structures of the AAV1-AAVR and AAV5-AAVR complexes, revealing the molecular details by which PKD1 recognizes AAV5 and PKD2 is solely engaged with AAV1. PKD2 lies on the plateau region of the AAV1 capsid. However, the AAV5-AAVR interface is strikingly different, in which PKD1 is bound at the opposite side of the spike of the AAV5 capsid than the PKD2-interacting region of AAV1. Residues in strands F/G and the CD loop of PKD1 interact directly with AAV5, whereas residues in strands B/C/E and the BC loop of PKD2 make contact with AAV1. These findings further the understanding of the distinct mechanisms by which AAVR recognizes various AAV serotypes and provide an example of a single receptor engaging multiple viral serotypes with divergent rules.
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