9RQT image
Deposition Date 2025-06-26
Release Date 2026-02-04
Last Version Date 2026-03-18
Entry Detail
PDB ID:
9RQT
Title:
Heptameric AAV2 Rep40-dsDNA (ITR) complex in presence of ATPgS
Biological Source:
Source Organism(s):
Expression System(s):
Method Details:
Experimental Method:
Resolution:
2.88 Å
Aggregation State:
PARTICLE
Reconstruction Method:
SINGLE PARTICLE
Macromolecular Entities
Polymer Type:polydeoxyribonucleotide
Molecule:DNA (28-MER)
Chain IDs:A (auth: H)
Chain Length:145
Number of Molecules:1
Biological Source:DNA molecule
Structures with similar UniProt ID
Protein Blast
Polymer Type:polypeptide(L)
Molecule:Protein Rep40
Gene (Uniprot):Rep40
Chain IDs:B (auth: a), C (auth: b), D (auth: c), E (auth: d), F (auth: e), G (auth: f), H (auth: g)
Chain Length:397
Number of Molecules:7
Biological Source:adeno-associated virus 2
Primary Citation
Structural basis for Rep-mediated adeno-associated virus packaging.
Cell Rep 45 117044 117044 (2026)
PMID: 41790558 DOI: 10.1016/j.celrep.2026.117044

Abstact

Adeno-associated viruses (AAVs) are parvoviruses utilized as gene therapy vectors. However, the AAV packaging mechanism is unresolved at the molecular level, creating a bottleneck for vector manufacturing, safety, and efficacy. Here, cryo-EM structures of the Rep helicase packaging motor in complex with the packaging marker DNA (ITR) and the Rep-AAV8 capsid complex are presented. Rep-ITR complexes reveal dynamic oligomeric states on the DNA, elucidating the strand separation mechanism coupled to its ATPase cycle. We observe Rep preferentially bound to empty capsids, with a binding interface likely conserved across the virus family. This complex also unveils a cryptic capsid ATP-binding site which, alongside Rep binding, triggers structural rearrangements priming the capsid for packaging. Collectively, these findings advance the understanding of Rep-mediated packaging, with significant implications for parvovirus virology and viral vector design.

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Primary Citation of related structures
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