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8GAN

Exploiting Activation and Inactivation Mechanisms in Type I-C CRISPR-Cas3 for Genome Editing Applications

Summary for 8GAN
Entry DOI10.2210/pdb8gan/pdb
EMDB information29901
DescriptorCas7, Cas11, Cas8, ... (8 entities in total)
Functional Keywordscrispr, type i-c, cascade, anti-crispr, hydrolase-rna-dna complex, hydrolase/rna/dna
Biological sourceNeisseria lactamica
More
Total number of polymer chains16
Total formula weight399279.19
Authors
Hu, C.,Nam, K.H.,Ke, A. (deposition date: 2023-02-23, release date: 2024-03-06)
Primary citationHu, C.,Myers, M.T.,Zhou, X.,Hou, Z.,Lozen, M.L.,Nam, K.H.,Zhang, Y.,Ke, A.
Exploiting activation and inactivation mechanisms in type I-C CRISPR-Cas3 for genome-editing applications.
Mol.Cell, 84:463-475.e5, 2024
Cited by
PubMed Abstract: Type I CRISPR-Cas systems utilize the RNA-guided Cascade complex to identify matching DNA targets and the nuclease-helicase Cas3 to degrade them. Among the seven subtypes, type I-C is compact in size and highly active in creating large-sized genome deletions in human cells. Here, we use four cryoelectron microscopy snapshots to define its RNA-guided DNA binding and cleavage mechanisms in high resolution. The non-target DNA strand (NTS) is accommodated by I-C Cascade in a continuous binding groove along the juxtaposed Cas11 subunits. Binding of Cas3 further traps a flexible bulge in NTS, enabling NTS nicking. We identified two anti-CRISPR proteins AcrIC8 and AcrIC9 that strongly inhibit Neisseria lactamica I-C function. Structural analysis showed that AcrIC8 inhibits PAM recognition through allosteric inhibition, whereas AcrIC9 achieves so through direct competition. Both Acrs potently inhibit I-C-mediated genome editing and transcriptional modulation in human cells, providing the first off-switches for type I CRISPR eukaryotic genome engineering.
PubMed: 38242128
DOI: 10.1016/j.molcel.2023.12.034
PDB entries with the same primary citation
Experimental method
ELECTRON MICROSCOPY (3.26 Å)
Structure validation

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PDB entries from 2024-11-13

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