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Review
. 2024:208:19-41.
doi: 10.1016/bs.pmbts.2024.07.013. Epub 2024 Aug 21.

Advances in CRISPR-Cas systems for human bacterial disease

Affiliations
Review

Advances in CRISPR-Cas systems for human bacterial disease

Anshu Mathuria et al. Prog Mol Biol Transl Sci. 2024.

Abstract

Prokaryotic adaptive immune systems called CRISPR-Cas systems have transformed genome editing by allowing for precise genetic alterations through targeted DNA cleavage. This system comprises CRISPR-associated genes and repeat-spacer arrays, which generate RNA molecules that guide the cleavage of invading genetic material. CRISPR-Cas is classified into Class 1 (multi-subunit effectors) and Class 2 (single multi-domain effectors). Its applications span combating antimicrobial resistance (AMR), targeting antibiotic resistance genes (ARGs), resensitizing bacteria to antibiotics, and preventing horizontal gene transfer (HGT). CRISPR-Cas3, for example, effectively degrades plasmids carrying resistance genes, providing a precise method to disarm bacteria. In the context of ESKAPE pathogens, CRISPR technology can resensitize bacteria to antibiotics by targeting specific resistance genes. Furthermore, in tuberculosis (TB) research, CRISPR-based tools enhance diagnostic accuracy and facilitate precise genetic modifications for studying Mycobacterium tuberculosis. CRISPR-based diagnostics, leveraging Cas endonucleases' collateral cleavage activity, offer highly sensitive pathogen detection. These advancements underscore CRISPR's transformative potential in addressing AMR and enhancing infectious disease management.

Keywords: Antibiotic resistance genes; Antimicrobial resistance; CRISPR-Cas systems; ESKAPE pathogens; Genetic modifications; Tuberculosis diagnostics.

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