Literature DB >> 30692695

Identification of preexisting adaptive immunity to Cas9 proteins in humans.

Carsten T Charlesworth1, Priyanka S Deshpande1, Daniel P Dever1, Joab Camarena1, Viktor T Lemgart1, M Kyle Cromer1, Christopher A Vakulskas2, Michael A Collingwood2, Liyang Zhang2, Nicole M Bode2, Mark A Behlke2, Beruh Dejene1, Brandon Cieniewicz1, Rosa Romano1, Benjamin J Lesch1, Natalia Gomez-Ospina1, Sruthi Mantri1, Mara Pavel-Dinu1, Kenneth I Weinberg3, Matthew H Porteus4.   

Abstract

The CRISPR-Cas9 system is a powerful tool for genome editing, which allows the precise modification of specific DNA sequences. Many efforts are underway to use the CRISPR-Cas9 system to therapeutically correct human genetic diseases1-6. The most widely used orthologs of Cas9 are derived from Staphylococcus aureus and Streptococcus pyogenes5,7. Given that these two bacterial species infect the human population at high frequencies8,9, we hypothesized that humans may harbor preexisting adaptive immune responses to the Cas9 orthologs derived from these bacterial species, SaCas9 (S. aureus) and SpCas9 (S. pyogenes). By probing human serum for the presence of anti-Cas9 antibodies using an enzyme-linked immunosorbent assay, we detected antibodies against both SaCas9 and SpCas9 in 78% and 58% of donors, respectively. We also found anti-SaCas9 T cells in 78% and anti-SpCas9 T cells in 67% of donors, which demonstrates a high prevalence of antigen-specific T cells against both orthologs. We confirmed that these T cells were Cas9-specific by demonstrating a Cas9-specific cytokine response following isolation, expansion, and antigen restimulation. Together, these data demonstrate that there are preexisting humoral and cell-mediated adaptive immune responses to Cas9 in humans, a finding that should be taken into account as the CRISPR-Cas9 system moves toward clinical trials.

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Year:  2019        PMID: 30692695      PMCID: PMC7199589          DOI: 10.1038/s41591-018-0326-x

Source DB:  PubMed          Journal:  Nat Med        ISSN: 1078-8956            Impact factor:   53.440


  38 in total

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Journal:  J Immunol Methods       Date:  1983-12-16       Impact factor: 2.303

5.  Targeting a CAR to the TRAC locus with CRISPR/Cas9 enhances tumour rejection.

Authors:  Justin Eyquem; Jorge Mansilla-Soto; Theodoros Giavridis; Sjoukje J C van der Stegen; Mohamad Hamieh; Kristen M Cunanan; Ashlesha Odak; Mithat Gönen; Michel Sadelain
Journal:  Nature       Date:  2017-02-22       Impact factor: 49.962

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Journal:  Science       Date:  2012-06-28       Impact factor: 47.728

7.  Comparison of antibody repertoires against Staphylococcus aureus in healthy individuals and in acutely infected patients.

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Journal:  Clin Diagn Lab Immunol       Date:  2005-03

8.  CD8(+) T-cell responses to adeno-associated virus capsid in humans.

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Journal:  BMC Pediatr       Date:  2012-01-09       Impact factor: 2.125

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Journal:  Nat Biotechnol       Date:  2014-10-30       Impact factor: 54.908

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4.  Multicellular Systems to Translate Somatic Cell Genome Editors to Humans.

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5.  Life-Long AAV-Mediated CRISPR Genome Editing in Dystrophic Heart Improves Cardiomyopathy without Causing Serious Lesions in mdx Mice.

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Journal:  Mol Ther       Date:  2019-05-15       Impact factor: 11.454

6.  CRISPR-Edited Immune Effectors: The End of the Beginning.

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7.  Coevolutionary Couplings Unravel PAM-Proximal Constraints of CRISPR-SpCas9.

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Review 9.  CRISPR-Based Therapeutic Genome Editing: Strategies and In Vivo Delivery by AAV Vectors.

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Journal:  Cell       Date:  2020-04-02       Impact factor: 41.582

10.  Engineered materials for in vivo delivery of genome-editing machinery.

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