In silico analysis of pathogenic CRB1  single nucleotide variants and their amenability to base editing as a potential lead for therapeutic intervention

Bellingrath, J-S; McClements, ME; Kaukonen, M; Fischer, MD; MacLaren, RE

Journal article

In silico analysis of pathogenic CRB1 single nucleotide variants and their amenability to base editing as a potential lead for therapeutic intervention

Abstract:: Mutations in the Crumbs homolog 1 (CRB1) gene cause both autosomal recessive retinitis pigmentosa (RP) and Leber congenital amaurosis (LCA). Since three separate CRB1 isoforms are expressed at meaningful levels in the human retina, base editing shows promise as a therapeutic approach. This retrospective analysis aims to summarise the reported pathogenic CRB1 variants and investigate their amenability to treatment with currently available DNA base editors. Pathogenic single nucleotide variants (SNVs) were extracted from the Leiden open-source variation database (LOVD) and ClinVar database and coded by mutational consequence. They were then analyzed for their amenability to currently available DNA base editors and available PAM sites from a selection of different Cas proteins. Of a total of 1115 unique CRB1 variants, 69% were classified as pathogenic SNVs. Of these, 62% were amenable to currently available DNA BEs. Adenine base editors (ABEs) alone have the potential of targeting 34% of pathogenic SNVs; 19% were amenable to a CBE while GBEs could target an additional 9%. Of the pathogenic SNVs targetable with a DNA BE, 87% had a PAM site for a Cas protein. Of the 33 most frequently reported pathogenic SNVs, 70% were targetable with a base editor. The most common pathogenic variant was c.2843G>A, p.Cys948Arg, which is targetable with an ABE. Since 62% of pathogenic CRB1 SNVs are amenable to correction with a base editor and 87% of these mutations had a suitable PAM site, gene editing represents a promising therapeutic avenue for CRB1-associated retinal degenerations

Publication status:: Published

Peer review status:: Peer reviewed

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APA Style

Bellingrath, J.-S., McClements, M. E., Kaukonen, M., Fischer, M. D., & MacLaren, R. E. (2021). In silico analysis of pathogenic CRB1 single nucleotide variants and their amenability to base editing as a potential lead for therapeutic intervention. Genes, 12(12).

MLA Style

Bellingrath, J-S, et al. “In Silico Analysis of Pathogenic CRB1 Single Nucleotide Variants and Their Amenability to Base Editing as a Potential Lead for Therapeutic Intervention.” Genes, vol. 12, no. 12, 2021.

Chicago Style

Bellingrath, J-S, ME McClements, M Kaukonen, MD Fischer, and RE MacLaren. 2021. “In Silico Analysis of Pathogenic CRB1 Single Nucleotide Variants and Their Amenability to Base Editing as a Potential Lead for Therapeutic Intervention.” Genes 12 (12).
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Files:: Bellingrath_et_al_2021_In_Silico_Analysis.pdf

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Publisher copy:: 10.3390/genes12121908

Authors

+ Bellingrath, J-S More by this author

Institution:: University of Oxford
Division:: MSD
Department:: Clinical Neurosciences
Oxford college:: St Cross College
Role:: Author

+ McClements, ME More by this author

Institution:: University of Oxford
Division:: MSD
Department:: Clinical Neurosciences
Role:: Author
ORCID:: 0000-0002-2941-4464

+ Kaukonen, M More by this author

Institution:: University of Oxford
Division:: MSD
Department:: Clinical Neurosciences
Role:: Author
ORCID:: 0000-0002-2146-4694

+ Fischer, MD More by this author

Institution:: University of Oxford
Division:: MSD
Department:: Clinical Neurosciences
Role:: Author
ORCID:: 0000-0001-7459-1024

+ MacLaren, RE More by this author

Institution:: University of Oxford
Division:: MSD
Department:: Clinical Neurosciences
Oxford college:: Merton College
Role:: Author
ORCID:: 0000-0002-3096-4682

+ National Institute for Health Research More from this funder

Grant:: NIHR201338

+ National Institute for Health Research (NIHR) More from this funder

Grant:: NIHR201338

Publisher:: MDPI
Journal:: Genes More from this journal
Volume:: 12
Issue:: 12
Article number:: 1908
Place of publication:: Switzerland
Publication date:: 2021-11-27
Acceptance date:: 2021-11-26
DOI:: 10.3390/genes12121908
EISSN:: 2073-4425
Pmid:: 34946856

Language:: English
Keywords:: inherited retinal disease

genetics

FFR

base editing

CRB1

CRISPR
Pubs id:: 1224107
Local pid:: pubs:1224107
Deposit date:: 2023-05-26
ARK identifier:: ark:/29072/ora_f3df4a8bcea94b759c25327c93a521e8

Terms of use

Copyright holder:: Bellingrath et al
Rights statement:: © 2021 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https:// creativecommons.org/licenses/by/ 4.0/).
Notes:: This work is related to the thesis Advancing RNA base editing treatments for inherited retinal disease.

Licence:: CC Attribution (CC BY)

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In silico analysis of pathogenic CRB1 single nucleotide variants and their amenability to base editing as a potential lead for therapeutic intervention

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