Reciprocal mutations of lung-tropic AAV capsids lead to improved transduction properties

Ashley L. Cooney; Christian M. Brommel; Soumba Traore; Gregory A. Newby; David R. Liu; Paul B. McCray; Patrick L. Sinn

doi:10.3389/fgeed.2023.1271813

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Reciprocal mutations of lung-tropic AAV capsids lead to improved transduction properties

Journal article

Open access

Peer reviewed

Reciprocal mutations of lung-tropic AAV capsids lead to improved transduction properties

Ashley L. Cooney, Christian M. Brommel, Soumba Traore, Gregory A. Newby, David R. Liu, Paul B. McCray and Patrick L. Sinn

Frontiers in genome editing, Vol.5, 1271813

11/01/2023

DOI: 10.3389/fgeed.2023.1271813

PMCID: PMC10702583

PMID: 38077224

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Abstract

Considerable effort has been devoted to developing adeno-associated virus (AAV)-based vectors for gene therapy in cystic fibrosis (CF). As a result of directed evolution and capsid shuffling technology, AAV capsids are available with widespread tropism for airway epithelial cells. For example, AAV2.5T and AAV6.2 are two evolved capsids with improved airway epithelial cell transduction properties over their parental serotypes. However, limited research has been focused on identifying their specific cellular tropism. Restoring cystic fibrosis transmembrane conductance regulator (CFTR) expression in surface columnar epithelial cells is necessary for the correction of the CF airway phenotype. Basal cells are a progenitor population of the conducting airways responsible for replenishing surface epithelial cells (including secretory cells and ionocytes), making correction of this cell population vital for a long-lived gene therapy strategy. In this study, we investigate the tropism of AAV capsids for three cell types in primary cultures of well-differentiated human airway epithelial (HAE) cells and primary human airway basal cells. We observed that AAV2.5T transduced surface epithelial cells better than AAV6.2, while AAV6.2 transduced airway basal cells better than AAV2.5T. We also investigated a recently developed capsid, AAV6.2FF, which has two surface tyrosines converted to phenylalanines. Next, we incorporated reciprocal mutations to create AAV capsids with further improved surface and basal cell transduction characteristics. Lastly, we successfully employed a split-intein approach using AAV to deliver an adenine base editor (ABE) to repair the CFTRR553X mutation. Our results suggest that rational incorporation of AAV capsid mutations improves AAV transduction of the airway surface and progenitor cells and may ultimately lead to improved pulmonary function in people with CF.

Cystic Fibrosis

Gene Therapy

adeno-associated virus capsid

airway epithelia

base editing

Details

Title: Subtitle: Reciprocal mutations of lung-tropic AAV capsids lead to improved transduction properties
Creators: Ashley L. Cooney - University of Iowa
Christian M. Brommel - University of Iowa
Soumba Traore - University of Iowa
Gregory A. Newby - Harvard University
David R. Liu - Broad Institute
Paul B. McCray - University of Iowa
Patrick L. Sinn - University of Iowa
Resource Type: Journal article
Publication Details: Frontiers in genome editing, Vol.5, 1271813
DOI: 10.3389/fgeed.2023.1271813
PMID: 38077224
PMCID: PMC10702583
NLM abbreviation: Front Genome Ed
eISSN: 2673-3439
Publisher: Frontiers Media S.A
Language: English
Date published: 11/01/2023
Academic Unit: Microbiology and Immunology; Pulmonary Medicine; Stead Family Department of Pediatrics; Internal Medicine
Record Identifier: 9984520559902771

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