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Development of a low-seroprevalence, αvβ6 integrin-selective virotherapy based on human adenovirus type 10
EA. Bates, JA. Davies, J. Váňová, D. Nestić, VS. Meniel, S. Koushyar, TG. Cunliffe, RM. Mundy, E. Moses, HK. Uusi-Kerttula, AT. Baker, DK. Cole, D. Majhen, PJ. Rizkallah, T. Phesse, JD. Chester, AL. Parker
Jazyk angličtina Země Spojené státy americké
Typ dokumentu časopisecké články
NLK
Directory of Open Access Journals
od 2014
Free Medical Journals
od 2014
PubMed Central
od 2014 do 2023
Europe PubMed Central
od 2014
Open Access Digital Library
od 2014-01-01
ROAD: Directory of Open Access Scholarly Resources
od 2014 do 2023
- Publikační typ
- časopisecké články MeSH
Oncolytic virotherapies (OV) hold immense clinical potential. OV based on human adenoviruses (HAdV) derived from HAdV with naturally low rates of pre-existing immunity will be beneficial for future clinical translation. We generated a low-seroprevalence HAdV-D10 serotype vector incorporating an αvβ6 integrin-selective peptide, A20, to target αvβ6-positive tumor cell types. HAdV-D10 has limited natural tropism. Structural and biological studies of HAdV-D10 knob protein highlighted low-affinity engagement with native adenoviral receptors CAR and sialic acid. HAdV-D10 fails to engage blood coagulation factor X, potentially eliminating "off-target" hepatic sequestration in vivo. We engineered an A20 peptide that selectively binds αvβ6 integrin into the DG loop of HAdV-D10 fiber knob. Assays in αvβ6+ cancer cell lines demonstrated significantly increased transduction mediated by αvβ6-targeted variants compared with controls, confirmed microscopically. HAdV-D10.A20 resisted neutralization by neutralizing HAdV-C5 sera. Systemic delivery of HAdV-D10.A20 resulted in significantly increased GFP expression in BT20 tumors. Replication-competent HAdV-D10.A20 demonstrated αvβ6 integrin-selective cell killing in vitro and in vivo. HAdV-D10 possesses characteristics of a promising virotherapy, combining low seroprevalence, weak receptor interactions, and reduced off-target uptake. Incorporation of an αvβ6 integrin-selective peptide resulted in HAdV-D10.A20, with significant potential for clinical translation.
Division of Cancer and Genetics School of Medicine Cardiff University Heath Park Cardiff CF14 4XN UK
Division of Molecular Biology Ruđer Bošković Institute Bijenička cesta 54 10000 Zagreb Croatia
European Cancer Stem Cell Research Institute Cardiff University Cardiff CF24 4HQ UK
Citace poskytuje Crossref.org
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