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Efficacy of CD46-targeting chimeric Ad5/35 adenoviral gene therapy for colorectal cancers

Authors :
Silvio Hemmi
Se-Young Kwon
Keesook Lee
Sang Jin Lee
Changjong Moon
Minsoo Kim
Young-Eun Joo
Manh-Hung Do
Young-Suk Cho
Chaeyong Jung
Kwonseop Kim
University of Zurich
Kim, Min Soo
Source :
Oncotarget
Publication Year :
2016
Publisher :
Impact Journals LLC, 2016.

Abstract

CD46 is a complement inhibitor membrane cofactor which also acts as a receptor for various microbes, including species B adenoviruses (Ads). While most Ad gene therapy vectors are derived from species C and infect cells through coxsackie-adenovirus receptor (CAR), CAR expression is downregulated in many cancer cells, resulting inefficient Ad-based therapeutics. Despite a limited knowledge on the expression status of many cancer cells, an increasing number of cancer gene therapy studies include fiber-modified Ad vectors redirected to the more ubiquitously expressed CD46. Since our finding from tumor microarray indicate that CD46 was overexpressed in cancers of the prostate and colon, fiber chimeric Ad5/35 vectors that have infection tropism for CD46 were employed to demonstrate its efficacy in colorectal cancers (CRC). CD46-overexpressed cells showed a significantly higher response to Ad5/35-GFP and to Ad5/35-tk/GCV. While CRC cells express variable levels of CD46, CD46 expression was positively correlated with Ad5/35-mediated GFP fluorescence and accordingly its cell killing. Injection of Ad5/35-tk/GCV caused much greater tumor-suppression in mice bearing CD46-overexpressed cancer xenograft compared to mock group. Analysis of CRC samples revealed that patients with positive CD46 expression had a higher survival rate (p=0.031), carried tumors that were well-differentiated, but less invasive and metastatic, and with a low T stage (all p

Details

Language :
English
ISSN :
19492553
Volume :
7
Issue :
25
Database :
OpenAIRE
Journal :
Oncotarget
Accession number :
edsair.doi.dedup.....75dc065203c9d54e5f64692c2689d4aa