Oncolytic measles virus retargeting by ligand display

Pavlos Msaouel; Ianko D. Iankov; Cory Allen; Stephen J. Russell; Evanthia Galanis

doi:10.1007/978-1-61779-340-0_11

Oncolytic measles virus retargeting by ligand display

Pavlos Msaouel, Ianko D. Iankov, Cory Allen, Stephen J. Russell, Evanthia Galanis

Research output: Chapter in Book/Report/Conference proceeding › Chapter

15 Scopus citations

Abstract

Despite significant advances in recent years, treatment of metastatic malignancies remains a significant challenge. There is an urgent need for development of novel therapeutic approaches. Virotherapy approaches have considerable potential, and among them measles virus (MV) vaccine strains have emerged as a promising oncolytic platform. Retargeted MV strains deriving from the Edmonston vaccine lineage (MV-Edm) have shown comparable antitumor efficacy to unmodified strains against receptor expressing tumor cells with improved therapeutic index. Here, we describe the construction, rescue, amplification, and titration of fully retargeted MV-Edm derivatives displaying tumor specific receptor binding ligands on the viral surface in combination with H protein CD46 and SLAM entry ablating mutations.

Original language	English (US)
Title of host publication	Oncolytic Viruses
Subtitle of host publication	Methods and Protocols
Publisher	Humana Press Inc.
Pages	141-162
Number of pages	22
ISBN (Print)	9781617793394
DOIs	https://doi.org/10.1007/978-1-61779-340-0_11
State	Published - 2012

Publication series

Name	Methods in Molecular Biology
Volume	797
ISSN (Print)	1064-3745
ISSN (Electronic)	1940-6029

Keywords

Measles engineering
Measles retargeting
Oncolytic measles virus
Virotherapy

ASJC Scopus subject areas

Molecular Biology
Genetics

Access to Document

10.1007/978-1-61779-340-0_11

Cite this

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abstract = "Despite significant advances in recent years, treatment of metastatic malignancies remains a significant challenge. There is an urgent need for development of novel therapeutic approaches. Virotherapy approaches have considerable potential, and among them measles virus (MV) vaccine strains have emerged as a promising oncolytic platform. Retargeted MV strains deriving from the Edmonston vaccine lineage (MV-Edm) have shown comparable antitumor efficacy to unmodified strains against receptor expressing tumor cells with improved therapeutic index. Here, we describe the construction, rescue, amplification, and titration of fully retargeted MV-Edm derivatives displaying tumor specific receptor binding ligands on the viral surface in combination with H protein CD46 and SLAM entry ablating mutations.",

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AU - Iankov, Ianko D.

AU - Allen, Cory

AU - Russell, Stephen J.

AU - Galanis, Evanthia

N1 - Publisher Copyright: © Springer Science+Business Media, LLC 2012.

PY - 2012

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N2 - Despite significant advances in recent years, treatment of metastatic malignancies remains a significant challenge. There is an urgent need for development of novel therapeutic approaches. Virotherapy approaches have considerable potential, and among them measles virus (MV) vaccine strains have emerged as a promising oncolytic platform. Retargeted MV strains deriving from the Edmonston vaccine lineage (MV-Edm) have shown comparable antitumor efficacy to unmodified strains against receptor expressing tumor cells with improved therapeutic index. Here, we describe the construction, rescue, amplification, and titration of fully retargeted MV-Edm derivatives displaying tumor specific receptor binding ligands on the viral surface in combination with H protein CD46 and SLAM entry ablating mutations.

AB - Despite significant advances in recent years, treatment of metastatic malignancies remains a significant challenge. There is an urgent need for development of novel therapeutic approaches. Virotherapy approaches have considerable potential, and among them measles virus (MV) vaccine strains have emerged as a promising oncolytic platform. Retargeted MV strains deriving from the Edmonston vaccine lineage (MV-Edm) have shown comparable antitumor efficacy to unmodified strains against receptor expressing tumor cells with improved therapeutic index. Here, we describe the construction, rescue, amplification, and titration of fully retargeted MV-Edm derivatives displaying tumor specific receptor binding ligands on the viral surface in combination with H protein CD46 and SLAM entry ablating mutations.

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KW - Measles retargeting

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KW - Virotherapy

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Oncolytic measles virus retargeting by ligand display

Abstract

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Keywords

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