Oncolytic H-1 Parvovirus Hijacks Galectin-1 to Enter Cancer Cells

Tiago Ferreira; Amit Kulkarni; Clemens Bretscher; Petr V. Nazarov; Jubayer A. Hossain; Lars A. R. Ystaas; Hrvoje Miletic; Ralph Röth; Beate Niesler; Antonio Marchini

doi:10.3390/v14051018

Viruses (May 2022)

Oncolytic H-1 Parvovirus Hijacks Galectin-1 to Enter Cancer Cells

Tiago Ferreira,
Amit Kulkarni,
Clemens Bretscher,
Petr V. Nazarov,
Jubayer A. Hossain,
Lars A. R. Ystaas,
Hrvoje Miletic,
Ralph Röth,
Beate Niesler,
Antonio Marchini

Affiliations

Tiago Ferreira: Laboratory of Oncolytic Virus Immuno-Therapeutics, German Cancer Research Centre, Im Neuenheimer Feld 242, 69120 Heidelberg, Germany
Amit Kulkarni: Laboratory of Oncolytic Virus Immuno-Therapeutics, Luxembourg Institute of Health, 84 Val Fleuri, L-1526 Luxembourg, Luxembourg
Clemens Bretscher: Laboratory of Oncolytic Virus Immuno-Therapeutics, German Cancer Research Centre, Im Neuenheimer Feld 242, 69120 Heidelberg, Germany
Petr V. Nazarov: Bioinformatics Platform and Multiomics Data Science Research Group, Department of Cancer Research, Luxembourg Institute of Health, L-1526 Luxembourg, Luxembourg
Jubayer A. Hossain: Department of Biomedicine, University of Bergen, 5007 Bergen, Norway
Lars A. R. Ystaas: Department of Biomedicine, University of Bergen, 5007 Bergen, Norway
Hrvoje Miletic: Department of Biomedicine, University of Bergen, 5007 Bergen, Norway
Ralph Röth: nCounter Core Facility, Institute of Human Genetics, University of Heidelberg, 69120 Heidelberg, Germany
Beate Niesler: nCounter Core Facility, Institute of Human Genetics, University of Heidelberg, 69120 Heidelberg, Germany
Antonio Marchini: Laboratory of Oncolytic Virus Immuno-Therapeutics, German Cancer Research Centre, Im Neuenheimer Feld 242, 69120 Heidelberg, Germany

DOI: https://doi.org/10.3390/v14051018
Journal volume & issue: Vol. 14, no. 5
p. 1018

Abstract

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Clinical studies in glioblastoma and pancreatic carcinoma patients strongly support the further development of H-1 protoparvovirus (H-1PV)-based anticancer therapies. The identification of cellular factors involved in the H-1PV life cycle may provide the knowledge to improve H-1PV anticancer potential. Recently, we showed that sialylated laminins mediate H-1PV attachment at the cell membrane. In this study, we revealed that H-1PV also interacts at the cell surface with galectin-1 and uses this glycoprotein to enter cancer cells. Indeed, knockdown/out of LGALS1, the gene encoding galectin-1, strongly decreases the ability of H-1PV to infect and kill cancer cells. This ability is rescued by the re-introduction of LGALS1 into cancer cells. Pre-treatment with lactose, which is able to bind to galectins and modulate their cellular functions, decreased H-1PV infectivity in a dose dependent manner. In silico analysis reveals that LGALS1 is overexpressed in various tumours including glioblastoma and pancreatic carcinoma. We show by immunohistochemistry analysis of 122 glioblastoma biopsies that galectin-1 protein levels vary between tumours, with levels in recurrent glioblastoma higher than those in primary tumours or normal tissues. We also find a direct correlation between LGALS1 transcript levels and H-1PV oncolytic activity in 53 cancer cell lines from different tumour origins. Strikingly, the addition of purified galectin-1 sensitises poorly susceptible GBM cell lines to H-1PV killing activity by rescuing cell entry. Together, these findings demonstrate that galectin-1 is a crucial determinant of the H-1PV life cycle.

Published in Viruses

ISSN: 1999-4915 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Microbiology
Website: http://www.mdpi.com/journal/viruses

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