Literature DB >> 18989355

Comparison of intravenous versus intraperitoneal administration of oncolytic herpes simplex virus 1 for peritoneal carcinomatosis in mice.

Y Kulu1, J D Dorfman, D Kuruppu, B C Fuchs, J M Goodwin, T Fujii, T Kuroda, M Lanuti, K K Tanabe.   

Abstract

hrR3 is an oncolytic herpes simplex virus 1 (HSV-1) mutant that replicates preferentially in tumors compared with normal tissues. Portal venous administration of hrR3 in mice bearing diffuse colorectal carcinoma liver metastases significantly reduces tumor burden and prolongs animal survival. In this study, we compared survival benefit and biodistribution of hrR3 following intravenous (i.v.) administration versus intraperitoneal (i.p.) administration in immunocompetent mice bearing colon carcinoma peritoneal metastases. Mice bearing peritoneal metastases received 1 x 10(8) plaque-forming units hrR3 or mock-infected media every other day for three doses and were randomized to have the viruses administered by either an i.p. or i.v. route. Biodistribution was assessed by PCR amplification of HSV-1-specific sequences from tumor and normal tissues including the small bowel, liver, spleen, kidney, lung, heart and brain. LD(50) for i.p. administration was compared with the LD(50) for i.v. administration. In subsequent experiments, animals were monitored for survival. The frequency of HSV-1 detection in peritoneal tumors was similar in mice randomized to either i.p. or i.v. administration. However, i.p. administration resulted in a more restricted systemic biodistribution, with a reduced frequency of virus detected in the kidney, lung and heart. The LD(50) associated with i.p. administration was higher than that with i.v. administration. Tumor burden was more effectively reduced with i.p. compared with i.v. administration. Median survival following i.p. administration was approximately twice that observed with i.v. administration. I.p. administration of an HSV-1 oncolytic mutant is associated with a more restricted biodistribution, less toxicity and greater efficacy against peritoneal metastases compared with i.v. administration.

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Year:  2008        PMID: 18989355      PMCID: PMC2657185          DOI: 10.1038/cgt.2008.83

Source DB:  PubMed          Journal:  Cancer Gene Ther        ISSN: 0929-1903            Impact factor:   5.987


  35 in total

Review 1.  Viral oncolysis.

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2.  Multi-attenuated herpes simplex virus-1 mutant G207 exerts cytotoxicity against epithelial ovarian cancer but not normal mesothelium and is suitable for intraperitoneal oncolytic therapy.

Authors:  G Coukos; A Makrigiannakis; S Montas; L R Kaiser; T Toyozumi; I Benjamin; S M Albelda; S C Rubin; K L Molnar-Kimber
Journal:  Cancer Gene Ther       Date:  2000-02       Impact factor: 5.987

3.  Positron emission tomography of herpes simplex virus 1 oncolysis.

Authors:  Darshini Kuruppu; Anna-Liisa Brownell; Aijun Zhu; Meixiang Yu; Xukui Wang; Yakup Kulu; Bryan C Fuchs; Hiroshi Kawasaki; Kenneth K Tanabe
Journal:  Cancer Res       Date:  2007-04-01       Impact factor: 12.701

4.  Multimodality therapy with a replication-conditional herpes simplex virus 1 mutant that expresses yeast cytosine deaminase for intratumoral conversion of 5-fluorocytosine to 5-fluorouracil.

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7.  Intraperitoneal delivery of hrR3 and ganciclovir prolongs survival in mice with disseminated pancreatic cancer.

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9.  Regulation of herpes simplex virus gamma(1)34.5 expression and oncolysis of diffuse liver metastases by Myb34.5.

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  18 in total

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Journal:  Drugs Future       Date:  2010       Impact factor: 0.148

2.  Stem cell-released oncolytic herpes simplex virus has therapeutic efficacy in brain metastatic melanomas.

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Journal:  Proc Natl Acad Sci U S A       Date:  2017-07-14       Impact factor: 11.205

Review 3.  Regional liver therapy using oncolytic virus to target hepatic colorectal metastases.

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Review 7.  Retargeting Strategies for Oncolytic Herpes Simplex Viruses.

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8.  Disruption of type I interferon signaling causes sexually dimorphic dysregulation of anti-viral cytokines.

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9.  Preclinical therapy of disseminated HER-2⁺ ovarian and breast carcinomas with a HER-2-retargeted oncolytic herpesvirus.

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Journal:  PLoS Pathog       Date:  2013-01-31       Impact factor: 6.823

10.  Effective combination immunotherapy using oncolytic viruses to deliver CAR targets to solid tumors.

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