## Abstract ## Objectives/Hypothesis: To analyze the outcomes of patients treated for minor salivary gland carcinoma with radiotherapy (RT), either alone or combined with surgery. ## Study Design: Retrospective review. ## Methods: Between September 1966 and December 2006, 140 patients were tre
Herpes oncolytic therapy of salivary gland carcinomas
โ Scribed by Vincent Reid; Zhenkun Yu; Theodore Schuman; Sen Li; Paramjeet Singh; Yuman Fong; Richard J. Wong
- Publisher
- John Wiley and Sons
- Year
- 2007
- Tongue
- French
- Weight
- 528 KB
- Volume
- 122
- Category
- Article
- ISSN
- 0020-7136
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โฆ Synopsis
Abstract
Oncolytic herpes simplex viruses (HSV) have demonstrated potent antitumoral effects against a variety of human malignancies in preclinical studies and are in early clinical trials. We explored the activity of an attenuated, replicationโcompetent, oncolytic HSV (NV1023) for the treatment of human salivary gland carcinomas. NV1023 was able to successfully enter into 4 mucoepidermoid carcinoma (H292, H3118, HTBโ41, UTโMUCโ1) and 2 adenocarcinoma (HSY, HSG) cell lines, as measured by lacZ assays after exposure to 5 viral particles per cell (MOI 5). Viral plaque assays showed variation of viral replication within these cell lines, ranging from a 268โfold increase (H292) to a 3โfold increase (HSG) in viral titer. At MOI 5, all cell lines showed >95% cytotoxicity from NV1023 by Day 7, except for HSY (73%). At MOI 0.1, H3118 and UTโMUCโ1 remained highly sensitive to NV1023, both showing >95% cytotoxicity by Day 7. The mucoepidermoid carcinomas were more sensitive to NV1023 at low viral concentrations compared with the adenocarcinomas. Flank tumors of H3118, HTBโ41 and HSY in nude mice showed significant tumor volume reductions after a single intratumoral injection of NV1023 (2 ร 10^7^ plaqueโforming units). These data suggest that oncolytic herpes viruses have significant efficacy entering, replicating within, and lysing human salivary gland carcinomas. These promising biologic agents should be further investigated as novel therapy for patients with salivary carcinomas failing conventional treatment. ยฉ 2007 WileyโLiss, Inc.
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