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Neuroblastomas Vary Widely in Their Sensitivities to Herpes Simplex Virotherapy Unrelated to Virus Receptors and Susceptibility

Although most high-risk neuroblastomas are responsive to chemotherapy, relapse is common and long-term survival is less than 40%, underscoring the need for more effective treatments. We evaluated the responsiveness of 12 neuroblastoma cell lines to the Δγ(1)34.5 attenuated oncolytic HSV, Seprehvir (...

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Autores principales: Wang, Pin-Yi, Swain, Hayley M., Kunkler, Anne L., Chen, Chun-Yu, Hutzen, Brian J., Arnold, Michael A., Streby, Keri A., Collins, Margaret H., Dipasquale, Betsy, Stanek, Joseph R., Conner, Joe, van Kuppevelt, Toin H., Glorioso, Joseph C., Grandi, Paola, Cripe, Timothy P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4742391/
https://www.ncbi.nlm.nih.gov/pubmed/26583803
http://dx.doi.org/10.1038/gt.2015.105
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author Wang, Pin-Yi
Swain, Hayley M.
Kunkler, Anne L.
Chen, Chun-Yu
Hutzen, Brian J.
Arnold, Michael A.
Streby, Keri A.
Collins, Margaret H.
Dipasquale, Betsy
Stanek, Joseph R.
Conner, Joe
van Kuppevelt, Toin H.
Glorioso, Joseph C.
Grandi, Paola
Cripe, Timothy P.
author_facet Wang, Pin-Yi
Swain, Hayley M.
Kunkler, Anne L.
Chen, Chun-Yu
Hutzen, Brian J.
Arnold, Michael A.
Streby, Keri A.
Collins, Margaret H.
Dipasquale, Betsy
Stanek, Joseph R.
Conner, Joe
van Kuppevelt, Toin H.
Glorioso, Joseph C.
Grandi, Paola
Cripe, Timothy P.
author_sort Wang, Pin-Yi
collection PubMed
description Although most high-risk neuroblastomas are responsive to chemotherapy, relapse is common and long-term survival is less than 40%, underscoring the need for more effective treatments. We evaluated the responsiveness of 12 neuroblastoma cell lines to the Δγ(1)34.5 attenuated oncolytic HSV, Seprehvir (HSV1716), which is currently used in pediatric phase I trials. We found that entry of Seprehvir in neuroblastoma cells is independent of the expression of nectin-1 and the sum of all four known major HSV entry receptors. We observed varying levels of sensitivity and permissivity to Seprehvir, suggesting that the cellular anti-viral response, not virus entry, is the key determinant of efficacy with this virus. In vivo, we found significant anti-tumor efficacy following Seprehvir treatment, which ranged from 6/10 complete responses in the CHP-134 model to a mild prolonged median survival in the SK-N-AS model. Taken together, these data suggest that anti-tumor efficacy cannot be solely predicted based on in vitro response. Whether or not this discordance holds true for other viruses or tumor types is unknown. Our results also suggest that profiling the expression of known viral entry receptors on neuroblastoma cells may not be entirely predictive of their susceptibility to Seprehvir therapy.
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spelling pubmed-47423912016-05-19 Neuroblastomas Vary Widely in Their Sensitivities to Herpes Simplex Virotherapy Unrelated to Virus Receptors and Susceptibility Wang, Pin-Yi Swain, Hayley M. Kunkler, Anne L. Chen, Chun-Yu Hutzen, Brian J. Arnold, Michael A. Streby, Keri A. Collins, Margaret H. Dipasquale, Betsy Stanek, Joseph R. Conner, Joe van Kuppevelt, Toin H. Glorioso, Joseph C. Grandi, Paola Cripe, Timothy P. Gene Ther Article Although most high-risk neuroblastomas are responsive to chemotherapy, relapse is common and long-term survival is less than 40%, underscoring the need for more effective treatments. We evaluated the responsiveness of 12 neuroblastoma cell lines to the Δγ(1)34.5 attenuated oncolytic HSV, Seprehvir (HSV1716), which is currently used in pediatric phase I trials. We found that entry of Seprehvir in neuroblastoma cells is independent of the expression of nectin-1 and the sum of all four known major HSV entry receptors. We observed varying levels of sensitivity and permissivity to Seprehvir, suggesting that the cellular anti-viral response, not virus entry, is the key determinant of efficacy with this virus. In vivo, we found significant anti-tumor efficacy following Seprehvir treatment, which ranged from 6/10 complete responses in the CHP-134 model to a mild prolonged median survival in the SK-N-AS model. Taken together, these data suggest that anti-tumor efficacy cannot be solely predicted based on in vitro response. Whether or not this discordance holds true for other viruses or tumor types is unknown. Our results also suggest that profiling the expression of known viral entry receptors on neuroblastoma cells may not be entirely predictive of their susceptibility to Seprehvir therapy. 2015-11-19 2016-02 /pmc/articles/PMC4742391/ /pubmed/26583803 http://dx.doi.org/10.1038/gt.2015.105 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Wang, Pin-Yi
Swain, Hayley M.
Kunkler, Anne L.
Chen, Chun-Yu
Hutzen, Brian J.
Arnold, Michael A.
Streby, Keri A.
Collins, Margaret H.
Dipasquale, Betsy
Stanek, Joseph R.
Conner, Joe
van Kuppevelt, Toin H.
Glorioso, Joseph C.
Grandi, Paola
Cripe, Timothy P.
Neuroblastomas Vary Widely in Their Sensitivities to Herpes Simplex Virotherapy Unrelated to Virus Receptors and Susceptibility
title Neuroblastomas Vary Widely in Their Sensitivities to Herpes Simplex Virotherapy Unrelated to Virus Receptors and Susceptibility
title_full Neuroblastomas Vary Widely in Their Sensitivities to Herpes Simplex Virotherapy Unrelated to Virus Receptors and Susceptibility
title_fullStr Neuroblastomas Vary Widely in Their Sensitivities to Herpes Simplex Virotherapy Unrelated to Virus Receptors and Susceptibility
title_full_unstemmed Neuroblastomas Vary Widely in Their Sensitivities to Herpes Simplex Virotherapy Unrelated to Virus Receptors and Susceptibility
title_short Neuroblastomas Vary Widely in Their Sensitivities to Herpes Simplex Virotherapy Unrelated to Virus Receptors and Susceptibility
title_sort neuroblastomas vary widely in their sensitivities to herpes simplex virotherapy unrelated to virus receptors and susceptibility
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4742391/
https://www.ncbi.nlm.nih.gov/pubmed/26583803
http://dx.doi.org/10.1038/gt.2015.105
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