HSV1716 injection into the brain adjacent to tumour following surgical resection of high-grade glioma: safety data and long-term survival

Following standard treatment, the prognosis remains poor in patients with high-grade glioma and new therapies are urgently required. Herpes simplex virus 1716 (HSV1716) is an ICP34.5 null mutant that is selectively replication competent and shown to be safe and to replicate following injection into...

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Veröffentlicht in:	Gene therapy 2004-11, Vol.11 (22), p.1648-1658
Hauptverfasser:	Harrow, S, Papanastassiou, V, Harland, J, Mabbs, R, Petty, R, Fraser, M, Hadley, D, Patterson, J, Brown, S M, Rampling, R
Format:	Artikel
Sprache:	eng
Schlagworte:	Adult Aged Biological and medical sciences Biological Therapy Biomedical and Life Sciences Biomedicine Brain - virology Brain Neoplasms - surgery Brain Neoplasms - therapy Brain Neoplasms - virology Brain tumors Cell Biology Chemotherapy Combined Modality Therapy Female Gene Expression Gene Therapy Genetic Therapy - methods Glioma Glioma - surgery Glioma - therapy Glioma - virology Herpes simplex Herpes Simplex - complications Herpes Simplex - virology Herpes simplex virus Herpesvirus 1, Human Human Genetics Humans Immunocompromised Host Injection Injections, Intraventricular Male Medical prognosis Medical sciences Middle Aged Nanotechnology Neoplasm Recurrence, Local - surgery Neoplasm Recurrence, Local - therapy Neoplasm Recurrence, Local - virology Neuroimaging Neurology Patients Radiation therapy research-article Safety Survival Rate Toxicity Tumors of the nervous system. Phacomatoses Virus Replication
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container_title	Gene therapy
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creator	Harrow, S Papanastassiou, V Harland, J Mabbs, R Petty, R Fraser, M Hadley, D Patterson, J Brown, S M Rampling, R
description	Following standard treatment, the prognosis remains poor in patients with high-grade glioma and new therapies are urgently required. Herpes simplex virus 1716 (HSV1716) is an ICP34.5 null mutant that is selectively replication competent and shown to be safe and to replicate following injection into high-grade glioma. We demonstrate that following surgical resection, HSV1716 is safe when injected into the brain adjacent to excised tumour. In all, 12 patients with recurrent or newly diagnosed high-grade glioma underwent maximal resection of the tumour. HSV1716 was injected into eight to 10 sites around the resulting tumour cavity with the intent of infecting residual tumour cells. As clinically indicated, patients proceeded to further radiotherapy or chemotherapy. There has been no clinical evidence of toxicity associated with the administration of HSV1716. Longitudinal follow-up has allowed the assessment of overall survival compared to that of similar patients not treated with HSV1716. Three patients remain alive and clinically stable at 15, 18 and 22 months postsurgery and HSV1716 injection. Remarkably, the first patient in the trial, who had extensive recurrent disease preprocedure, is alive at 22 months since injection of HSV1716 and 29 months since first diagnosis. Imaging has demonstrated a reduction of residual tumour over the 22-month period despite no further medical intervention since the surgery and HSV1716 injection. In this study, we demonstrate that on the basis of clinical observations, there has been no toxicity following the administration of HSV1716 into the resection cavity rim in patients with high-grade glioma. The survival and imaging data, in addition to the lack of toxicity, give us confidence to proceed to a clinical trial to demonstrate efficacy of HSV1716 in glioma patients.
doi_str_mv	10.1038/sj.gt.3302289
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Herpes simplex virus 1716 (HSV1716) is an ICP34.5 null mutant that is selectively replication competent and shown to be safe and to replicate following injection into high-grade glioma. We demonstrate that following surgical resection, HSV1716 is safe when injected into the brain adjacent to excised tumour. In all, 12 patients with recurrent or newly diagnosed high-grade glioma underwent maximal resection of the tumour. HSV1716 was injected into eight to 10 sites around the resulting tumour cavity with the intent of infecting residual tumour cells. As clinically indicated, patients proceeded to further radiotherapy or chemotherapy. There has been no clinical evidence of toxicity associated with the administration of HSV1716. Longitudinal follow-up has allowed the assessment of overall survival compared to that of similar patients not treated with HSV1716. Three patients remain alive and clinically stable at 15, 18 and 22 months postsurgery and HSV1716 injection. Remarkably, the first patient in the trial, who had extensive recurrent disease preprocedure, is alive at 22 months since injection of HSV1716 and 29 months since first diagnosis. Imaging has demonstrated a reduction of residual tumour over the 22-month period despite no further medical intervention since the surgery and HSV1716 injection. In this study, we demonstrate that on the basis of clinical observations, there has been no toxicity following the administration of HSV1716 into the resection cavity rim in patients with high-grade glioma. 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Herpes simplex virus 1716 (HSV1716) is an ICP34.5 null mutant that is selectively replication competent and shown to be safe and to replicate following injection into high-grade glioma. We demonstrate that following surgical resection, HSV1716 is safe when injected into the brain adjacent to excised tumour. In all, 12 patients with recurrent or newly diagnosed high-grade glioma underwent maximal resection of the tumour. HSV1716 was injected into eight to 10 sites around the resulting tumour cavity with the intent of infecting residual tumour cells. As clinically indicated, patients proceeded to further radiotherapy or chemotherapy. There has been no clinical evidence of toxicity associated with the administration of HSV1716. Longitudinal follow-up has allowed the assessment of overall survival compared to that of similar patients not treated with HSV1716. Three patients remain alive and clinically stable at 15, 18 and 22 months postsurgery and HSV1716 injection. 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subjects	Adult Aged Biological and medical sciences Biological Therapy Biomedical and Life Sciences Biomedicine Brain - virology Brain Neoplasms - surgery Brain Neoplasms - therapy Brain Neoplasms - virology Brain tumors Cell Biology Chemotherapy Combined Modality Therapy Female Gene Expression Gene Therapy Genetic Therapy - methods Glioma Glioma - surgery Glioma - therapy Glioma - virology Herpes simplex Herpes Simplex - complications Herpes Simplex - virology Herpes simplex virus Herpesvirus 1, Human Human Genetics Humans Immunocompromised Host Injection Injections, Intraventricular Male Medical prognosis Medical sciences Middle Aged Nanotechnology Neoplasm Recurrence, Local - surgery Neoplasm Recurrence, Local - therapy Neoplasm Recurrence, Local - virology Neuroimaging Neurology Patients Radiation therapy research-article Safety Survival Rate Toxicity Tumors of the nervous system. Phacomatoses Virus Replication
title	HSV1716 injection into the brain adjacent to tumour following surgical resection of high-grade glioma: safety data and long-term survival
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