Literature DB >> 15674397

Variability in infectivity of primary cell cultures of human brain tumors with HSV-1 amplicon vectors.

M A Rueger1, A Winkeler, H Miletic, C Kaestle, R Richter, G Schneider, R Hilker, M T Heneka, R I Ernestus, J A Hampl, C Fraefel, A H Jacobs.   

Abstract

We investigated the variability in infectivity of cells in primary brain tumor samples from different patients using an HSV-1 amplicon vector. We studied the infectivity of HSV-1 amplicon vectors in tumor samples derived from neurosurgical resections of 20 patients. Cells were infected with a definite amount of HSV-1 amplicon vector HSV-GFP. Transduction efficiency in primary tumor cell cultures was compared to an established human glioma line. Moreover, duration of transgene expression was monitored in different tumor cell types. All primary cell cultures were infectable with HSV-GFP with variable transduction efficiencies ranging between 3.0 and 42.4% from reference human Gli36 Delta EGFR glioma cells. Transduction efficiency was significantly greater in anaplastic gliomas and meningiomas (26.7+/-17.4%) compared to more malignant tumor types (glioblastomas, metastases; 11.2+/-8.5%; P=0.05). To further investigate the possible underlying mechanism of this variability, nectin-1/HevC expression was analyzed and was found to contribute, at least in part, to this variability in infectability. The tumor cells expressed the exogenous gene for 7 to 61 days with significant shorter expression in glioblastomas (18+/-13 d) compared to anaplastic gliomas (42+/-24 d; P<0.05). Interindividual variability of infectivity by HSV-1 virions might explain, at least in part, why some patients enrolled in gene therapy for glioblastoma in the past exhibited a sustained response to HSV-1-based gene- and virus therapy. Infectivity of primary tumor samples from respective patients should be tested to enable the development of efficient and safe herpes vector-based gene and virus therapy for clinical application.

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Year:  2005        PMID: 15674397     DOI: 10.1038/sj.gt.3302462

Source DB:  PubMed          Journal:  Gene Ther        ISSN: 0969-7128            Impact factor:   5.250


  14 in total

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3.  FasL and FADD delivery by a glioma-specific and cell cycle-dependent HSV-1 amplicon virus enhanced apoptosis in primary human brain tumors.

Authors:  Ivy A Ho; Wai H Ng; Paula Y Lam
Journal:  Mol Cancer       Date:  2010-10-13       Impact factor: 27.401

4.  Effective treatment of an orthotopic xenograft model of human glioblastoma using an EGFR-retargeted oncolytic herpes simplex virus.

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5.  Nectin-1 (HveC) is expressed at high levels in neural subtypes that regulate radial migration of cortical and cerebellar neurons of the developing human and murine brain.

Authors:  Emese Prandovszky; Szatmár Horváth; Levente Gellért; S Krisztián Kovács; Zoltán Janka; József Toldi; Deepak Shukla; Tibor Vályi-Nagy
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6.  Preventing growth of brain tumors by creating a zone of resistance.

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7.  Engineered herpes simplex viruses efficiently infect and kill CD133+ human glioma xenograft cells that express CD111.

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Journal:  J Neurooncol       Date:  2009-06-12       Impact factor: 4.130

8.  Differential SELEX in human glioma cell lines.

Authors:  Laura Cerchia; Carla Lucia Esposito; Andreas H Jacobs; Bertrand Tavitian; Vittorio de Franciscis
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9.  Expression of HSV-1 receptors in EBV-associated lymphoproliferative disease determines susceptibility to oncolytic HSV.

Authors:  P-Y Wang; M A Currier; L Hansford; D Kaplan; E A Chiocca; H Uchida; W F Goins; J B Cohen; J C Glorioso; T H van Kuppevelt; X Mo; T P Cripe
Journal:  Gene Ther       Date:  2012-12-20       Impact factor: 5.250

10.  Pediatric glioma stem cells: biologic strategies for oncolytic HSV virotherapy.

Authors:  Gregory K Friedman; Joel Raborn; Virginia M Kelly; Kevin A Cassady; James M Markert; G Yancey Gillespie
Journal:  Front Oncol       Date:  2013-02-28       Impact factor: 6.244

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