Hypoxic-response elements in the oncolytic parvovirus Minute virus of mice do not allow for increased vector production at low oxygen concentration

Servais, Charlotte; Caillet-Fauquet, Perrine; Draps, Marie-Louise; Velu, Thierry; Launoit, Yvan de; Brandenburger, Anne-Nicole

doi:10.1099/vir.0.81754-0

Cited by 8 publications

(5 citation statements)

References 27 publications

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“…While one study showed that GADD34 expression (induced by hypoxia in our study) impairs replication of vesicular stomatitis virus,30 an RNA virus, another study argued that hypoxia does not affect vesicular stomatitis virus replication, using indirect evidence in the form of viral replication in hypoxic areas of a tumor 31. Hypoxia has also been shown to inhibit the replication of the oncolytic DNA virus, Minute virus of mice 32. Further, hypoxia has been demonstrated to inhibit the replication of other DNA viruses that have not yet been used as oncolytic viruses, such as simian virus 40 (ref.…”

Section: Discussionmentioning

confidence: 51%

Hypoxia Enhances the Replication of Oncolytic Herpes Simplex Virus

et al. 2009

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Hypoxia contributes to the resistance of tumors to conventional therapies. We hypothesized that their replication in hypoxic environments like brain or oral mucosa would make oncolytic herpes simplex viruses (HSVs) such as G207 (which has undergone clinical trials) replicate to a greater extent in hypoxic tumors like glioblastoma. Hypoxic cultured U87 cells yielded 4% more wild-type HSV (P = 0.04) and 3.6-fold more G207 (P = 0.001) after 48 hours of infection when compared with normoxic cells. Real-time RT-PCR confirmed a fivefold hypoxia-induced U87 upregulation of GADD34 mRNA, a factor complementing the γ34.5 gene deletion in G207. The viral yield under conditions of hypoxia, as against normoxia, in GADD34 siRNA-treated U87 cells was 65% of that in control siRNA-treated cells. Treating subcutaneous U87 tumors in athymic mice with erythropoietin lowered the tumoral hypoxic fraction from 57.5 to 24.5%. Tumoral hypoxia dropped to 2.5% during 4 hours/day of hyperbaric chamber treatment. Each tumor-oxygenating maneuver reduced the G207 yield fourfold (P = 0.0001). Oncolytic HSV G207 exhibited enhanced replication in hypoxic environments, partly on account of increased GADD34 expression in hypoxic cells. The unique tropism of oncolytic HSVs for hypoxic environments contrasts with the hypoxia-mediated impairment of standard (radiation, chemotherapy) and other experimental therapies, and enhances HSV's appeal and efficacy in treating tumors like glioblastoma.

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Section: Discussionmentioning

confidence: 51%

Hypoxia Enhances the Replication of Oncolytic Herpes Simplex Virus

et al. 2009

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“…Hypoxia (1% O 2 ) induces lytic replication of EBV [92] and Kaposi sarcoma-associated herpesvirus [93], but suppresses replication of oncolytic parvovirus Minute virus of mice [94], adenovirus [95] or Moloney murine leukemia virus [96]. Primary T cells cultured at 3–6% O 2 maintain an intracellular redox environment similar to the in vivo situation, as opposed to T cells cultured at atmospheric 21% O 2 , in which the intracellular redox state is significantly altered [97].…”

Section: Effect Of Hypoxia On Hiv-1mentioning

confidence: 99%

Role of Cellular Iron and Oxygen in the Regulation of HIV-1 Infection

2013

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Despite efficient antiretroviral therapy, eradication of HIV-1 infection is challenging and requires novel biological insights and therapeutic strategies. Among other physiological and environmental factors, intracellular iron greatly affects HIV-1 replication. Higher iron stores were shown to be associated with faster progression of HIV-1 infection and to inversely correlate with the survival of HIV-1 infected patients. Iron is required for several steps in the HIV-1 life cycle, including reverse transcription, HIV-1 gene expression and capsid assembly. Here, the authors present a comprehensive review of the molecular mechanisms involved in iron- and oxygen-mediated regulation of HIV-1 replication. We also propose key intracellular pathways that may be involved in regulating HIV-1 replication, via protein kinase complexes, CDK9/cyclin T1 and CDK 2/cyclin E, protein phosphatase-1 and other host factors.

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“…The two features of tumor cells that attract parvoviruses are mitosis and hypoxia. The environment ruled by hypoxia--inducible transcription factor-α and hypoxia-responsive element favors parvovirus replication [338]. The oncotropic oncoselective minute viruses of mice (MVMi and prototype MVMp) replicate in human tumor cells in vitro without displaying any pathogenicity in the human host.…”

Section: Myxomavirusmentioning

confidence: 99%

Natural and genetically engineered viral agents for oncolysis and gene therapy of human cancers

Sinkovics

Horváth

2008

Arch. Immunol. Ther. Exp.

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Based on personal acquaintances and experience dating back to the early 1950s, the senior author reviews the history of viral therapy of cancer. He points out the difficulties encountered in the treatment of human cancers, as opposed by the highly successful viral therapy of experimentally maintained tumors in laboratory animals, especially that of ascites carcinomas in mice. A detailed account of viral therapy of human tumors with naturally oncolytic viruses follows, emphasizing the first clinical trials with viral oncolysates. The discrepancy between the high success rates, culminating in cures, in the treatment of tumors of laboratory animals, and the moderate results, such as stabilizations of disease, partial responses, very rare complete remissions, and frequent relapses with virally treated human tumors is recognized. The preclinical laboratory testing against established human tumor cell lines that were maintained in tissue cultures for decades, and against human tumors extricated from their natural habitat and grown in xenografts, may not yield valid results predictive of the viral therapy applied against human tumors growing in their natural environment, the human host. Since the recent discovery of the oncosuppressive efficacy of bacteriophages, the colon could be regarded as the battlefield, where incipient tumor cells and bacteriophages vie for dominance. The inner environment of the colon will be the teaching ground providing new knowledge on the value of the anti-tumor efficacy of phage-induced innate anti-tumor immune reactions. Genetically engineered oncolytic viruses are reviewed next. The molecular biology of viral oncolysis is explained in details. Elaborate efforts are presented to elucidate how gene product proteins of oncolytic viruses switch off the oncogenic cascades of cancer cells. The facts strongly support the conclusion that viral therapy of human cancers will remain in the front lines of modern cancer therapeutics. It may be a combination of naturally oncolytic viruses and wild-type viruses rendered oncolytic and harmless by genetic engineering, that will induce complete remissions of human tumors. It may be necessary to co-administer certain chemotherapeutic agents, advanced cancer vaccines, or even immune lymphocytes, and targeted therapeuticals, to ascertain, that remissions induced by the viral agents will remain complete and durable; will co-operate with anti-tumor host immune reactions, and eventually will result in cures of advanced metastatic human cancers.

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Hypoxic-response elements in the oncolytic parvovirus Minute virus of mice do not allow for increased vector production at low oxygen concentration

Cited by 8 publications

References 27 publications

Hypoxia Enhances the Replication of Oncolytic Herpes Simplex Virus

Hypoxia Enhances the Replication of Oncolytic Herpes Simplex Virus

Role of Cellular Iron and Oxygen in the Regulation of HIV-1 Infection

Natural and genetically engineered viral agents for oncolysis and gene therapy of human cancers

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