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August 10, 2004; 63 (3) Views & Reviews

Genetically modified adenoviruses against gliomas

From bench to bedside

Candelaria Gomez-Manzano, W.K. Alfred Yung, Ramon Alemany, Juan Fueyo
First published August 9, 2004, DOI: https://doi.org/10.1212/01.WNL.0000133302.15022.7F
Candelaria Gomez-Manzano
MD
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W.K. Alfred Yung
MD
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Ramon Alemany
PhD
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Juan Fueyo
MD
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Citation
Genetically modified adenoviruses against gliomas
From bench to bedside
Candelaria Gomez-Manzano, W.K. Alfred Yung, Ramon Alemany, Juan Fueyo
Neurology Aug 2004, 63 (3) 418-426; DOI: 10.1212/01.WNL.0000133302.15022.7F

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Abstract

Oncolytic or tumor-selective adenoviruses are constructed as novel antiglioma therapies. After infection, the invading genetic adenoviral material is activated within the host cell. E1A and E1B adenoviral proteins are expressed immediately. E1A protein interacts with cell cycle regulatory proteins, such as retinoblastoma (Rb), driving the cell into the S phase and ensuing viral replication. The action of E1A stimulates the cellular p53 tumor suppressor system, which results in growth arrest or apoptosis, and halts adenovirus replication. However, adenoviral E1B interacts with p53 protein, preventing the DNA replication process from being abrogated by the induction of p53-mediated apoptosis. It was subsequently hypothesized that mutant adenoviruses that were unable to express wild-type E1A or E1B proteins could not replicate in normal cells with functional Rb or p53 pathways but instead would replicate and kill glioma cells that had defects in the regulation of these tumor suppressor pathways. Mutant E1B adenoviruses have already entered the clinical setting as an experimental treatment for patients with malignant gliomas. Mutant E1A adenoviruses are now in preclinical development as antiglioma therapy. In this review, the authors describe the mechanisms underlying the production of oncolytic adenoviruses, preclinical and clinical experiences with specific oncolytic adenoviruses, and the possibilities of combining mutant oncolytic adenoviruses with gene therapy or conventional therapies for managing malignant gliomas.

  • Received August 18, 2003.
  • Accepted March 8, 2004.
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  • Article
    • Abstract
    • Tumor-selective adenovirus.
    • E1B-mutant oncolytic adenovirus: the dl1520 paradigm.
    • E1A-mutant adenoviruses: the Delta-24 paradigm.
    • Modification of the tropism of adenoviruses: the RGD paradigm.
    • Tumor selectivity through transcriptional regulation of adenoviral genes.
    • Combining oncolysis and gene therapy.
    • Combining oncolysis and chemotherapy.
    • Combining oncolysis and radiotherapy.
    • Other oncolytic agents used for the management of human brain tumors.
    • Potential pitfalls of oncolytic adenoviral therapy.
    • Acknowledgments
    • Footnotes
    • References
  • Figures & Data
  • Info & Disclosures
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