Cytostatic Agents in the Management of Malignant Gliomas

Author:

Mikkelsen Tom12

Affiliation:

1. Department of Neurology at Case Western Reserve University, Cleveland, Ohio

2. Departments of Neurology and Neurosurgery at Henry Ford Medical Center, Detroit, Mich.

Abstract

Background: Cytotoxic therapy for malignant gliomas is limited by poor delivery and drug resistance, and local therapy is ineffective in managing migratory cells. However, recent developments in malignant glioma therapy involve trials of cytostatic rather than conventional cytotoxic agents. Methods: The biology of the brain extracellular matrix, tumor invasion, and angiogenesis are reviewed, and the cytostatic agents that inhibit matrix metalloproteinases, angiogenesis, cell proliferation, and signal transduction are discussed, as well as studies of the angiogenic and migratory capacity of malignant brain tumors. Results: Two specific and interrelated areas, anti-invasion (migration) and anti-angiogenesis, are potential areas to develop new treatment strategies. Tumor invasion and angiogenesis are important components of the spread and biologic effects of malignant gliomas. Several proteinase inhibitors are in clinical trial, as well as anti-angiogenic agents and signal transduction cascade inhibitors. Conclusions: Biologic control of brain tumor cell populations may offer a new management approach to add to currently available management options for malignant brain tumors.

Publisher

SAGE Publications

Subject

Oncology,Hematology,General Medicine

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1. Photodynamic therapy of malignant brain tumors (literature review;Vestnik nevrologii, psihiatrii i nejrohirurgii (Bulletin of Neurology, Psychiatry and Neurosurgery);2023-11-27

2. Molecular Imaging of Urogenital Diseases;Seminars in Nuclear Medicine;2014-03

3. Sensitization of cerebral tissue in nude mice with photodynamic therapy induces ADAM17/TACE and promotes glioma cell invasion;Cancer Letters;2008-07

4. Radiobiology and vascular targeting in glioma;Current Opinion in Neurology;2003-12

5. Justification of glioma biology beyond a cellular basis of interpretation;Medical Hypotheses;2003-10

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