Neoplasm Metastasis Clinical Trial
Official title:
Gene Therapy for the Treatment of Brain Tumors Using Intra-Tumoral Transduction With the Thymidine Kinase Gene and Intravenous Ganciclovir
Malignant brain tumors are responsible for a significant amount of deaths in children and
adults. Even with advances in surgery, radiation therapy, and chemotherapy, many patients
diagnosed with a malignant brain tumor survive only months to weeks.
In an attempt to improve the prognosis for these patients, researchers have developed a new
approach to brain tumor therapy. This approach makes use of DNA technology to transfer genes
sensitive to therapy into the cells of the tumor.
Infections with the herpes simplex virus can cause cold sores in the area of the mouth. A
drug called ganciclovir (Cytovene) can kill the virus. Ganciclovir is effective because the
herpes virus contains a gene (Herpes-Thymidine Kinase TK gene) that is sensitive to the drug.
Researchers have been able to separate this gene from the virus.
Using DNA technology, researchers hope to transfer and implant the TK gene into tumor cells
making them sensitive to ganciclovir. In theory, giving patients ganciclovir will kill all
tumor cells that have the TK gene incorporated into them.
Malignant brain tumors are responsible for significant morbidity and mortality in both
pediatric and adult populations. These common tumors present an enormous therapeutic
challenge due to their poor outcome despite radical surgery, high dose radiotherapy and
chemotherapy. Survival of patients from the time of diagnosis is measured in months and
recurrence after treatment is associated with a life expectancy of weeks.
In an attempt to improve this grim prognosis of patients with malignant brain tumors (both
primary tumors and secondary metastasis from systemic cancer such as melanoma, lung and
breast cancer), we developed a novel approach to the therapy of brain tumors. This approach
makes use of recombinant DNA technology to transfer a sensitivity gene into a brain tumor.
This is achieved by direct injection of the tumor with a cell line actively producing a
retroviral vector carrying a gene conferring drug sensitivity to the tumor. A retroviral
vector is a mouse retrovirus genetically engineered to replace its own genes with a new gene.
Such vectors are capable of "infecting" mammalian cells and stably incorporate their new
genetic material into the genome of the infected host. The producer cell is an NIH 3T3 cell
that has been genetically engineered to continually produce retroviral vectors. The new gene
is incorporated into the genome of the tumor cells and expresses the protein which is encoded
by the new gene. This protein (the herpes simplex virus enzyme thymidine kinase, HS-tk)
sensitizes the tumor cells to an antiviral drug (ganciclovir, GCV) which is a natural
substrate for HS-tk. The enzymatic process induced by GCV leads to death of a natural
substrate for HS-tk. The enzymatic process induced by GCV leads to death of the cell
expressing the herpes TK activity, i.e., death of the tumor cells. Since the HS-tk enzyme
which is normally present in mammalian cells has very low affinity for GCV, systemic toxicity
related to this mechanism is not observed. This type of in vivo gene transfer has several
unique features. First, these retroviral-vectors will only integrate and express their genes
in cells which are actively synthesizing DNA. Therefore, surrounding non-proliferating normal
brain tissue should not acquire the HS-tk gene and will remain insensitive to GCV. Second,
all of the transduced tumor cells (and retroviral vector producing cells) will be killed by
the host immune response and/or GCV treatment eliminating potential concern about insertional
mutagenesis giving rise to malignant cells.
This is the first clinical attempt to treat malignant tumors in human beings by in-vivo
genetic manipulation of tumor's genome.
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