AI Article Synopsis
- Researchers implanted modified murine cells that produce retroviral vectors with the HSV-TK gene into the brains of rodents, showing tumor regression after administering ganciclovir (GCV).
- In a study with 15 patients having recurrent malignant brain tumors, some smaller tumors (around 1.4 ml) showed antitumor activity.
- The findings indicated that the presence of vector-producing cells was maintained for a week, but limited gene transfer means better methods for delivering the gene are necessary for effective clinical outcomes.
Article Abstract
Intratumoral implantation of murine cells modified to produce retroviral vectors containing the herpes simplex virus-thymidine kinase (HSV-TK) gene induces regression of experimental brain tumors in rodents after ganciclovir (GCV) administration. We evaluated this approach in 15 patients with progressive growth of recurrent malignant brain tumors. Antitumor activity was detected in five of the smaller tumors (1.4 +/- 0.5 ml). In situ hybridization for HSV-TK demonstrated survival of vector-producing cells (VPCs) at 7 days but indicated limited gene transfer to tumors, suggesting that indirect, "bystander," mechanisms provide local antitumor activity in human tumors. However, the response of only very small tumors in which a high density of vector-producing cells had been placed suggests that techniques to improve delivery and distribution of the therapeutic gene will need to be developed if clinical utility is to be achieved with this approach.
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| http://dx.doi.org/10.1038/nm1297-1354 | DOI Listing |
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