Open AccessJournal Article
Tumor Chemosensitivity Conferred by Inserted Herpes Thymidine Kinase Genes: Paradigm for a Prospective Cancer Control Strategy
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TLDR
The lack of highly exploitable biochemical differences between normal tissues and some tumors can be circumvented by a strategy utilizing gene insertion prophylactically to create tissue mosaicism for drug sensitivity, thereby ensuring that any tumor arising clonally will differ from part of the normal cell population.Abstract:
The lack of highly exploitable biochemical differences between normal tissues and some tumors can theoretically be circumvented by a strategy utilizing gene insertion prophylactically to create tissue mosaicism for drug sensitivity, thereby ensuring that any tumor arising clonally will differ from part of the normal cell population. Elements of the strategy were tested with neoplastic BALB/c murine cell lines bearing the herpes thymidine kinase gene. Exposure to the herpes thymidine kinase-specific substrate 9-([2-hydroxy-1-(hydroxymethyl)ethoxy]methyl)guanine ablated the clonogenic potential of the cells in vitro, and administration of this drug to BALB/c mice bearing tumors produced by the cell lines uniformly induced complete regression of the tumors. The observed responses to therapy imply that the strategy may prove valuable when the genetic technology needed for its human implementation becomes available.read more
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Selectivity of action of an antiherpetic agent, 9-(2-hydroxyethoxymethyl)guanine
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TL;DR: Acycloguanosine triphosphate inhibits herpes simplex virus DNA polymerase (DNA nucleotidyltransferase) 10-30 times more effectively than cellular (HeLa S3) DNA polymerases, contributing to the drug's selectivity.
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Cellular Oncogenes and Multistep Carcinogenesis
TL;DR: Two dozen cellular proto-oncogenes have been discovered to date through the study of retroviruses and the use of gene transfer, and recent work provides experimental strategies by which many of them, as well as oncogene of DNA tumor viruses, may be placed into functional categories.
Journal ArticleDOI
The Chromosomal Basis of Human Neoplasia
TL;DR: It is proposed that chromosomal rearrangements play a central role in human neoplasia and may exert their effects through related genomic mechanisms and a translocation could serve to place an oncogene next to an activating DNA sequence, a deletion to eliminate anOncogene repressor, and trisomy to carry extra gene dosage.
Journal ArticleDOI
Somatic expression of herpes thymidine kinase in mice following injection of a fusion gene into eggs
Ralph L. Brinster,Howard Y. Chen,Myrna E. Trumbauer,Allen W. Senear,Raphael Warren,Richard D. Palmiter +5 more
TL;DR: A plasmid containing the structural gene for thymidine kinase from herpes simplex virus fused to the promoter/regulatory region of the mouse metallothionein-I gene was injected into the pronucleus of fertilized one-cell mouse eggs; the eggs were subsequently reimplanted into the oviducts of pseudopregnant mice.