Biotinated Probe Containing a Long-Terminal Repeat Hybridized to a Mouse Colon Tumor and Normal Tissue

23 December 1983

journal article
research article
Published by American Association for the Advancement of Science (AAAS) in Science

Vol. 222 (4630), 1339-1341
https://doi.org/10.1126/science.6689218

Abstract

The cloned complementary DNA pMCT-1, which contains an intracisternal A particle long-terminal repeat, is more highly expressed in a mouse colon tumor than in the normal mouse colon. In situ hybridization of biotin-substituted pMCT-1 to fixed frozen sections shows that expression of pMCT-1 is seen throughout the tumor and is highly heterogeneous on a cellular basis, while expression is undetectable in any cell in the normal colonic mucosa.

This publication has 20 references indexed in Scilit:

Elevated expression of an endogenous retroviral long terminal repeat in a mouse colon tumor.
Journal of Biological Chemistry, 1984
Detection of viral genomes in cultured cells and paraffin-embedded tissue sections using biotin-labeled hybridization probes
Virology, 1983
Biological Diversity in Metastatic Neoplasms: Origins and Implications
Science, 1982
Visna DNA synthesis and the tempo of infection in vitro
Virology, 1982
Measles Virus Nucleotide Sequences: Detection by Hybridization in Situ
Science, 1981
Detection of poly A⁺RNA in sea urchin eggs and embryos by quantitative in situ hybridization
Nucleic Acids Research, 1981
The pathogenesis of cancer metastasis
Nature, 1980
Sequences associated with intracisternal a particles are reiterated in the mouse genome
Cell, 1977
Detection of myosin heavy chain mRNA during myogenesis in tissue culture by in vitro and in situ hybridization
Cell, 1977
Localisation of cellular globin messenger RNA by in situ hybridisation to complementary DNA
FEBS Letters, 1973

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