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Volumn 211, Issue 8-9, 2001, Pages 458-465
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Reduction of Cre recombinase toxicity in proliferating Drosophila cells by estrogen-dependent activity regulation
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Author keywords
Chromosomal aberration; Clones; Cre recombinase; loxP; Toxicity
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Indexed keywords
BETA GALACTOSIDASE;
CRE RECOMBINASE;
ESTROGEN;
ESTROGEN RECEPTOR;
GENE PRODUCT;
LIGAND;
ANIMAL CELL;
ANIMAL TISSUE;
ARTICLE;
CELL PROLIFERATION;
CONTROLLED STUDY;
CYTOTOXICITY;
DROSOPHILA MELANOGASTER;
ENZYME ACTIVITY;
ESTROGEN ACTIVITY;
GENETIC ANALYSIS;
GENETIC MODEL;
GENETIC RECOMBINATION;
LIGAND BINDING;
MAMMAL CELL;
MOLECULAR CLONING;
MOSAICISM;
NONHUMAN;
PRIORITY JOURNAL;
PROTEIN DOMAIN;
PROTEIN EXPRESSION;
TISSUE SPECIFICITY;
TRANSGENE;
ANIMALS;
ANIMALS, GENETICALLY MODIFIED;
APOPTOSIS;
ATTACHMENT SITES, MICROBIOLOGICAL;
CELL DIVISION;
CELL LINE;
DOSE-RESPONSE RELATIONSHIP, DRUG;
DROSOPHILA MELANOGASTER;
ENZYME ACTIVATION;
ESTRADIOL;
EYE;
GENE EXPRESSION REGULATION, DEVELOPMENTAL;
HUMANS;
INTEGRASES;
MUTAGENESIS, SITE-DIRECTED;
ORGAN SPECIFICITY;
RECEPTORS, ESTROGEN;
RECOMBINANT FUSION PROTEINS;
RECOMBINATION, GENETIC;
TRANSGENES;
VIRAL PROTEINS;
WING;
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EID: 0034811154
PISSN: 0949944X
EISSN: None
Source Type: Journal
DOI: 10.1007/s004270100167 Document Type: Article |
Times cited : (52)
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References (21)
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