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Cleavage of human MDR1 mRNA by a hammerhead ribozyme
[摘要]

We designed a hammerhead ribozyme which site-specifically cleaved the GUC sequence in codon 179 of MDR1 mRNA. The cleavage site was 6 amino acids upstream from the drug binding site and was considered sufficiently close to the essential locus for P-glycoprotein function. The ribozyme cleaved the MDR1 mRNA under physiological conditions in vitro. The cleavage was dependent on ribozyme concentration and on incubation time. Mg2+ ion was essential for the cleavage. These results show that a potentially useful tool is at hand which may inactivate MDR1 mRNA and revert the multidrug resistance phenotype.

[发布日期]  [发布机构] 
[效力级别]  [学科分类] 生物化学/生物物理
[关键词] Hammerhead ribozyme;Multidrug resistance;MDR;multidrug resistance;FBS;fetal bovine serum;VCR;vincristine;TMQ;trimetrexate;RT-PCR;reverse transcription polymerase chain reaction;CTAB;cetyl-trimethylammonium bromide [时效性] 
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