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Cloning and in vivo metabolizing activity study of CYP3A4 on amiodarone drug residues: A possible probiotic and therapeutic option

Biomed Pharmacother. 2020-04; 
Banoth S,?Tangutur AD,?Anthappagudem A,?Ramaiah J,?Bhukya B
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Codon Optimization Codon optimization was carried out for the sequence and later the sequence was deposited in National Centre for Biotechnology Information database (GenBank MG604235), synthesized at GenScript, USA and received in a carrier vector pUC57 which has?lacZ?promoter and a kanamycin selection marker. Get A Quote

摘要

BACKGROUND: Amiodarone represents a principal antiarrhythmic pharmaceutical drug available in the market for the treatment of ventricular arrhythmias. However, despite its better efficacy, the usage of amiodarone is associated with extracardiac toxicity. The human body evolved a system of cytochrome P450 enzymes which play an essential role in the metabolism of harmful foreign substances. Therefore, CYP enzymes may either lead to the elimination or degradation of the leftover drug residues. OBJECTIVE: The present study focused on successful utilization of Saccharomyces cerevisiae strain OBS2 with probiotic- cum- therapeutic potential and expressing in silico enhanced human cytochrome P4503A4 for the degradation... More

關鍵詞

Amiodarone; Cardiovascular disease (CVD); Cytochrome P450 3A4; Docking simulation; Gene expression; Molecular cloning; Saccharomyces cerevisiae
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