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A genome-scale drug discovery pipeline uncovers new therapeutic targets and a unique p97 allosteric binding site in Schistosoma mansoni

biorxiv. 2016-03; 
Dylon R Stephens; Ho Yee Joyce Fung; Yan Han; Jue Liang; Zhe Chen; Joseph Ready; James J Collins
Products/Services Used Details Operation
PCR Cloning and Subcloning wildtype Schistosoma mansoni p97 (Smp_018240) or Homo sapiens p97 ( P55072 ) were synthesized and cloned into pET28a(+) with a C-terminal 6x His tag by GenScript (Piscaaway, NJ). E. coli BL21 (DE3) containing the desired plasmid were grown in LB medium containing 50 g/L kanamycin while shaking at 37 C to an Get A Quote

摘要

Schistosomes are parasitic flatworms that infect more than 200 million people globally. However, there is a shortage of molecular tools that enable the discovery of potential drug targets within schistosomes. Thus, praziquantel has remained the frontline treatment for schistosomiasis despite known liabilities. Here, we have conducted a genome-wide study in S. mansoni using the human druggable genome as a bioinformatic template to identify essential genes within schistosomes bearing similarity to catalogued drug targets. Then, we assessed these candidate targets in silico using a set of unbiased criteria to determine which possess ideal characteristics for a ready-made drug discovery campaign. Following this pri... More

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