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Structures of Pathogenic Fungal FKBP12s Reveal Possible Self-Catalysis Function.

MBio.. 2016-04; 
Tonthat NK, Juvvadi PR, Zhang H, Lee SC, Venters R, Spicer L, Steinbach WJ, Heitman J, Schumacher MA.
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Codon Optimization ... Protein expression and purification.Genes encoding the C.áalbicans and A.áfumigatus FKBP12s that were codon optimized for E.ácoli expression were purchased from the GenScript Corporation (Piscataway, NJ) and subcloned into pET15b such that a hexahistidine tag (His ... Get A Quote
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摘要

Invasive fungal infections remain difficult to treat and require novel targeting strategies. The 12-kDa FK506-binding protein (FKBP12) is a ubiquitously expressed peptidyl-prolyl isomerase with considerable homology between fungal pathogens and is thus a prime candidate for future targeting efforts to generate a panfungal strategy. Despite decades of research on FKBPs, their substrates and mechanisms of action remain unclear. Here we describe structural, biochemical, and in vivo analyses of FKBP12s from the pathogenic fungi Candida albicans, Candida glabrata, and Aspergillus fumigatus Strikingly, multiple apo A. fumigatus and C. albicans FKBP12 crystal structures revealed a symmetric, intermolecular interaction... More

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