| Literature DB >> 33375075 |
Lyubomir Dimitrov Stanchev1,2, Magdalena Marek2, Feng Xian3, Mara Klöhn1, Daniele Silvestro2, Gunnar Dittmar3, Rosa Laura López-Marqués2, Thomas Günther Pomorski1,2.
Abstract
The pleiotropic drug resistance (PDR) transporter Pdr11p is expressed under anaerobic growth conditions at the plasma membrane of the yeast Saccharomyces cerevisiae, where it facilitates the uptake of exogenous sterols. Members of the fungal PDR family contain six conserved cysteines in their extracellular loops (ECL). For the functional analysis of these cysteine residues in Pdr11p, we generated a series of single cysteine-to-serine mutants. All mutant proteins expressed well and displayed robust ATPase activity upon purification. Mass-spectrometry analysis identified two cysteine residues (C582 and C603) in ECL3 forming a disulfide bond. Further characterization by cell-based assays showed that all mutants are compromised in facilitating sterol uptake, protein stability, and trafficking to the plasma membrane. Our data highlight the fundamental importance of all six extracellular cysteine residues for the functional integrity of Pdr11p and provide new structural insights into the PDR family of transporters.Entities:
Keywords: ABC transport proteins; ATPase activity; disulfide bonds; protein trafficking; sterol uptake
Year: 2020 PMID: 33375075 PMCID: PMC7822014 DOI: 10.3390/jof7010002
Source DB: PubMed Journal: J Fungi (Basel) ISSN: 2309-608X