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Structure-based analysis of CysZ-mediated cellular uptake of sulfate

Author: Assur Zahra
Banerjee Surajit
Belcher Dufrisne Meagan Leigh
Clarke Oliver B.
Giesem M. Hunter
Hendrickson Wayne A.
Kloss Brian
Leal-Pinto Edgar
Liu Qun
Logothetis Diomedes
Love James
Mancia Filippo
Punta Marco
Quick Matthias
Rajashankar Kanagalaghatta R.
Rost Burkhard
Tabuso Shantelle
Wiriyasermkul Pattama
Publication venue: 'Columbia University Libraries/Information Services'
Publication date: 01/01/2018
Field of study

Sulfur, most abundantly found in the environment as sulfate (SO42-), is an essential element in metabolites required by all living cells, including amino acids, co-factors and vitamins. However, current understanding of the cellular delivery of SO42- at the molecular level is limited. CysZ has been described as a SO42- permease, but its sequence family is without known structural precedent. Based on crystallographic structure information, SO42- binding and flux experiments, we provide insight into the molecular mechanism of CysZ-mediated translocation of SO42- across membranes. CysZ structures from three different bacterial species display a hitherto unknown fold and have subunits organized with inverted transmembrane topology. CysZ from Pseudomonas denitrificans assembles as a trimer of antiparallel dimers and the CysZ structures from two other species recapitulate dimers from this assembly. Mutational studies highlight the functional relevance of conserved CysZ residues

Columbia University Academic Commons

Structural basis for catalysis in a CDP-alcohol phosphotransferase.

Author: Banerjee Surajit
Byfield Rushelle
Clarke Oliver B
Cohn Raphael
Graziano Joseph H
Kloss Brian
Mancia Filippo
Rajashankar Kanagalaghatta R
Sciara Giuliano
Shapiro Lawrence
Slavkovic Vesna
Tabuso Shantelle
Tomasek David
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2014
Field of study

The CDP-alcohol phosphotransferase (CDP-AP) family of integral membrane enzymes catalyses the transfer of a substituted phosphate group from a CDP-linked donor to an alcohol acceptor. This is an essential reaction for phospholipid biosynthesis across all kingdoms of life, and it is catalysed solely by CDP-APs. Here we report the 2.0 Å resolution crystal structure of a representative CDP-AP from Archaeoglobus fulgidus. The enzyme (AF2299) is a homodimer, with each protomer consisting of six transmembrane helices and an N-terminal cytosolic domain. A polar cavity within the membrane accommodates the active site, lined with the residues from an absolutely conserved CDP-AP signature motif (D(1)xxD(2)G(1)xxAR...G(2)xxxD(3)xxxD(4)). Structures in the apo, CMP-bound, CDP-bound and CDP-glycerol-bound states define functional roles for each of these eight conserved residues and allow us to propose a sequential, base-catalysed mechanism universal for CDP-APs, in which the fourth aspartate (D4) acts as the catalytic base