Structures of aminoarabinose transferase ArnT suggest a molecular basis for lipid A glycosylation | Zendy

Vasileios I. Petrou | Zendy; Carmen M. Herrera | Zendy; Kathryn M. Schultz | Zendy; Oliver B. Clarke | Zendy; Jérémie Vendôme | Zendy; David Tomasek | Zendy; Surajit Banerjee | Zendy; Kanagalaghatta R. Rajashankar | Zendy; Meagan Belcher Dufrisne | Zendy; Brian Kloss | Zendy; Edda Kloppmann | Zendy; Burkhard Rost | Zendy; Candice S. Klug | Zendy; M. Stephen Trent | Zendy; Lawrence Shapiro | Zendy; Filippo Mancia | Zendy

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Structures of aminoarabinose transferase ArnT suggest a molecular basis for lipid A glycosylation

Author(s) -

Vasileios I. Petrou,

Carmen M. Herrera,

Kathryn M. Schultz,

Oliver B. Clarke,

Jérémie Vendôme,

David Tomasek,

Surajit Banerjee,

Kanagalaghatta R. Rajashankar,

Meagan Belcher Dufrisne,

Brian Kloss,

Edda Kloppmann,

Burkhard Rost,

Candice S. Klug,

M. Stephen Trent,

Lawrence Shapiro,

Filippo Mancia

Publication year - 2016

Publication title -

science

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 12.556

H-Index - 1186

eISSN - 1095-9203

pISSN - 0036-8075

DOI - 10.1126/science.aad1172

Subject(s) - transferase , lipid a , aryl hydrocarbon receptor nuclear translocator , biochemistry , chemistry , bacterial outer membrane , active site , enzyme , stereochemistry , biology , escherichia coli , bacteria , aryl hydrocarbon receptor , transcription factor , gene , genetics

Polymyxins are antibiotics used in the last line of defense to combat multidrug-resistant infections by Gram-negative bacteria. Polymyxin resistance arises through charge modification of the bacterial outer membrane with the attachment of the cationic sugar 4-amino-4-deoxy-l-arabinose to lipid A, a reaction catalyzed by the integral membrane lipid-to-lipid glycosyltransferase 4-amino-4-deoxy-L-arabinose transferase (ArnT). Here, we report crystal structures of ArnT from Cupriavidus metallidurans, alone and in complex with the lipid carrier undecaprenyl phosphate, at 2.8 and 3.2 angstrom resolution, respectively. The structures show cavities for both lipidic substrates, which converge at the active site. A structural rearrangement occurs on undecaprenyl phosphate binding, which stabilizes the active site and likely allows lipid A binding. Functional mutagenesis experiments based on these structures suggest a mechanistic model for ArnT family enzymes.

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