Literature DB >> 28069938

Crystal structure and mechanistic basis of a functional homolog of the antigen transporter TAP.

Anne Nöll1, Christoph Thomas1, Valentina Herbring1, Tina Zollmann1, Katja Barth1,2, Ahmad Reza Mehdipour3, Thomas M Tomasiak4, Stefan Brüchert1, Benesh Joseph2, Rupert Abele1, Vincent Oliéric5, Meitian Wang5, Kay Diederichs6, Gerhard Hummer3,7, Robert M Stroud8, Klaas M Pos1, Robert Tampé9.   

Abstract

ABC transporters form one of the largest protein superfamilies in all domains of life, catalyzing the movement of diverse substrates across membranes. In this key position, ABC transporters can mediate multidrug resistance in cancer therapy and their dysfunction is linked to various diseases. Here, we describe the 2.7-Å X-ray structure of heterodimeric Thermus thermophilus multidrug resistance proteins A and B (TmrAB), which not only shares structural homology with the antigen translocation complex TAP, but is also able to restore antigen processing in human TAP-deficient cells. TmrAB exhibits a broad peptide specificity and can concentrate substrates several thousandfold, using only one single active ATP-binding site. In our structure, TmrAB adopts an asymmetric inward-facing state, and we show that the C-terminal helices, arranged in a zipper-like fashion, play a crucial role in guiding the conformational changes associated with substrate transport. In conclusion, TmrAB can be regarded as a model system for asymmetric ABC exporters in general, and for TAP in particular.

Entities:  

Keywords:  ABC transporter; conformational dynamics; membrane proteins; peptide transport; transporter associated with antigen processing

Mesh:

Substances:

Year:  2017        PMID: 28069938      PMCID: PMC5278451          DOI: 10.1073/pnas.1620009114

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


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