Literature DB >> 25981043

Transmembrane Complexes of DAP12 Crystallized in Lipid Membranes Provide Insights into Control of Oligomerization in Immunoreceptor Assembly.

Konstantin Knoblich1, Soohyung Park2, Mariam Lutfi3, Leonie van 't Hag4, Charlotte E Conn5, Shane A Seabrook6, Janet Newman6, Peter E Czabotar1, Wonpil Im2, Matthew E Call7, Melissa J Call7.   

Abstract

The membrane-spanning α helices of single-pass receptors play crucial roles in stabilizing oligomeric structures and transducing biochemical signals across the membrane. Probing intermolecular transmembrane interactions in single-pass receptors presents unique challenges, reflected in a gross underrepresentation of their membrane-embedded domains in structural databases. Here, we present two high-resolution structures of transmembrane assemblies from a eukaryotic single-pass protein crystallized in a lipidic membrane environment. Trimeric and tetrameric structures of the immunoreceptor signaling module DAP12, determined to 1.77-Å and 2.14-Å resolution, respectively, are organized by the same polar surfaces that govern intramembrane assembly with client receptors. We demonstrate that, in addition to the well-studied dimeric form, these trimeric and tetrameric structures are made in cells, and their formation is competitive with receptor association in the ER. The polar transmembrane sequences therefore act as primary determinants of oligomerization specificity through interplay between charge shielding and sequestration of polar surfaces within helix interfaces.
Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.

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Year:  2015        PMID: 25981043      PMCID: PMC4449314          DOI: 10.1016/j.celrep.2015.04.045

Source DB:  PubMed          Journal:  Cell Rep            Impact factor:   9.423


  39 in total

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2.  Exploring the in meso crystallization mechanism by characterizing the lipid mesophase microenvironment during the growth of single transmembrane α-helical peptide crystals.

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5.  Structural Basis and Functional Role of Intramembrane Trimerization of the Fas/CD95 Death Receptor.

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6.  Transmembrane features governing Fc receptor CD16A assembly with CD16A signaling adaptor molecules.

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  10 in total

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