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Ionic Interactions Promote Transmembrane Helix-Helix Association Depending on Sequence Context |
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| Authors: | Jana R. Herrmann Angelika Fuchs Thomas Eckert Stephanie Unterreitmeier Dmitrij Frishman |
| Affiliation: | 1 Lehrstuhl für Chemie der Biopolymere, Department für biowissenschaftliche Grundlagen, Technische Universität München, Weihenstephaner Berg 3, 85354 Freising, Germany 2 Munich Center For Integrated Protein Science (CIPSM), Munich, Germany 3 Lehrstuhl für Genomorientierte Bioinformatik, Department für biowissenschaftliche Grundlagen, Technische Universität München, Wissenschaftszentrum Weihenstephan, 85350 Freising, Germany |
| Abstract: | Folding and oligomerization of integral membrane proteins frequently depend on specific interactions of transmembrane helices. Interacting amino acids of helix-helix interfaces may form complex motifs and exert different types of molecular forces. Here, a set of strongly self-interacting transmembrane domains (TMDs), as isolated from a combinatorial library, was found to contain basic and acidic residues, in combination with polar nonionizable amino acids and C-terminal GxxxG motifs. Mutational analyses of selected sequences and reconstruction of high-affinity interfaces confirmed the cooperation of these residues in homotypic interactions. Probing heterotypic interaction indicated the presence of interhelical charge-charge interactions. Furthermore, simple motifs of an ionizable residue and GxxxG are significantly overrepresented in natural TMDs, and a specific combination of these motifs exhibits high-affinity heterotypic interaction. We conclude that intramembrane charge-charge interactions depend on sequence context. Moreover, they appear important for homotypic and heterotypic interactions of numerous natural TMDs. |
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