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Self-interaction of a SNARE transmembrane domain promotes the hemifusion-to-fusion transition |
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| Authors: | Hofmann Mathias W Peplowska Karolina Rohde Jan Poschner Bernhard C Ungermann Christian Langosch Dieter |
| Institution: | Lehrstuhl Chemie der Biopolymere, Technische Universit?t München, Weihenstephaner Berg 3, 85354 Freising, Germany. |
| Abstract: | SNARE proteins mediate intracellular fusion of eukaryotic membranes. Some SNAREs have previously been shown to dimerise via interaction of their transmembrane domains. However, the functional significance of these interactions had remained unclear. Here, we show that mutating alternate faces of the transmembrane helix of the yeast vacuolar Q-SNARE Vam3p reduces the ability of the full-length protein to induce contents mixing in yeast vacuole fusion to different extents. Examination of liposome fusion induced by synthetic transmembrane domains revealed that inner leaflet mixing is delayed relative to outer leaflet mixing, suggesting that fusion transits through a hemifusion intermediate. Interestingly, one of the mutations impaired inner leaflet mixing in the liposome system. This suggests that the defect seen in vacuolar contents mixing is due to partial arrest of the reaction at hemifusion. Since covalent dimerisation of this mutant recovered wild-type behaviour, homodimerisation of a SNARE transmembrane domain appears to control the transition of a hemifusion intermediate to complete lipid mixing. |
| Keywords: | SNARE soluble NSF (N-ethylmaleimide-sensitive factor) attachment protein receptor GPI glycosylphosphatidyinositol TMD transmembrane domain PC phosphatidylcholine PE phosphatidylethanolamine PS phosphatidylserine NBD 7-nitro-2-1 3-benzoxadiazol-4-yl Rh Lissamine Rhodamine B Sulfonyl TFE trifluoroethanol wt wild-type |
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