3i2w
From Proteopedia
Crystal structure of EFC/F-BAR domain of Drosophila Syndapin/PACSIN
Structural highlights
Evolutionary Conservation Check, as determined by ConSurfDB. You may read the explanation of the method and the full data available from ConSurf. Publication Abstract from PubMedPACSIN/Syndapin proteins are membrane-active scaffolds that participate in endocytosis. The structure of the Drosophila Syndapin N-terminal EFC domain reveals a crescent shaped antiparallel dimer with a high affinity for phosphoinositides and a unique membrane-inserting prong upon the concave surface. Combined structural, biochemical and reverse genetic approaches in zebrafish define an important role for Syndapin orthologue, Pacsin3, in the early formation of the notochord during embryonic development. In pacsin3-morphant embryos, midline convergence of notochord precursors is defective as axial mesodermal cells fail to polarize, migrate and differentiate properly. The pacsin3 morphant phenotype of a stunted body axis and contorted trunk is rescued by ectopic expression of Drosophila Syndapin, and depends critically on both the prong that protrudes from the surface of the bowed Syndapin EFC domain and the ability of the antiparallel dimer to bind tightly to phosphoinositides. Our data confirm linkage between directional migration, endocytosis and cell specification during embryonic morphogenesis and highlight a key role for Pacsin3 in this coupling in the notochord. Structural requirements for PACSIN/Syndapin operation during zebrafish embryonic notochord development.,Edeling MA, Sanker S, Shima T, Umasankar PK, Honing S, Kim HY, Davidson LA, Watkins SC, Tsang M, Owen DJ, Traub LM PLoS One. 2009 Dec 3;4(12):e8150. PMID:19997509[1] From MEDLINE®/PubMed®, a database of the U.S. National Library of Medicine. References
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Categories: Drome | Large Structures | Edeling, M A | Owen, D J | Traub, L M | Efc | Endocytosis | Fbar | Sh3 domain
