Literature DB >> 29153507

Structural Evidence for a Role of the Multi-functional Human Glycoprotein Afamin in Wnt Transport.

Andreas Naschberger1, Andrew Orry2, Stefan Lechner3, Matthew W Bowler4, Didier Nurizzo5, Mislav Novokmet6, Markus A Keller7, Gregor Oemer6, Daniele Seppi8, Martin Haslbeck9, Kathrin Pansi8, Hans Dieplinger3, Bernhard Rupp10.   

Abstract

Afamin, a human plasma glycoprotein and putative transporter of hydrophobic molecules, has been shown to act as extracellular chaperone for poorly soluble, acylated Wnt proteins, forming a stable, soluble complex with functioning Wnt proteins. The 2.1-Å crystal structure of glycosylated human afamin reveals an almost exclusively hydrophobic binding cleft capable of harboring large hydrophobic moieties. Lipid analysis confirms the presence of lipids, and density in the primary binding pocket of afamin was modeled as palmitoleic acid, presenting the native O-acylation on serine 209 in human Wnt3a. The modeled complex between the experimental afamin structure and a Wnt3a homology model based on the XWnt8-Fz8-CRD fragment complex crystal structure is compelling, with favorable interactions comparable with the crystal structure complex. Afamin readily accommodates the conserved palmitoylated serine 209 of Wnt3a, providing a structural basis how afamin solubilizes hydrophobic and poorly soluble Wnt proteins.
Copyright © 2017 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Wnt proteins; Wnt3a-afamin complex model; acylation; afamin; cell signaling; crystal structure; glycosylation; lipid transport; plasma glycoprotein

Mesh:

Substances:

Year:  2017        PMID: 29153507     DOI: 10.1016/j.str.2017.10.006

Source DB:  PubMed          Journal:  Structure        ISSN: 0969-2126            Impact factor:   5.006


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