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Role of O ‐linked glucose‐fucose disaccharide modification of thrombospondin type I repeats in protein folding and embryo development
Author(s) -
Holdener Bernadette
Publication year - 2020
Publication title -
the faseb journal
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.709
H-Index - 277
eISSN - 1530-6860
pISSN - 0892-6638
DOI - 10.1096/fasebj.2020.34.s1.00145
Subject(s) - disaccharide , biology , biochemistry , chemistry , genetics
We propose that Protein O‐ fucosyltransferase 2 (POFUT2) and β3‐glucosyltransferase (B3GLCT) function to ensure efficient folding of forty‐nine proteins containing tandemly repeated T hrombospondin T ype 1 R epeats (TSRs). In the endoplasmic reticulum (ER), POFUT2 and B3GLCT recognize properly folded TSRs and act sequentially to add the unusual O‐ linked Glucoseβ1‐3Fucose disaccharide to either a serine or threonine residue located within the POFUT2 consensus sequence (C‐X‐X‐S/T‐C). Once all TSRs are modified the target protein exits the ER. In crystal structures the disaccharide forms H‐bonds and van der Waals interactions with underlying amino acids in the TSR, raising the possibility that the disaccharide functions as a surrogate amino acid to stabilize the correctly folded TSR. Results from in vitro folding/refolding assays provide evidence that the disaccharide stabilizes the TSR fold and accelerates the overall rate of protein folding. Consistent with this prediction, loss of POFUT2 or B3GLCT in cell culture impairs trafficking of POFUT2/B3GLCT targets. To begin to evaluate the function of the disaccharide in vivo , we generated mouse loss of function mutations in Pofut2 and B3glct. Loss of Pofut2 causes early embryo lethality due to a block in gastrulation. In contrast, B3glct animals survive, but have craniofacial and skeletal abnormalities, defects in pigmentation, soft tissue syndactyly, and develop hydrocephalus. The mouse B3glct phenotype shares similarities to Peters Plus syndrome in humans, caused by recessive mutations in B3GLCT. The distinct differences in the effects of these mutations during mouse development support a model whereby the O‐ linked fucose is essential for folding and secretion of all POFUT2/B3GLCT target proteins and that B3GLCT‐mediated extension to the glucose‐fucose disaccharide is only required by a subset of sensitive targets. Support or Funding Information These studies were supported by funding from NIH R01 HD090156 and NIH R01 HD096030 and 2019 Hydrocephalus Association Innovator Award.Model for how POFUT2/B3GLCT mediated addition of the O‐ linked glucose‐fucose disaccharide promotes efficient folding of target proteins containing the Thrombospondin Type 1 Repeats (TSR) fold. Addition of fucose prevents reentry of the TSR to the folding cycle and stabilizes the fold. Extension with glucose provides further stability to the TSR. Once the target protein is fully modified it exits the endoplasmic reticulum (ER).