Missense mutations near the N-glycosylation site of the A2 domain lead to various intracellular trafficking defects in coagulation factor VIII

dc.citation.doi10.1038/srep45033
dc.citation.issn2045-2322
dc.citation.jtitleScientific Reports
dc.citation.spage14
dc.citation.volume7
dc.contributor.authorWei, W.
dc.contributor.authorZheng, C. L.
dc.contributor.authorZhu, M.
dc.contributor.authorZhu, X. F.
dc.contributor.authorYang, R. C.
dc.contributor.authorMisra, Saurav
dc.contributor.authorZhang, B.
dc.contributor.authoreidmisras
dc.contributor.kstateMisra, Saurav
dc.date.accessioned2017-11-30T21:40:53Z
dc.date.available2017-11-30T21:40:53Z
dc.date.issued2017-03-22
dc.date.published2017
dc.descriptionCitation: Wei, W., Zheng, C. L., Zhu, M., Zhu, X. F., Yang, R. C., Misra, S., & Zhang, B. (2017). Missense mutations near the N-glycosylation site of the A2 domain lead to various intracellular trafficking defects in coagulation factor VIII. Scientific Reports, 7, 14. doi:10.1038/srep45033
dc.description.abstractMissense mutation is the most common mutation type in hemophilia. However, the majority of missense mutations remain uncharacterized. Here we characterize how hemophilia mutations near the unused N-glycosylation site of the A2 domain (N582) of FVIII affect protein conformation and intracellular trafficking. N582 is located in the middle of a short 3(10)-helical turn (D580-S584), in which most amino acids have multiple hemophilia mutations. All 14 missense mutations found in this 3(10)-helix reduced secretion levels of the A2 domain and full-length FVIII. Secreted mutants have decreased activities relative to WT FVIII. Selected mutations also lead to partial glycosylation of N582, suggesting that rapid folding of local conformation prevents glycosylation of this site in wild-type FVIII. Protease sensitivity, stability and degradation of the A2 domain vary among mutants, and between non-glycosylated and glycosylated species of the same mutant. Most of the mutants interact with the ER chaperone BiP, while only mutants with aberrant glycosylation interact with calreticulin. Our results show that the short 3(10)-helix from D580 to S584 is critical for proper biogenesis of the A2 domain and FVIII, and reveal a range of molecular mechanisms by which FVIII missense mutations lead to moderate to severe hemophilia A.
dc.identifier.urihttp://hdl.handle.net/2097/38333
dc.relation.urihttps://doi.org/10.1038/srep45033
dc.rightsAttribution 4.0 International (CC BY 4.0)
dc.rights.urihttps://creativecommons.org/licenses/by/4.0/
dc.subjectVon-Willebrand-Factor
dc.subjectTo-Golgi Transport
dc.subjectHemophilia-A
dc.subjectEndothelial-Cells
dc.subjectFactor-V
dc.subjectProtein Glycosylation
dc.titleMissense mutations near the N-glycosylation site of the A2 domain lead to various intracellular trafficking defects in coagulation factor VIII
dc.typeArticle

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