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Conference Paper: Mechanistic insight into point mutations in sedlin that result in spondyloepiphyseal dysplasia tarda

TitleMechanistic insight into point mutations in sedlin that result in spondyloepiphyseal dysplasia tarda
Authors
Choi, MYChan, CChan, DLuk, KDKCheah, KSETanner, JA
Issue Date2006
PublisherFederation of American Societies for Experimental Biology.
Citation
The 2006 Annual Meeting of the Federation of American Societies for Experimental Biology (EB), San Francisco, CA., 1-5 April 2006. In The FASEB Journal, 2006, v. 20 n. 5 (meeting abstracts), p. A1364 How to Cite?
AbstractSpondyloepiphyseal dysplasia tarda (SEDT) is the only osteochondrodysplasia which has been shown so far to be due to a defect in trafficking, via mutations in a gene (SEDL) that encodes sedlin, involved in ER-Golgi transport. A number of mutations have previously been identified in patients with SEDT including nonsense mutations, missense mutations, deletions, insertions and splicing errors. Here, we investigate the functional properties of four point mutants of sedlin, D47Y, S73L, F83S and V130D, and compare to the wild type protein. On expression in E. coli in a number of conditions, only WT and D47Y were found to express in the soluble fraction, whilst the other three point mutants entered inclusion bodies. D47Y and WT sedlin were found to be very similar by circular dichroism, steady-state fluorescence and chaotrope induced unfolding, suggesting that D47Y only caused a local perturbation to structure compared to all other mutants which led to misfolding. We also tested expression of all mutants in a variety of mammalian cell lines. All point mutants expressed at significantly lower levels compared to wild type and localization was investigated. We were able to correlate specific mutations with severity of mild clinical symptoms. Our data provides a mechanistic understanding at the protein level of the varying clinical severities of spondyloepiphyseal dysplasia tarda and lays a foundation for further work into the specific protein-protein interactions of sedlin. This work was funded by the Hong Kong UGC under the Area of Excellence Programme in Developmental Genomics and Skeletal Research.
Persistent Identifierhttp://hdl.handle.net/10722/67991
ISSN
0892-6638
2021 Impact Factor: 5.834
2020 SCImago Journal Rankings: 1.709

 

DC FieldValueLanguage
dc.contributor.authorChoi, MYen_HK
dc.contributor.authorChan, Cen_HK
dc.contributor.authorChan, Den_HK
dc.contributor.authorLuk, KDKen_HK
dc.contributor.authorCheah, KSEen_HK
dc.contributor.authorTanner, JAen_HK
dc.date.accessioned2010-09-06T06:00:15Z-
dc.date.available2010-09-06T06:00:15Z-
dc.date.issued2006en_HK
dc.identifier.citationThe 2006 Annual Meeting of the Federation of American Societies for Experimental Biology (EB), San Francisco, CA., 1-5 April 2006. In The FASEB Journal, 2006, v. 20 n. 5 (meeting abstracts), p. A1364en_HK
dc.identifier.issn0892-6638en_HK
dc.identifier.urihttp://hdl.handle.net/10722/67991-
dc.description.abstractSpondyloepiphyseal dysplasia tarda (SEDT) is the only osteochondrodysplasia which has been shown so far to be due to a defect in trafficking, via mutations in a gene (SEDL) that encodes sedlin, involved in ER-Golgi transport. A number of mutations have previously been identified in patients with SEDT including nonsense mutations, missense mutations, deletions, insertions and splicing errors. Here, we investigate the functional properties of four point mutants of sedlin, D47Y, S73L, F83S and V130D, and compare to the wild type protein. On expression in E. coli in a number of conditions, only WT and D47Y were found to express in the soluble fraction, whilst the other three point mutants entered inclusion bodies. D47Y and WT sedlin were found to be very similar by circular dichroism, steady-state fluorescence and chaotrope induced unfolding, suggesting that D47Y only caused a local perturbation to structure compared to all other mutants which led to misfolding. We also tested expression of all mutants in a variety of mammalian cell lines. All point mutants expressed at significantly lower levels compared to wild type and localization was investigated. We were able to correlate specific mutations with severity of mild clinical symptoms. Our data provides a mechanistic understanding at the protein level of the varying clinical severities of spondyloepiphyseal dysplasia tarda and lays a foundation for further work into the specific protein-protein interactions of sedlin. This work was funded by the Hong Kong UGC under the Area of Excellence Programme in Developmental Genomics and Skeletal Research.-
dc.languageengen_HK
dc.publisherFederation of American Societies for Experimental Biology.en_HK
dc.relation.ispartofThe FASEB Journalen_HK
dc.titleMechanistic insight into point mutations in sedlin that result in spondyloepiphyseal dysplasia tardaen_HK
dc.typeConference_Paperen_HK
dc.identifier.openurlhttp://library.hku.hk:4550/resserv?sid=HKU:IR&issn=0892-6638&volume=&spage=873.9&epage=&date=2006&atitle=Mechanistic+insight+into+point+mutations+in+sedlin+that+result+in+spondyloepiphyseal+dysplasia+tardaen_HK
dc.identifier.emailChoi, MY: meiychoi@yahoo.caen_HK
dc.identifier.emailChan, C: andrcc@gmail.comen_HK
dc.identifier.emailChan, D: chand@hkucc.hku.hken_HK
dc.identifier.emailLuk, KDK: hrmoldk@hkucc.hku.hken_HK
dc.identifier.emailCheah, KSE: hrmbdkc@hkusua.hku.hken_HK
dc.identifier.emailTanner, JA: jatanner@hku.hken_HK
dc.identifier.authorityLuk, KDK=rp00333en_HK
dc.identifier.authorityCheah, KSE=rp00342en_HK
dc.identifier.authorityTanner, JA=rp00495en_HK
dc.identifier.hkuros115425en_HK
dc.identifier.volume20-
dc.identifier.issue5 (meeting abstracts)-
dc.identifier.spageA1364-
dc.identifier.epageA1364-
dc.identifier.issnl0892-6638-

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