Identification of the gene (SEDL) causing X-linked spondyloepiphyseal dysplasia tarda

Gedeon, Agi; Colley, Alison; Jamieson, Robyn V; Thompson, Elizabeth; Rogers, John G.; Sillence, David; Tiller, George E.; Mulley, John C.; Gécz, Jozef

doi:10.1038/11976

Cited by 172 publications

(210 citation statements)

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“…Both transcripts from the two chromosomes are expressed in the affected tissue, epiphyseal cartilage, and also in most other tissues (17). A compensatory effect of SEDL originating from chromosome 19 could contribute to the absence of a phenotypic effect in most tissues of SEDT patients (12).…”

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confidence: 99%

“…Trs20p, the SEDL orthologue in yeast, is also a component of yeast TRAPP I and TRAPP II. The identification of SEDL as the gene responsible for SEDT was unexpected, since different types of chondrodysplasias and skeletal dysplasias are accounted mostly by the genes encoding structural molecules of cartilage such as collagen and cartilage oligomeric matrix protein (12,16). A pseudogene of SEDL on human chromosome 19 was found to encode a protein identical to that of SEDL.…”

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confidence: 99%

“…SEDT is caused by mutations in SEDL located at human chromosome Xp22 (12)(13)(14). SEDL (also known as Sedlin) is a component of human TRAPP as shown by an immunoblotting analysis (15).…”

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Crystal Structure of SEDL and Its Implications for a Genetic Disease Spondyloepiphyseal Dysplasia Tarda

Jang

Kim

Cho

et al. 2002

Journal of Biological Chemistry

100

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SEDL is an evolutionarily highly conserved protein in eukaryotic organisms. Deletions or point mutations in the SEDL gene are responsible for the genetic disease spondyloepiphyseal dysplasia tarda (SEDT), an X-linked skeletal disorder. SEDL has been identified as a component of the transport protein particle (TRAPP), critically involved in endoplasmic reticulum-to-Golgi vesicle transport. Herein, we report the 2.4 Å resolution structure of SEDL, which reveals an unexpected similarity to the structures of the N-terminal regulatory domain of two SNAREs, Ykt6p and Sec22b, despite no sequence homology to these proteins. The similarity and the presence of unusually many solvent-exposed apolar residues of SEDL suggest that it serves regulatory and/or adaptor functions through multiple protein-protein interactions. Of the four known missense mutations responsible for SEDT, three mutations (S73L, F83S, V130D) map to the protein interior, where the mutations would disrupt the structure, and the fourth (D47Y) on a surface at which the mutation may abrogate functional interactions with a partner protein.Intracellular targeting and fusion of transport vesicles in eukaryotes are tightly regulated to avoid inappropriate mixing of the contents in different compartments. Central components of the membrane fusion are the proteins denoted as SNAREs 1 (soluble N-ethylmaleimide-sensitive factor attachment receptor proteins). SNAREs constitute a superfamily of proteins that share a highly conserved sequence motif, the SNARE motif composed of 60 -70 amino acids (1). Most SNAREs are membrane proteins anchored on vesicular carriers (v-SNARE) and target organelles (t-SNARE) (1). Association of the SNARE domains between v-and t-SNAREs to form a helical bundle, termed the core complex (2), is believed to be the prime event that drives membrane fusion (3, 4). While the specific pairing of v-and t-SNAREs is one mechanism of providing the fidelity of membrane fusion, other proteins or protein complexes such as the transport protein particle (TRAPP) are known to provide further specificity by controlling the tethering process, in which a transport vesicle is properly docked on target membrane prior to pairing of SNAREs (5). TRAPP is localized to an early Golgi compartment (6) and is able to exchange the nucleotide of Ypt1p GTPase, which is an upstream event of v-and t-SNARE interactions (7,8). Recent in vitro transport studies showed that yeast TRAPP I binds COPII, the vesicle coat derived from the endoplasmic reticulum (ER), indicating that TRAPP I is the receptor for tethering COPII vesicles to Golgi membranes (6). The TRAPP complexes (TRAPP I and TRAPP II) are composed of 7-10 different polypeptides, which are highly conserved in evolution, with the yeast subunits sharing between 29 and 54% sequence identity with their human counterparts (9). The biochemical function of any of the constituent proteins is virtually unknown, although the TRAPP complex was shown to stimulate nucleotide exchange on the Ypt1p and the Ypt31/32 GTPases (10).Spond...

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Crystal Structure of SEDL and Its Implications for a Genetic Disease Spondyloepiphyseal Dysplasia Tarda

Jang

Kim

Cho

et al. 2002

Journal of Biological Chemistry

100

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“…8 DNA extraction was performed using the salting-out method. 9 Exons 3, 4, 5 and 6 (containing the coding sequence) of SEDL and adjacent splice sites were amplified by PCR and sequenced in both directions, as described by Gedeon et al 1 Sequencing reactions were performed with Big-Dye terminators and an ABI 3730 automated sequencer. All of the sequences were compared against the normal sequences of unrelated controls and the UCSC and NCBI databases.…”

Section: Patients and Clinical Diagnosismentioning

confidence: 99%

“…SEDL is a highly conserved gene with orthologs identified in yeast, flies and vertebrates, and it is widely expressed in tissues, including fibroblasts, lymphoblasts and fetal cartilage. 1 It contains six exons 2 and spans a genomic region of approximately 23 kb on Xp22 in the human genome; it also escapes from X-inactivation. 3 As a small gene with alternative splicing involving exon 2, 4 ubiquitously expressed SEDL mRNA is about 2.8 kb in size.…”

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confidence: 99%

Noncanonical and canonical splice sites: a novel mutation at the rare noncanonical splice-donor cut site (IVS4+1A>G) of SEDL causes variable splicing isoforms in X-linked spondyloepiphyseal dysplasia tarda

Xiong

Gao

et al. 2008

Eur J Hum Genet

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X-linked spondyloepiphyseal dysplasia tarda can be caused by mutations in the SEDL gene. This study describes an interesting novel mutation (IVS4 þ 1A4G) located exactly at the rare noncanonical AT-AC consensus splicing donor point of SEDL, which regained the canonical GT-AG consensus splicing junction in addition to several other rarer noncanonical splice patterns. The mutation activated several cryptic splice sites and generated the production of seven erroneous splicing isoforms, which we confirmed by sequencing of RT-PCR products and resequencing of cDNA clones. All the practical splice donors/acceptors were further assessed using FSPLICE 1.0 and SPL(M) Platforms to predict potential splice sites in genomic DNA. Subsequently, the expression levels of SEDL among the affected patients, carriers and controls were estimated using real-time quantitative PCR. Expression analyses showed that the expression levels of SEDL in both patients and carriers were decreased. Taken together, these results illustrated how disruption of the AT donor site in a rare AT-AC intron, leading to a canonical GT donor site, resulted in a multitude of aberrant transcripts, thus impairing exon definition. The unexpected splicing patterns resulting from the special mutation provide additional challenges and opportunities for understanding splicing mechanisms and specificity.

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SEDL(SEDT) Gene

Gedeon¹,

Gécz²

2002

Wiley Encyclopedia of Molecular Medicine

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Identification of the gene (SEDL) causing X-linked spondyloepiphyseal dysplasia tarda

Cited by 172 publications

References 21 publications

Crystal Structure of SEDL and Its Implications for a Genetic Disease Spondyloepiphyseal Dysplasia Tarda

Crystal Structure of SEDL and Its Implications for a Genetic Disease Spondyloepiphyseal Dysplasia Tarda

Noncanonical and canonical splice sites: a novel mutation at the rare noncanonical splice-donor cut site (IVS4+1A>G) of SEDL causes variable splicing isoforms in X-linked spondyloepiphyseal dysplasia tarda

SEDL(SEDT) Gene

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