TY - JOUR
T1 - Human wild-type SEDL protein functionally complements yeast Trs20p but some naturally occurring SEDL mutants do not
AU - Gécz, Jozef
AU - Shaw, Marie A.
AU - Bellon, Jennifer R.
AU - De Barros Lopes, Miguel
N1 - Funding Information:
This work was supported by grant from the Australian National Health and Medical Research Council. JB and MBL acknowledge the support of the Grape and Wine Research Development Corporation.
PY - 2003/11/27
Y1 - 2003/11/27
N2 - X-linked spondyloepiphyseal dysplasia tarda (SEDT, or SEDL) is a primary skeletal dysplasia affecting mostly spinal vertebral bodies and epiphyses. Previously, we have identified the SEDL gene and determined the spectrum of 21 different SEDL causing mutations. The SEDL gene is a highly conserved gene with an as yet unknown function. The yeast SEDL protein ortholog, Trs20p, has been isolated as a member of a large multi-protein complex (∼10 proteins) called transport protein particle (TRAPP), which is involved in endoplasmic reticulum (ER)-to-Golgi transport. While the SEDL gene mutations cause a tissue-specific (epiphyses) and relatively mild phenotype, the Trs20p function is essential for the yeast cell. We now provide evidence that recombinant human SEDL protein is able to functionally complement the Saccharomyces cerevisiae TRS20 (TRAPP subunit 20 gene) knockout mutant. This finding strongly supports the speculated conserved nature of the SEDL/Trs20p function. To shed further light on the SEDL/Trs20p protein function, five different naturally occurring SEDL gene mutations have been tested in complementation studies. While two truncation mutations (157delAT and C271T) and one missense mutation (G139T) were unable to rescue the trs20Δ lethal phenotype, two other missense mutations (C218T and T389A) did complement trs20Δ. Interestingly, there is no obvious correlation between the nature and position of the SEDL mutation and the clinical severity of the disorder among the human SEDL patients. Although the identification of complementing SEDL gene mutations may suggest the existence of subtle phenotypic differences among SEDL patients, it might also point towards the identification of SEDL protein residues/domains specific for normal, vertebrate bone growth.
AB - X-linked spondyloepiphyseal dysplasia tarda (SEDT, or SEDL) is a primary skeletal dysplasia affecting mostly spinal vertebral bodies and epiphyses. Previously, we have identified the SEDL gene and determined the spectrum of 21 different SEDL causing mutations. The SEDL gene is a highly conserved gene with an as yet unknown function. The yeast SEDL protein ortholog, Trs20p, has been isolated as a member of a large multi-protein complex (∼10 proteins) called transport protein particle (TRAPP), which is involved in endoplasmic reticulum (ER)-to-Golgi transport. While the SEDL gene mutations cause a tissue-specific (epiphyses) and relatively mild phenotype, the Trs20p function is essential for the yeast cell. We now provide evidence that recombinant human SEDL protein is able to functionally complement the Saccharomyces cerevisiae TRS20 (TRAPP subunit 20 gene) knockout mutant. This finding strongly supports the speculated conserved nature of the SEDL/Trs20p function. To shed further light on the SEDL/Trs20p protein function, five different naturally occurring SEDL gene mutations have been tested in complementation studies. While two truncation mutations (157delAT and C271T) and one missense mutation (G139T) were unable to rescue the trs20Δ lethal phenotype, two other missense mutations (C218T and T389A) did complement trs20Δ. Interestingly, there is no obvious correlation between the nature and position of the SEDL mutation and the clinical severity of the disorder among the human SEDL patients. Although the identification of complementing SEDL gene mutations may suggest the existence of subtle phenotypic differences among SEDL patients, it might also point towards the identification of SEDL protein residues/domains specific for normal, vertebrate bone growth.
KW - Bone dysplasia
KW - Functional complementation
KW - Spondyloepiphyseal dysplasia tarda
KW - TRS20
KW - X-linked
KW - Yeast model
UR - http://www.scopus.com/inward/record.url?scp=0242298582&partnerID=8YFLogxK
U2 - 10.1016/S0378-1119(03)00819-9
DO - 10.1016/S0378-1119(03)00819-9
M3 - Article
C2 - 14597397
AN - SCOPUS:0242298582
SN - 0378-1119
VL - 320
SP - 137
EP - 144
JO - Gene
JF - Gene
IS - 1-2
ER -