TY - JOUR
T1 - Mutations in GLIS3 are responsible for a rare syndrome with neonatal diabetes mellitus and congenital hypothyroidism
AU - Senée, Valérie
AU - Chelala, Claude
AU - Duchatelet, Sabine
AU - Feng, Daorong
AU - Blanc, Hervé
AU - Cossec, Jack Christophe
AU - Charon, Céline
AU - Nicolino, Marc
AU - Boileau, Pascal
AU - Cavener, Douglas R.
AU - Bougnères, Pierre
AU - Taha, Doris
AU - Julier, Cécile
N1 - Funding Information:
We thank F. Badghaish for contacting and providing detailed clinical information on family NDH2, and we thank the families for their kind participation to this study. We are grateful to M. Pontoglio for discussions and critical reading of the manuscript. We thank P. Ghandil and S. Blanchard for their technical contributions. This work was funded in part by a joined Juvenile Diabetes Research Foundation (JDRF)/INSERM/Fondation pour la Recherche Médicale (FRM) grant to C.J. and by a US National Institutes of Health (NIH) grant (NIDDK62049) to D.R.C. We thank the Hospices Civils de Lyon for their support.
PY - 2006/6
Y1 - 2006/6
N2 - We recently described a new neonatal diabetes syndrome associated with congenital hypothyroidism, congenital glaucoma, hepatic fibrosis and polycystic kidneys. Here, we show that this syndrome results from mutations in GLIS3, encoding GLI similar 3, a recently identified transcription factor. In the original family, we identified a frameshift mutation predicted to result in a truncated protein. In two other families with an incomplete syndrome, we found that affected individuals harbor deletions affecting the 11 or 12 5′-most exons of the gene. The absence of a major transcript in the pancreas and thyroid (deletions from both families) and an eye-specific transcript (deletion from one family), together with residual expression of some GLIS3 transcripts, seems to explain the incomplete clinical manifestations in these individuals. GLIS3 is expressed in the pancreas from early developmental stages, with greater expression in β cells than in other pancreatic tissues. These results demonstrate a major role for GLIS3 in the development of pancreatic β cells and the thyroid, eye, liver and kidney.
AB - We recently described a new neonatal diabetes syndrome associated with congenital hypothyroidism, congenital glaucoma, hepatic fibrosis and polycystic kidneys. Here, we show that this syndrome results from mutations in GLIS3, encoding GLI similar 3, a recently identified transcription factor. In the original family, we identified a frameshift mutation predicted to result in a truncated protein. In two other families with an incomplete syndrome, we found that affected individuals harbor deletions affecting the 11 or 12 5′-most exons of the gene. The absence of a major transcript in the pancreas and thyroid (deletions from both families) and an eye-specific transcript (deletion from one family), together with residual expression of some GLIS3 transcripts, seems to explain the incomplete clinical manifestations in these individuals. GLIS3 is expressed in the pancreas from early developmental stages, with greater expression in β cells than in other pancreatic tissues. These results demonstrate a major role for GLIS3 in the development of pancreatic β cells and the thyroid, eye, liver and kidney.
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U2 - 10.1038/ng1802
DO - 10.1038/ng1802
M3 - Article
C2 - 16715098
AN - SCOPUS:33745268851
SN - 1061-4036
VL - 38
SP - 682
EP - 687
JO - Nature Genetics
JF - Nature Genetics
IS - 6
ER -
