The mutated human gene encoding hepatocyte nuclear factor 1β inhibits kidney formation in developing
            <i>Xenopus</i>
            embryos

Wild, Wiltrud; Strandmann, Elke Pogge von; Nastos, Aristotelis; Senkel, Sabine; Lingott-Frieg, Anja; Bulman, Michael P.; Bingham, Coralie; Ellard, Sian; Hattersley, Andrew T.; Ryffel, Gerhart U.

doi:10.1073/pnas.080010897

Cited by 71 publications

(92 citation statements)

References 42 publications

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“…However, transfecting low amounts of Y352 expression vector, the transactivation potential of the mutant is lower compared with the wild type, whereas at higher amounts, the mutant reaches the transactivation potential of the wild type ( Figure 3B). We previously found a similar behavior for the mutant P328L329, although in this case, at high input, the mutant was even more active than the wild type, suggesting a gain of function mutation (15). To compare directly the transactivation potential between the two mutants, we transfected HeLa cells with increasing concentrations of either of these expression vectors.…”

Section: Mutants Differ In Their Transactivation Potentialmentioning

confidence: 99%

“…The expression vector encoding human HNF1␤ wild-type, P328L329del CCTCT, and R137-K161del have been described (15). The additional HNF1␤ mutations were made by site-directed mutagenesis (Quick Change site-directed mutagenesis kit; Stratagene, La Jolla, CA) on the myc-Rc/CMVHNF1␤ construct using the following primer pairs: S151P, 5'-CGCACCTCCCCCAGCATC-3', 5'-GAT-GCTGGGGGAGGTGCG-3'; E101X, 5'-CTCAACACCTAGGAGGC-GG-3', 5'-CCGCCTCCTAGGTGTTGAG-3'; R177X, 5'-CAGAAAGC-AATGAGAGATC-3', 5'-GATCTCTCATTGCTTTCTG-3'; P159delT, 5'-CAAGGGCACCCCATGAAGACCCAG-3', 5'-CTGGGTCTTCAT-GGGG-TGCCCTTG-3'; Q243delC, 5'-CCC-GCGTCCAGCAAATC-3', 5'-GATTTGCTGGACGC-GGG-3'; A263insGG, 5'-GAGAGAGAGG-GGCCTTAGTGGAGG-3', 5'-CCTCCACTAAGGC-CCCTCTCTCTC-3'; Y352insA, 5'-GAGTGCGCTAACAGCCAGCAG-3', 5'-CTGCTG-GCTGTTAGCGCACTC-3'.…”

Section: Plasmid Constructionsmentioning

confidence: 99%

“…In amphibians, the pronephros is the functional kidney throughout larval development, and the frog Xenopus laevis is most attractive to analyze the molecular and cellular events in pronephros formation (13,14). Using the Xenopus system, we have shown that the introduction of a mutated human HNF1␤ transcription factor into the developing frog embryo leads to partial or even complete agenesis of the pronephric tubules and duct (15).…”

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confidence: 99%

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Distinct Molecular and Morphogenetic Properties of Mutations in the Human HNF1β Gene That Lead to Defective Kidney Development

Bohn

Thomas²,

Turan³

et al. 2003

Journal of the American Society of Nephrology

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Section: Mutants Differ In Their Transactivation Potentialmentioning

confidence: 99%

Section: Plasmid Constructionsmentioning

confidence: 99%

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confidence: 99%

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Distinct Molecular and Morphogenetic Properties of Mutations in the Human HNF1β Gene That Lead to Defective Kidney Development

Bohn

Thomas²,

Turan³

et al. 2003

Journal of the American Society of Nephrology

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“…We found the S36F mutation in a Japanese MODY family and functional analysis showed that it was a gain-of-function mutation [43]. It has been reported that overexpression of wild-type HNF-1b in Xenopus embryos leads to impaired development of the pronephros [44].…”

Section: Hnf-1b Diabetesmentioning

confidence: 99%

Regulation of Pancreatic .BETA.-cell Function by the HNF Transcription Network: Lessons from Maturity-Onset Diabetes of the Young (MODY)

Yamagata

2003

Endocr J

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“…Gain-of-function could be a third mechanism, although its pathogenesis of impaired insulin secretion is not known. Recently, it has been reported that a frameshift mutation (P328L329fsdelCCTCT), identified in a European MODY5 family with renal abnormalities, acts as a gain-of-function mutation (~twofold) [8]. Thus, S36F mutation in the HNF-1b gene might affect the clinical phenotypes in this MODY family.…”

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confidence: 99%

Identification of a gain-of-function mutation in the HNF-1β gene in a Japanese family with MODY

Available¹

2002

Diabetologia

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This mutation was identified with renal dysfunction in all six affected patients in a dominant way of inheritance over three generations and was never observed in 100 control chromosomes.Our study represents the first Italian molecular characterization of a MODY-5 family and further confirm that mutations in HNF-1b gene are associated with a syndrome characterized by MODY and kidney disease.The presence of this splice site HNF-1b mutation support previously reported results [3], suggesting that alterations in the conserved sequence elements at the splice donor site of intron 2 might be a hot spot region for mutations in the HNF-1b gene.Acknowledgements. This work was supported by grants from the Italian Ministry of Health (Ricerca Corrente ± G.Gaslini Institute, 1999) . In order to ascertain the prevalence of HNF1b mutations in early-onset Type II (non-insulin-dependent) diabetes mellitus in Japanese more precisely, we screened a larger group of 111 Japanese patients with early-onset Type II diabetes for mutations in the HNF-1b gene. Ten of the patients were classified as having MODY, with Type II diabetes in at least three generations consistent with autosomal dominant transmission and onset of the disease in patients before 25 years of age. The study group also includes 85 non-obese (BMI < 25 kg/m 2 ) patients with Type II diabetes diagnosed before 15 years of age because our previous study of MODY3 in young Japanese patients suggested that many of these patients have a monogenic form of diabetes [7]. The other sixteen patients were diagnosed with diabetes before 35 years of age and had a family history of diabetes among first-degree relatives. The minimal promoter, coding regions and flanking introns of the HNF-1b gene were directly sequenced in these patients, resulting in the identification of a novel missense mutation (TCC to TTC: S36F) in the heterozygous state in one MODY family. The serine residue at codon 36 is conserved in human, mouse, and rat HNF-1b. This nucleotide alteration was not found in any of the 100 Japanese control subjects (200 alleles). The subject with the S36F mutation is a 46-year-old female who was diagnosed with Type II diabetes at 17 years of age. She also has proteinuria and two cysts (diameter; 6.9 cm and 8.9 cm) in the left kidney. Her serum creatinine concentration is normal (0.6 mg/dl; normal 0.6 to 1.0 mg/dl) at present. Genotyping of other family members with diabetes was done (Fig. 1A). The mutation was found in the subject's elder daughter who was diagnosed with Type II diabetes at 14 years of age (BMI = 22.9) and is being treated with insulin. The same mutation was also present in the 68-year-old mother, who was diagnosed with Type II diabetes around 60 years of age. However, interestingly, the S36F mutation was not identified in the other 17-year-old daughter (BMI = 20.3), whose glycosuria was noticed at 11 years of age by an annual health examination, suggesting that other diabetogenic factors contributed to the development of diabetes in this subject.In order to det...

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The mutated human gene encoding hepatocyte nuclear factor 1β inhibits kidney formation in developing Xenopus embryos

Cited by 71 publications

References 42 publications

Distinct Molecular and Morphogenetic Properties of Mutations in the Human HNF1β Gene That Lead to Defective Kidney Development

Distinct Molecular and Morphogenetic Properties of Mutations in the Human HNF1β Gene That Lead to Defective Kidney Development

Regulation of Pancreatic .BETA.-cell Function by the HNF Transcription Network: Lessons from Maturity-Onset Diabetes of the Young (MODY)

Identification of a gain-of-function mutation in the HNF-1β gene in a Japanese family with MODY

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