Diabetes, Associated Clinical Spectrum, Long-term Prognosis, and Genotype/Phenotype Correlations in 201 Adult Patients With Hepatocyte Nuclear Factor 1B (<i>HNF1B</i>) Molecular Defects

Dubois‐Laforgue, Danièle; Saint‐Martin, Cécile; Coste, Joël; Bellanné‐Chantelot, Christine; Timsit, José

doi:10.2337/dc16-2462

Cited by 134 publications

(191 citation statements)

References 34 publications

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“…The neighboring residues Trp238 (cyan) and Lys237 (blue) are annotated as having a “specific DNA base contact[s]” or being involved in “DNA binding,” respectively (based on NCBI NP_000449.1). Additionally, the variant c.712T>C, p.(Trp238Arg), has been reported as pathogenic . The typical alpha‐helix breaker glycine at position 239 is located at the end of an alpha‐helix motif (residues 240‐252; purple), and its deletion (I1 described herein) or substitution likely disrupts the conformation and positioning of the AAs Lys237 and Trp238 required for DNA binding of the HNF1B transcription factor.…”

Section: Resultsmentioning

confidence: 87%

“…Two missense variants (c.715G>C, p.(Gly239Arg); and c.716G>A, p.(Gly239Glu)) affecting the same AA were reported in a boy with bilateral renal cysts, kidney failure, and diabetes in childhood and in a girl with MODY, renal cysts in the right kidney, agenesis of left kidney, and pancreas atrophy, respectively. Furthermore, a variant affecting the neighboring residue Trp238 (c.712T>C, p.(Trp238Arg)) was described as pathogenic (Figure ) . On the basis of the ACMG criteria ( de novo occurrence, no inclusion in population databases, previously described variant at the same position, affected highly conserved AA, and computationally indicated pathogenicity), we classified the identified variant as pathogenic (class 5).…”

Section: Resultsmentioning

confidence: 99%

“…Genetic variants affecting HNF1B are associated with multiple phenotypes . Aberrations of HNF1B were initially described as causative for maturity‐onset diabetes of the young type 5 (MODY5; MIM #137920) .…”

Section: Introductionmentioning

confidence: 99%

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Prenatal diagnosis of HNF1B‐associated renal cysts: Is there a need to differentiate intragenic variants from 17q12 microdeletion syndrome?

et al. 2019

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Objective 17q12 microdeletions containing HNF1B and intragenic variants within this gene are associated with variable developmental, endocrine, and renal anomalies, often already noted prenatally as hyperechogenic/cystic kidneys. Here, we describe prenatal and postnatal phenotypes of seven individuals with HNF1B aberrations and compare their clinical and genetic data to those of previous studies. Methods Prenatal sequencing and postnatal chromosomal microarray analysis were performed in seven individuals with renal and/or neurodevelopmental phenotypes. We evaluated HNF1B‐related clinical features from 82 studies and reclassified 192 reported intragenic HNF1B variants. Results In a prenatal case, we identified a novel in‐frame deletion p.(Gly239del) within the HNF1B DNA‐binding domain, a mutational hot spot as demonstrated by spatial clustering analysis and high computational prediction scores. The six postnatally diagnosed individuals harbored 17q12 microdeletions. Literature screening revealed variable reporting of HNF1B‐associated clinical traits. Overall, both mutation groups showed a high phenotypic heterogeneity. The reclassification of all previously reported intragenic HNF1B variants provided an up‐to‐date overview of the mutational spectrum. Conclusions We highlight the value of prenatal HNF1B screening in renal developmental diseases. Standardized clinical reporting and systematic classification of HNF1B variants are necessary for a more accurate risk quantification of prenatal and postnatal clinical features, improving genetic counseling and prenatal decision making.

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Section: Resultsmentioning

confidence: 87%

Section: Resultsmentioning

confidence: 99%

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Prenatal diagnosis of HNF1B‐associated renal cysts: Is there a need to differentiate intragenic variants from 17q12 microdeletion syndrome?

et al. 2019

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“…Both HNF1B deletion and truncating mutations would be expected to cause complete loss of a single allele. One hypothesis suggested by DuboisLaforgue et al (1) is that some intragenic HNF1B mutations may exert a dominant negative effect that results in a more severe phenotype. Although truncating mutations anywhere other than the terminal exon usually cause transcript degradation via the nonsense-mediated decay pathway (4), previous work has shown that there is a considerable variation in the degree of nonsense-mediated decay that is seen with different HNF1B mutations (5).…”

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confidence: 99%

Comment on Dubois-Laforgue et al. Diabetes, Associated Clinical Spectrum, Long-term Prognosis, and Genotype/Phenotype Correlations in 201 Adult Patients With Hepatocyte Nuclear Factor 1B (HNF1B) Molecular Defects. Diabetes Care 2017;40:1436–1443

et al. 2017

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“…In a recently published large series of HNF1β syndrome involving 201 adult patients (mutations (n=101) or deletion (n=100)), abnormalities have been found in 16 of 20 males investigated specifically for genital tract anomalies. Seminal abnormalities have been detected in seven, epididymal cysts in four, cryptorchidism in three, varicocele in three, enlarged seminal vesicles in two and absent vas deferens in one of these individuals 13. The exact mechanism of asthenospermia in patients of MODY 5 is still unknown.…”

Section: Discussionmentioning

confidence: 98%

Primary male factor infertility due to asthenospermia in maturity-onset diabetes of the young type 5 (MODY 5): uncommon presentation of an uncommon disease

et al. 2018

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Mutations in hepatocyte nuclear factor-1β gene result in a multisystemic syndrome where a monogenic form of diabetes (maturity-onset diabetes of young type 5; MODY 5) and renal anomalies, usually bilateral multiple cysts are the most characteristic findings. Many of them have pancreatic structural abnormalities as well. A plethora of extrapancreatic manifestations like altered liver function tests, hypomagnesaemia, hyperuricaemia with/without gout and urogenital malformations, particularly in females are also components of the syndrome. Structural malformation of male urogenital tract is rare in MODY 5, even rarer is asthenospermia. We encountered a young non-obese individual having insulin-requiring diabetes following secondary oral agent failure with primary male factor infertility secondary to asthenospermia. A suggestive family history, lack of acanthosis, negative pancreatic autoimmunity, hypomagnesaemia, bilateral renal and epididymal cysts, and absence of body and tail of pancreas pointed towards underlying MODY 5.

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Diabetes, Associated Clinical Spectrum, Long-term Prognosis, and Genotype/Phenotype Correlations in 201 Adult Patients With Hepatocyte Nuclear Factor 1B (HNF1B) Molecular Defects

Cited by 134 publications

References 34 publications

Prenatal diagnosis of HNF1B‐associated renal cysts: Is there a need to differentiate intragenic variants from 17q12 microdeletion syndrome?

Prenatal diagnosis of HNF1B‐associated renal cysts: Is there a need to differentiate intragenic variants from 17q12 microdeletion syndrome?

Comment on Dubois-Laforgue et al. Diabetes, Associated Clinical Spectrum, Long-term Prognosis, and Genotype/Phenotype Correlations in 201 Adult Patients With Hepatocyte Nuclear Factor 1B (HNF1B) Molecular Defects. Diabetes Care 2017;40:1436–1443

Primary male factor infertility due to asthenospermia in maturity-onset diabetes of the young type 5 (MODY 5): uncommon presentation of an uncommon disease

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