A Novel Mutation in the Upstream Open Reading Frame of the CDKN1B Gene Causes a MEN4 Phenotype

Occhi, Gianluca; Regazzo, Daniela; Trivellin, Giampaolo; Boaretto, Francesca; Ciato, Denis; Bobisse, Sara; Ferasin, Sergio; Cetani, Filomena; Pardi, Elena; Korbonits, Márta; Pellegata, Natalia S.; Sidarovich, Viktoryia; Quattrone, Alessandro; Opocher, Giuseppe; Mantero, Franco; Scaroni, Carla

doi:10.1371/journal.pgen.1003350

Cited by 134 publications

(112 citation statements)

References 43 publications

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“…Following this original description, other patients presenting with a MEN1 phenotype, but no germline mutations in the MEN1 gene, were described (1,4,10). In the evaluated cases, CDKN1B gene mutations generate a decrease in its encoded product, through various mechanisms, encompassing the synthesis of a truncated protein and/or the reduction of either protein expression (4,5,6,8). One of the identified mutations consists of a nucleotide variation at a stop codon associated with the formation of a protein longer than normal, mostly localized in the cytoplasm rather than in the nucleus, with a low stability and a reduced CDK2 binding affinity (1).…”

Section: Discussionmentioning

confidence: 99%

“…PHPT has a high penetrance in MEN4 and, similar to MEN1, is the first diagnosed endocrinopathy in most cases, but with an age at onset more than two decades later than in MEN1 (mean 56 years in MEN4 vs 20-25 years in MEN1) (1,4,5,6,7,8). In about half of the MEN4 patients, only one gland was affected and responsible for PHPT, without genotype/phenotype relationships ever described regarding the severity and the number of the involved parathyroids (1,4,5,6,7,8). The follow-up of these patients is often lacking, and no information on the persistence or recurrence of PHPT is usually referred.…”

Section: Discussionmentioning

confidence: 99%

“…Heterozygote inactivating mutations of the CDKN1B gene have been evidenced in !2% of patients screened for the presence of a MEN1 phenotype not harboring MEN1 gene mutations (1,4,5,6,7,8,9,10), with a total of eight different germline mutations of the CDKN1B gene having been published so far (Table 1). This new syndrome, that in humans presents with an autosomal dominant pattern of inheritance, named MEN4 (4) (OMIM 610755, gene locus 600788 on chromosome 12p13.1), to distinguish it from MEN1, MEN2A (OMIM 171400, gene locus 164761 on chromosome 10q11.21), and MEN2B (formerly MEN3) (OMIM 162300, gene locus 164761 on chromosome 10q11.21), exhibits MEN1-like clinical manifestations but not MEN2-associated tumors in all the reported conditions (Table 1) (1, 4,5,6,7,8,9,10). In this paper, we report a case of a Caucasian female patient with a long clinical history suggestive of a MEN1 syndrome, but with a negative MEN1 genetic test, in which a novel germline heterozygote frameshift mutation of the CDKN1B gene has been identified.…”

Section: Introductionmentioning

confidence: 99%

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A heterozygous frameshift mutation in exon 1 of CDKN1B gene in a patient affected by MEN4 syndrome

Tonelli

Giudici

Giusti

et al. 2014

European Journal of Endocrinology

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Objective: Multiple endocrine neoplasia type 4 (MEN4) is an autosomal dominant disorder that presents with a spectrum of clinical manifestations overlapping with those of MEN1 syndrome. It is caused by inactivating mutations of the CDKN1B gene, encoding for p27 kip1 cyclin-dependent kinase 2 inhibitor, implicated in cell cycle control. Eight mutations of CDKN1B in MEN4 patients have been published so far. The aim of this study was to characterize the molecular basis of a case of MEN1-like syndrome with a neuroendocrine tumor and persistent primary hyperparathyroidism (PHPT). Methods: Clinical, biochemical, and genetic evaluation were undertaken in the proband (a 53-year-old Caucasian woman) and in one 34-year-old son. The proband was operated for recurrent PHPT. Sequence analysis of the MEN1 and CDKN1B genes was performed on constitutional and parathyroid tissue DNA. Staining for p27 was carried out in parathyroid tissue. Results: Neither MEN1 mutations nor large deletions encompassing the MEN1 gene on chromosome 11q13.1 could be detected in the proband. A germline frameshift mutation of CDKN1B (371delCT) was revealed, predicted to generate a truncated p27 (CDKN1B) protein. This mutation was confirmed on somatic DNA from the pathological parathyroid tissue, with the retention of the WT allele. Conclusions:We report a germline heterozygote frameshift mutation of the CDKN1B gene in a Caucasian woman with a long clinical history of MEN1-like multiple endocrine tumors, along with the finding of the mutation in her son. This is the first report of positive CDKN1B mutation analysis in a male subject and also the first description of recurrent hyperparathyroidism in MEN4.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A heterozygous frameshift mutation in exon 1 of CDKN1B gene in a patient affected by MEN4 syndrome

Tonelli

Giudici

Giusti

et al. 2014

European Journal of Endocrinology

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“…A pathogenic truncating mutation in the human orthologue CDKN1B was identified in a 48-year-old woman with a personal history of acromegaly and primary hyperparathyroidism and a family history of renal Printed in Great Britain angiomyolipoma in a confirmed mutation carrier (Pellegata et al 2006). Subsequently, a number of cases of both functional (Georgitsi et al 2007, Agarwal et al 2009, Tichomirowa et al 2012, Occhi et al 2013, Sambugaro et al 2015 and non-functional (Molatore et al 2010) PAs have been reported in patients with germline mutations in CDKN1B, although they account for only a minority of MEN1 mutation negative patients (Ozawa et al 2007, Igreja et al 2009). Mutations in other cyclin-dependent kinase inhibitors have also been linked to MEN.…”

Section: Men4mentioning

confidence: 99%

15 YEARS OF PARAGANGLIOMA: The association of pituitary adenomas and phaeochromocytomas or paragangliomas

O'Toole¹,

Dénes²,

Robledo³

et al. 2015

Endocrine-Related Cancer

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The combination of pituitary adenomas (PA) and phaeochromocytomas (phaeo) or paragangliomas (PGL) is a rare event. Although these endocrine tumours may occur together by coincidence, there is mounting evidence that, in at least some cases, classical phaeo/PGL-predisposing genes may also play a role in pituitary tumorigenesis. A new condition that we termed '3Pas' for the association of PA with phaeo and/or PGL was recently described in patients with succinate dehydrogenase mutations and PAs. It should also be noted that the classical tumour suppressor gene, MEN1 that is the archetype of the PA-predisposing genes, is also rarely associated with phaeos in both mice and humans with MEN1 defects. In this report, we review the data leading to the discovery of 3PAs, other associations linking PAs with phaeos and/or PGLs, and the corresponding clinical and molecular genetics.

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“…The defect led to a reduction in CDKN1B mRNA levels, altered secondary mRNA structure, and reduced transcriptional activity of the gene in laboratory studies [14]. The report by Sambugaro and Di Ruvo et al follows the identification of another 4-bp deletion (c.-456_-453delCCTT) in a highly conserved regulatory region of the 5 0 UTR of the CDKN1B gene in a patient with a pituitary adenoma and a well-differentiated pancreatic neoplasm [15].…”

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confidence: 97%

A giant? Think of genetics: growth hormone-producing adenomas in the young are almost always the result of genetic defects

Stratakis

2015

Endocrine

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A Novel Mutation in the Upstream Open Reading Frame of the CDKN1B Gene Causes a MEN4 Phenotype

Cited by 134 publications

References 43 publications

A heterozygous frameshift mutation in exon 1 of CDKN1B gene in a patient affected by MEN4 syndrome

A heterozygous frameshift mutation in exon 1 of CDKN1B gene in a patient affected by MEN4 syndrome

15 YEARS OF PARAGANGLIOMA: The association of pituitary adenomas and phaeochromocytomas or paragangliomas

A giant? Think of genetics: growth hormone-producing adenomas in the young are almost always the result of genetic defects

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