Different somatic alterations of the HRPT2 gene in a patient with recurrent sporadic primary hyperparathyroidism carrying an HRPT2 germline mutation

Cetani, Filomena; Pardi, Elena; Ambrogini, Elena; Viacava, Paolo; Borsari, Simona; Lemmi, M; Cianferotti, Luisella; Miccoli, Paolo; Pinchera, Aldo; Arnold, Andrew; Marcocci, Claudio

doi:10.1677/erc-06-0092

Cited by 38 publications

(21 citation statements)

References 26 publications

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“…Germline mutations have also been identified in sporadic parathyroid carcinomas [Cetani et al, 2004;Shattuck et al, 2003], suggesting that patients with apparent sporadic parathyroid carcinoma, and their relatives should be assessed for HPT-JT-associated tumors and offered mutational analysis. The observation of combined somatic and germline mutations in a subset of sporadic parathyroid carcinomas as well as HPT-JT-associated parathyroid tumors provides evidence for biallelic CDC73 inactivation that is consistent with Knudson's ''two-hit'' model of inherited cancer and a tumor suppressor role for CDC73 and its encoded protein, parafibromin Cetani et al, 2007b;Howell et al, 2003;Knudson, 1971;Moon et al, 2005;Shattuck et al, 2003]. Such a tumor suppressor role is further supported by the reports of a LOH involving the CDC73 locus in $50% of HPT-JT-associated tumors [Carpten et al, 2002;Teh et al, 1996Teh et al, , 1998]; and a loss of parafibromin immunoreactivity in 13 out of 17 parathyroid tumors from HPT-JT kindreds with CDC73 mutations, and in 65-95% of sporadic parathyroid carcinomas [Cetani et al, 2007a;Gill et al, 2006;Juhlin et al, 2006Juhlin et al, , 2007.…”

Section: Cdc73 Mutations In Nonfamilial Tumorssupporting

confidence: 67%

Cell division cycle protein 73 homolog (CDC73) mutations in the hyperparathyroidism-jaw tumor syndrome (HPT-JT) and parathyroid tumors

et al. 2010

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ABSTRACT:The hyperparathyroidism-jaw tumor (HPT-JT) syndrome is an autosomal dominant disorder characterized by the occurrence of parathyroid tumors in association with ossifying fibromas of the maxilla and/or mandible. The gene responsible for HPT-JT, known as CDC73, was identified in 2002 and encodes a 531 amino acid protein known as parafibromin. Parafibromin is predominantly a nuclear protein that interacts directly with b-catenin and also forms part of the RNA polymerase associated factor-1 complex (Paf1C) that regulates transcription. Heterozygous germline CDC73 mutations are detected in the majority of patients with HPT-JT, and the demonstration of loss of heterozygosity (LOH) at the CDC73 locus in tumors from affected individuals is consistent with a tumor suppressor role. Somatic CDC73 mutations are a frequent finding in nonfamilial (i.e., sporadic) parathyroid carcinomas and have also been reported in benign sporadic parathyroid tumors as well as sporadic renal and fibro-osseous jaw tumors. To date, 111 independent CDC73 mutations have been identified (68 germline; 38 somatic; 5 undefined), and these occur throughout the coding region and splice sites of the CDC73 gene, with the majority (480%) predicting premature truncation of the parafibromin protein. These CDC73 mutations, together with their clinical and biological relevance, are reviewed.

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Section: Cdc73 Mutations In Nonfamilial Tumorssupporting

confidence: 67%

Cell division cycle protein 73 homolog (CDC73) mutations in the hyperparathyroidism-jaw tumor syndrome (HPT-JT) and parathyroid tumors

et al. 2010

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“…Loss of heterozygosity at the HRPT2 locus and 'second-hit' mutations in the coding region of HRPT2 have been reported and are consistent with Knudson's 'two-hit' hypothesis for inactivation of tumor suppressor genes (Howell et al 2003, Bradley et al 2006, Kelly et al 2006, Cetani et al 2007). However, allelic loss at the HRPT2 locus is not always observed in parathyroid tumors with either a known or suspected HRPT2 mutation (Carpten et al 2002, Howell et al 2003, Shattuck et al 2003.…”

Section: Introductionsupporting

confidence: 62%

CDC73/HRPT2 CpG island hypermethylation and mutation of 5′-untranslated sequence are uncommon mechanisms of silencing parafibromin in parathyroid tumors

Hahn¹,

Howell²,

Gill³

et al. 2010

Endocrine-Related Cancer

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The tumor suppressor HRPT2/CDC73 is mutated in constitutive DNA from patients with the familial disorder hyperparathyroidism-jaw tumor syndrome and in w70% of all parathyroid carcinomas. In a number of HRPT2 mutant tumors however, expression of the encoded protein parafibromin is lost in the absence of a clear second event such as HRPT2 allelic loss or the presence of a second mutation in this tumor suppressor gene. We sought to determine whether hypermethylation of a 713 bp CpG island extending 648 nucleotides upstream of the HRPT2 translational start site and 65 nucleotides into exon 1 might be a mechanism contributing to the loss of expression of parafibromin in parathyroid tumors. Furthermore, we asked whether mutations might be present in the 5 0 -untranslated region (5 0 -UTR) of HRPT2. We investigated a pool of tissue from 3 normal parathyroid glands, as well as 15 individual parathyroid tumor samples including 6 tumors with known HRPT2 mutations, for hypermethylation of the HRPT2 CpG island. Methylation was not identified in any specimens despite complete loss of parafibromin expression in two parathyroid carcinomas with a single detectable HRPT2 mutation and retention of the wild-type HRPT2 allele. Furthermore, no mutations of a likely pathogenic nature were identified in the 5 0 -UTR of HRPT2. These data strongly suggest that alternative mechanisms such as mutation in HRPT2 intronic regions, additional epigenetic regulation such as histone modifications, or other regulatory inactivation mechanisms such as targeting by microRNAs may play a role in the loss of parafibromin expression.

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“…2). This nonsense mutation, which is predicted to cause a premature termination of translation in codon 54, has been previously reported in three sporadic parathyroid tumors (two carcinomas and one adenoma) [7,8,31].…”

Section: Dna Sequencing and Restriction Enzyme Analysis Of The Hrpt2 mentioning

confidence: 54%

Identification of De Novo Germline Mutations in the HRPT2 Gene in Two Apparently Sporadic Cases with Challenging Parathyroid Tumor Diagnoses

Cavaco

Santos²,

Félix

et al. 2011

Endocr Pathol

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The diagnosis of parathyroid carcinomas is often difficult. HRPT2 mutations have been identified in familial [hyperparathyroidism-jaw tumor (HPT-JT) syndrome] and sporadic parathyroid carcinomas, supporting that HRPT2 mutations may confer a malignant potential to parathyroid tumors. In this study, we report the clinical, histopathological, and genetic investigation of two unrelated cases, whom had apparently sporadic malignant parathyroid tumors, initially diagnosed as adenomas. In one case, the differential diagnosis was complicated by cervical seeding of parathyroid tumor cells. Genetic studies identified de novo HRPT2 germline mutations in cases 1 (c.518_521delTGTC

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Different somatic alterations of the HRPT2 gene in a patient with recurrent sporadic primary hyperparathyroidism carrying an HRPT2 germline mutation

Cited by 38 publications

References 26 publications

Cell division cycle protein 73 homolog (CDC73) mutations in the hyperparathyroidism-jaw tumor syndrome (HPT-JT) and parathyroid tumors

Cell division cycle protein 73 homolog (CDC73) mutations in the hyperparathyroidism-jaw tumor syndrome (HPT-JT) and parathyroid tumors

CDC73/HRPT2 CpG island hypermethylation and mutation of 5′-untranslated sequence are uncommon mechanisms of silencing parafibromin in parathyroid tumors

Identification of De Novo Germline Mutations in the HRPT2 Gene in Two Apparently Sporadic Cases with Challenging Parathyroid Tumor Diagnoses

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