Multiple endocrine neoplasia type 2A in two families with the familial medullary thyroid carcinoma associated G533C mutation of the RET proto-oncogene

Peppa, Μelpomeni; Boutati, Eleni; Kamakari, Smaragda; Pikounis, Vasilios; Peros, George; Panayiotides, Ioannis G.; Economopoulos, Theofanis; Raptis, Sotirios A.; Hadjidakis, Dimitrios

doi:10.1530/eje-08-0476

Cited by 39 publications

(35 citation statements)

References 23 publications

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“…Codon 533 is located in exon 8 of the RET proto-oncogene, a region that is not routinely sequenced in most commercial laboratories in the United States offering RET analysis; therefore, patients with this mutation could easily be missed, which might account for its apparent rarity. Even though the majority of the 71 codon 533 patients came from a single large Brazilian family or from one of 5 different families of Greek ancestry (10,16,33,47), our data argue in favor of routinely sequencing exon 8, given that it is now a well-characterized and clearly deleterious mutation.…”

Section: Figmentioning

confidence: 80%

Prevalence by Age and Predictors of Medullary Thyroid Cancer in Patients with Lower Risk GermlineRETProto-Oncogene Mutations

Rich

Feng

Busaidy

et al. 2014

Thyroid

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Background: Age-related risk of medullary thyroid carcinoma (MTC) development in presymptomatic carriers of lower risk germline RET mutations is uncertain; such data may aid counseling patients regarding timing of thyroidectomy. Methods: From an institutional database and an exhaustive literature review, we identified 679 patients with American Thyroid Association (ATA) level A or B mutations who were identified because of family screening (index cases of MTC were excluded to minimize selection bias). We evaluated age at thyroidectomy or last evaluation if no thyroidectomy, preoperative calcitonin level (elevated or not), the mutated codon, and outcome (MTC vs. no MTC after thyroidectomy or no clinical evidence of MTC if thyroid intact). Data were used to estimate the cumulative prevalence of MTC and/or assess likelihood of MTC stratified by codon. After exclusion of cases with missing data or small representation, 503 patients with mutations in codons 533, 609, 611, 618, 620, 791, and 804 were analyzed. Results: 236 patients had MTC. Cumulative prevalence and median time to MTC varied by codon and within ATA risk levels ( p < 0.0001). Patients with a codon 620 mutation were 2.8-6.9 times more likely to have MTC than other level B mutation carriers, and 5.1-21.7 times more likely than level A mutation carriers included in our focus population. The youngest median time to MTC was 19 years for codon 620 and the oldest was 56 years for codon 611. Cumulative prevalence of MTC by age 20 was 10% or lower for codons 533, 609, 611, 791, and 804. By age 50, it ranged from 18% for codon 791 to 95% for codon 620. An elevated preoperative calcitonin level strongly predicted MTC on final pathology, though false-negative rates varied by codon ( p < 0.0001). Positive predictive values ranged from 76% to 100% by codon with an overall positive predictive value of 87% across codons. Conclusions: This study offers a better understanding of the age-related development of MTC in lower risk RET mutation carriers, provides evidence of further distinctions between lower risk mutations within ATA subgroups, and clarifies the clinical significance of codon 791 mutations. The data support individualized ''codon-based'' management approaches coupled with clinical data such as calcitonin levels.

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Section: Figmentioning

confidence: 80%

Prevalence by Age and Predictors of Medullary Thyroid Cancer in Patients with Lower Risk GermlineRETProto-Oncogene Mutations

Rich

Feng

Busaidy

et al. 2014

Thyroid

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“…FMTC (OMIM*155240) is associated with mutations either in the extracellular or in the intracellular domain of RET, mostly affecting exons 10, 11, 13, 14 and 15 and never involving exon 16. Mutations in exons 5 and 8 have been reported respectively in one Czech family (8) and in five families originating from Brazil (9), Italy (10) and Greece (11)(12)(13). Nevertheless, the genetic analysis of these exons is routinely performed only in few centres, consistent with the very recent ATA guidelines for the management of MTCs (14), which include among the relevant exons of RET to be screened only exons 10 …”

Section: Introductionmentioning

confidence: 79%

“…It is also tempting to speculate that the high in vitro transforming potential found for this variant could be responsible for the aggressive behaviour of MTC with lung metastases found in patient 2. It is worth noting that another non-cysteine variant in RET exon 8 (Gly533Cys) has been described previously, but not functionally characterized, in five Greek families, three with MEN2A (11,13) and two with FMTC (12), and in one large Brazilian multigenerational family with FMTC (9). On the basis of all these data, exon 8 appears to be an underestimated hotspot of RET variants with an oncogenic potential.…”

Section: Discussionmentioning

confidence: 98%

Four novel RET germline variants in exons 8 and 11 display an oncogenic potential in vitro

Muzza¹,

Cordella²,

Bombled³

et al. 2010

European Journal of Endocrinology

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Context: Most germline-activating mutations of the RET proto-oncogene associated with inherited medullary thyroid cancer (MTC) are localized in exons 10, 11 and 13-15. Four novel RET variants, located in the extracellular domain (p.A510V, p.E511K and p.C531R) coded by exon 8 and in the intracellular juxtamembrane region (p.K666N) coded by exon 11, were identified on the leukocyte DNA from apparently sporadic cases. Methods: Plasmids carrying Ret9-wild-type (Ret9-WT), Ret9-C634R and all Ret9 variants were transfected, and the phosphorylation levels of RET and ERK were evaluated by western blot analyses. The transforming potentials were assessed by the focus formation assay. Results: The p.A510V, p.E511K and p.C531R variants were found to generate RET and ERK phosphorylation levels and to have a transforming activity higher than that of Ret9-WT variant, but lower than that of Ret9-C634R variant. Differently, the p.K666N variant, located immediately downstream of the transmembrane domain, and involving a conserved residue, displayed high kinase and transforming activities. Computational analysis predicted non-conservative alterations in the mutant proteins consistent with putative modifications of the receptor conformation. Conclusions: The molecular analyses revealed an oncogenic potential for all the novel germline RET variants. Therefore, the prevalence of exon 8 genomic variations with an oncogenic potential may be higher than previously thought, and the analysis of this exon should be considered after the exclusion of mutations in the classical hotspots. In addition, on the basis of these functional data, it is advisable to extend the genetic screening to all the first-degree relatives of the MTC patients, and to perform a strict follow-up of familial carriers.

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“…Furthermore, the MTC was least aggressive as it was not clinically apparent, while none of the family members died from MTC-related causes. (Peppa 2008) Moreover, Kamakari et al, have identified the same G533C mutation in 11 unrelated families with FMTC and 4 with MEN2A, explaining the 'RET-negative' FMTC/MEN2A patients. .…”

Section: Diagnosis Of Medullary Thyroid Carcinomamentioning

confidence: 99%

“…(Schuffenecker 1998, Karga 1998 In addition, the same mutations are associated with significantly earlier progression from C-cell hyperplasia to MTC and earlier lymph node involvement than patients with most other mutations related to MEN2A and FMTC. (Peppa 2008, Hofstra 1994 According to the International RET Exon 10 Consortium, codon-associated penetrance by age 50, ranged from 60% (codon 611) to 86% (620) while more advanced stage and increasing risk of metastases correlated with mutation in codon position (609→620) near the juxtamembrane domain. 50%) family members.…”

Section: Diagnosis Of Medullary Thyroid Carcinomamentioning

confidence: 99%

Medullary Thyroid Carcinoma Associated with RET Mutations Located in Exon 8

Peppa¹,

Raptis²

2011

Contemporary Aspects of Endocrinology

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Multiple endocrine neoplasia type 2A in two families with the familial medullary thyroid carcinoma associated G533C mutation of the RET proto-oncogene

Cited by 39 publications

References 23 publications

Prevalence by Age and Predictors of Medullary Thyroid Cancer in Patients with Lower Risk GermlineRETProto-Oncogene Mutations

Prevalence by Age and Predictors of Medullary Thyroid Cancer in Patients with Lower Risk GermlineRETProto-Oncogene Mutations

Four novel RET germline variants in exons 8 and 11 display an oncogenic potential in vitro

Medullary Thyroid Carcinoma Associated with RET Mutations Located in Exon 8

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