Clinical studies of multiple endocrine neoplasia type 1 (MEN1)

Trump, Dorothy; Farren, B; Wooding, C; Pang, J T; Besser, G. M.; Buchanan, K.D.; Edwards, Caitlin; Heath, David A.; Jackson, Charles E.; Jansen, Silvia; Lips, K.; Monson, JP; O’Halloran, Domhnall J; Sampson, Julian R.; Shalet, S; Wheeler, MalcolmH.; Zink, Alexander M.; Thakker, Rajesh

doi:10.1093/qjmed/89.9.653

Cited by 434 publications

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“…Foregut carcinoid tumors (thymic and bronchial), adrenocortical hyperplasia, multiple lipomas, facial angiofibromas, and skin collagenomas may also be seen in the syndrome. [1][2][3][4] Unusual features of MEN1-related tumors include their multiplicity, both within and among target organs, and an earlier age of onset than similar sporadic tumors. 5 Symptoms in MEN1 are caused by an overproduction of specific hormones, neoplasm mass effects, or malignant transformation.…”

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confidence: 99%

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Clinical testing for multiple endocrine neoplasia type 1 in a DNA diagnostic laboratory

Klein

Salih

Bessoni

et al. 2005

Genetics in Medicine

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Purpose: Based on results of diagnostic MEN1 testing, we have attempted to further define the mutational spectrum of the MEN1 gene and the clinical features most frequently associated with MEN1 mutations. Methods:Mutation testing was performed on blood samples by PCR amplification and sequencing of exons 2 to 10 of the MEN1 gene and the corresponding intron-exon junctions. Pedigree phenotypic information was obtained by written questionnaire. Results: Among 288 presumably unrelated pedigrees, 73 independent mutations were found in 89 families. Five mutations were found in 2 pedigrees, and 4 mutations were seen in more than 2 pedigrees. There were 17 nonsense mutations (23.3%), 2 in-frame deletions (2.7%), 18 frameshift-deletion mutations (24.7%), 10 frameshift-insertion or -duplication mutations (13.7%), 13 splice-site mutations (17.8%), and 13 presumptive

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confidence: 99%

“…Clinical disease is uncommon before 10 years of age. 1,3,8 The MEN1 gene, located at chromosome 11q13, is approximately 9.8 kb in length and contains 10 exons. The 1830-bp coding region in exons 2 to 10 generates a 610 amino acid protein of unknown function called "menin."…”

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confidence: 99%

Clinical testing for multiple endocrine neoplasia type 1 in a DNA diagnostic laboratory

Klein

Salih

Bessoni

et al. 2005

Genetics in Medicine

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“…On the other hand, it has recently been reported that a Japanese patient with FHP had a germline mutation of the MEN1 gene (Y353X in exon 8), although the clinical evaluation for MEN1 was not described in this family [13]. Primary hyperparathyroidism is usually expressed at an early age (85% by age 35) and has a high penetrance (95%) in MEN1 [14]. Patients with MEN1 may initially have primary hyperparathyroidism as the only manifestation of their disease and therefore, are difficult to distinguish from patients with primary hyperparathyroidism without MEN1.…”

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confidence: 90%

Germline Mutation of the Multiple Endocrine Neoplasia Type 1(MEN1) Gene in a Family with Primary Hyperparathyroidism.

et al. 1998

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Abstract. Familial primary hyperparathyroidism(FHP) is a rare hereditary disorder characterized by isolated parathyroid tumors without any other lesions related to multiple endocrine neoplasia (MEN). Primary hyperparathyroidism is usually expressed at an early age and is highly penetrated in MEN type 1(MEN1), suggesting that some FHP may be a variant type or early stage of MEN1. The MEN1 gene has recently been cloned and its germline mutations have been considered to play an important role in the tumorigenesis of MEN1. We studied a Japanese family with primary hyperparathyroidism which included 4 patients. To investigate the possible relationship between primary hyperparathyroidism in this family and the MEN1 gene, we analyzed a proband for a germline mutation of the MEN1 gene in this study. We identified a novel heterozygous mutation (1350de13) at codon 414 in exon 9. Restriction digestion analysis revealed the same mutation pattern in his brother with hyperparathyroidism. These findings suggest that our patients may belong to a variant type of MEN1.

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“…Our index patient presented with assumed PHPT, which is typically the first manifestation of MEN1 and occurs in 95% of cases 18, 19. In addition, he had a NET (formerly known as carcinoid), which have been reported to occur in 4% of MEN1 patients 16, 19, 20. In retrospect, the clinical MEN1 diagnosis was not clear‐cut, with several lines of evidence suggesting that our index patient was most likely a so‐called phenocopy, that is, a phenotype resembling MEN1 without being it 21, 22.…”

Section: Discussionmentioning

confidence: 94%

“…In addition, the patient was negative for all mutations known to cause MEN1, although about 5–15% of considered MEN1 cases are genetically unverified 17, 23, 24. Furthermore, only the index patient had affection of more than one organ, and as the penetrance of MEN1 is close to 100% in patients older than 50 years, it is unlikely that the 71‐year‐old father should be unaffected 20, 25. The low CCCR is also not typical for PHPT, but can occur due to low vitamin D. According to Thakker et al, MEN1 phenocopies are seen in up to 10% of cases with the causative mutations found in other genes including CDC73 and CASR .…”

Section: Discussionmentioning

confidence: 99%

Multiple endocrine neoplasia phenocopy revealed as a co‐occurring neuroendocrine tumor and familial hypocalciuric hypercalcemia type 3

Hovden

Jespersen

Nissen

et al. 2016

Clinical Case Reports

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Clinical studies of multiple endocrine neoplasia type 1 (MEN1)

Cited by 434 publications

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Clinical testing for multiple endocrine neoplasia type 1 in a DNA diagnostic laboratory

Clinical testing for multiple endocrine neoplasia type 1 in a DNA diagnostic laboratory

Germline Mutation of the Multiple Endocrine Neoplasia Type 1(MEN1) Gene in a Family with Primary Hyperparathyroidism.

Multiple endocrine neoplasia phenocopy revealed as a co‐occurring neuroendocrine tumor and familial hypocalciuric hypercalcemia type 3

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