Germline and somatic mutation of the gene for multiple endocrine neoplasia type 1 (MEN1).

Stephen J Marx ,Shodimu-Emmanuel Olufemi ,Richard Alexander ,Y S Kim ,Francis S Collins ,Christina Heppner ,Irina A Lubensky ,M R Emmert-Buck ,Siradanahalli C Guru ,Sunita Agarwal ,Larisa V Debelenko ,Lance A Liotta ,Monica C Skarulis ,Allen M Spiegel ,Mary Beth Kester ,John L Doppman ,Settara C Chandrasekharappa ,Zhengping Zhuang ,Pachiappan Manickam ,A Lee Burns

doi:10.1046/j.1365-2796.1998.00348.x

Stephen J Marx , Shodimu-Emmanuel Olufemi + Show 18 more

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https://doi.org/10.1046/j.1365-2796.1998.00348.x

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Abstract

Dideoxyfingerprinting was used to screen for germline and somatic MEN1 mutations. This method, applied to a panel of germline DNA from 15 probands with multiple endocrine neoplasia type 1 (MEN-1), allowed confident discovery of the MEN1 gene. Germline MEN1 mutation has been found in 47 out of 50 probands with familial MEN-1, in 7 out of 8 cases with sporadic MEN-1, and in 1 out of 3 cases with atypical sporadic MEN-1. Germline MEN1 mutation was not found in any of five probands with familial hyperparathyroidism. Somatic MEN1 mutations were found in 7 out of 33 parathyroid tumours not associated with MEN-1. Allowing for repeating mutations, a total of 47 different germline or somatic MEN1 mutations have been identified. Most predict inactivation of the encoded 'menin' protein. supporting expectations that MEN1 is a tumour suppressor gene. The 16 observed missense mutations were distributed across the gene, suggesting that many domains are important to its as yet unknown functions.

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