Articolo in rivista, 2004, ENG

Molecular pathology of the MEN1 gene.

Agarwal SK; Lee Burns A; Sukhodolets KE; Kennedy PA; Obungu VH; Hickman AB; Mullendore ME; Whitten I; Skarulis MC; Simonds WF; Mateo C; Crabtree JS; Scacheri PC; Ji Y; Novotny EA; Garrett-Beal L; Ward JM; Libutti SK; Richard Alexander H; Cerrato A; Parisi.

SUNTTA K. AGARWAL? A. LEE BURNS,' KAREN E. SUKHODOLETS: PATRICIA A. KENNEDY? VICTOR H. OBUNGU,' ALISON B. HICKMAN? MICHAEL E. MULLENDORE,' IRA WHITTEN,' MONICA C. SKARULIS? WILLIAM F. SIMONDS,~C ARMEN MATEO,~J UDY s. CRAB TREE,^ PETER c . SCACHERI,~YOUNGMIJ I ,E~L IZABETH A. NOVOTNY,~ LISA GARRETT-BEAL,~JE RROLD M. WARD,^ STEVEN K. LIBUTTI: SONIA SANTA ANNA-A,~B RIAN OLIVER? SETTARA c. CHANDRASEKHARAPPA,~F RANCIS s. COLLINS,~ ALLEN M. SPIEGEL! AND STEPHEN J. MARXU H. RICHARD ALEXANDER,' ANIELLO CERRATO? MICHAEL J. PARISI,' aNational Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland 20892, USA bNational Human Genome Research Institute, National Institutes of Health, Bethesda, Maryland 20892, USA 'National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892, USA dNalional Institute of Deafness and Communication Disorders, National Institutes of Health, Bethesda, Maryland 20892, USA

Multiple endocrine neoplasia type 1 (MEND, among all syndromes, causes tumors in the highest number of tissue types. Most of the tumors are hormone producing (e.g., parathyroid, enteropancreatic endocrine, anterior pituitary) but some are not (e.g., angiofibroma). MEN1 tumors are multiple for organ type, for regions of a discontinuous organ, and for subregions of a continuous organ. Cancer contributes to late mortality; there is no effective prevention or cure for MEN1 cancers. Morbidities are more frequent from benign than malignant tumor, and both are indicators for screening. Onset age is usually earlier in a tumor type of MEN1 than of nonhereditary cases. Broad trends contrast with those in nonneoplastic excess of hormones (e.g., persistent hyperinsulinemic hypoglycemia of infancy). Most germline or somatic mutations in the MEN] gene predict truncation or absence of encoded menin. Similarly, 11q13 loss of heterozygosity in tumors predicts inactivation of the other MEN] copy. MEN] somatic mutation is prevalent in nonhereditary, MEN1-like tumor types. Compiled germline and somatic mutations show almost no genotype/phenotype relation. Normal menin is 67 kDa, widespread, and mainly nuclear. It may partner with junD, NF-kB, PEM, SMAD3, RPA2, FANCD2, NM23beta, nonmuscle myosin heavy chain II-A, GFAP, and/or vimentin. These partners have not clarified menin's pathways in normal or tumor tissues. Animal models have opened approaches to menin pathways. Local overexpression of menin in Drosophila reveals its interaction with the junkinase pathway. The Men1+/- mouse has robust MEN1; its most important difference from human MEN1 is marked hyperplasia of pancreatic islets, a tumor precursor stage.

Annals of the New York Academy of Sciences 1014 , pp. 189–198

Keywords

CNR authors

Cerrato Aniello

CNR institutes

IEOS – Istituto per l'endocrinologia e l'oncologia "Gaetano Salvatore"

ID: 21133

Year: 2004

Type: Articolo in rivista

Creation: 2009-06-16 00:00:00.000

Last update: 2020-09-25 14:45:16.000

External links

OAI-PMH: Dublin Core

OAI-PMH: Mods

OAI-PMH: RDF

External IDs

CNR OAI-PMH: oai:it.cnr:prodotti:21133

ISI Web of Science (WOS): 000221898100020