Allen M. Spiegel scite author profile

Multiple endocrine neoplasia-type 1 (MEN1) is an autosomal dominant familial cancer syndrome characterized by tumors in parathyroids, enteropancreatic endocrine tissues, and the anterior pituitary. DNA sequencing from a previously identified minimal interval on chromosome 11q13 identified several candidate genes, one of which contained 12 different frameshift, nonsense, missense, and in-frame deletion mutations in 14 probands from 15 families. The MEN1 gene contains 10 exons and encodes a ubiquitously expressed 2.8-kilobase transcript. The predicted 610-amino acid protein product, termed menin, exhibits no apparent similarities to any previously known proteins. The identification of MEN1 will enable improved understanding of the mechanism of endocrine tumorigenesis and should facilitate early diagnosis.

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Activating Mutations of the Stimulatory G Protein in the McCune–Albright Syndrome

Weinstein

et al. 1991

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Menin Interacts with the AP1 Transcription Factor JunD and Represses JunD-Activated Transcription

Agarwal

Guru

Heppner

et al. 1999

Cell

560

425

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MEN1 is a tumor suppressor gene that encodes a 610 amino acid nuclear protein (menin) of previously unknown function. Using a yeast two-hybrid screen with menin as the bait, we have identified the transcription factor JunD as a direct menin-interacting partner. Menin did not interact directly with other Jun and Fos family members. The menin-JunD interaction was confirmed in vitro and in vivo. Menin repressed transcriptional activation mediated by JunD fused to the Gal4 DNA-binding domain from a Gal4 responsive reporter, or by JunD from an AP1-responsive reporter. Several naturally occurring and clustered MEN1 missense mutations disrupted menin interaction with JunD. These observations suggest that menin's tumor suppressor function involves direct binding to JunD and inhibition of JunD activated transcription.

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Allen M. Spiegel

Positional Cloning of the Gene for Multiple Endocrine Neoplasia-Type 1

Activating Mutations of the Stimulatory G Protein in the McCune–Albright Syndrome

Menin Interacts with the AP1 Transcription Factor JunD and Represses JunD-Activated Transcription

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