Fine mapping of the MLK-3 gene within 11q13 and its exclusion as the MEN1 susceptibility gene |
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| Authors: | N J Lassam Zheng Lin Michael G Shennan Anouk Courseaux Bin T Teh Patrick Gaudray Catharina Larsson |
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| Institution: | (1) Division of Clinical Oncology Toronto-Sunnybrook Regional Cancer Centre, 2075 Bayview Avenue, Toronto, Ontario, Canada, M4N 3M5 Tel. +1-416-978-1527; Fax +1-416-978-8765; e-mail: norman.lassam@utoronto.ca, CA;(2) Department of Molecular Medicine, Karolinska Hospital, S-171 76 Stockholm, Sweden, SE;(3) LGMCH, CNRS URA 1462, Avenue de Valombrose, F-06107 Nice, France, FR |
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| Abstract: | MLK-3 kinase is a widely expressed serine/ threonine kinase that bears multiple protein interaction domains and regulates
signals mediated by the stress-responsive pathway. Thus, MLK-3 signaling affects numerous cellular processes, raising the
possibility that MLK-3 might play a role in oncogenesis. In this report, we describe the fine mapping of the MLK-3 gene within the 11q13.1 chromosomal region. By integrating data from somatic cell hybrids and double color fluorescence in
situ hybridization on metaphase chromosomes and DNA fibers, MLK-3 has been assigned approximately 1 Mb telomeric of PYGM, close to the D11S546 locus. Since the MEN1 susceptibility locus is also located within the 11q13.1 region, we have carried
out Southern and Northern blot analyses, as well as protein truncation assays to establish whether abnormalities in MLK-3 lead to the development of this familial cancer syndrome. Our observations exclude MLK-3 as the MEN1 gene.
Received: 25 September 1996 / Revised: 16 December 1996 |
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