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Isolation and mapping of polymorphic cosmid clones used for sublocalization of the multiple endocrine neoplasia type 1 (MEN1) locus
Authors:Catharina Larsson  Günther Weber  Eva Kvanta  Kathy Lewis  Marie Janson  Carol Jones  Tom Glaser  Glen Evans  Magnus Nordenskjöld
Affiliation:(1) Department of Clinical Genetics, Karolinska Hospital, S-10401 Stockholm, Sweden;(2) Molecular Genetics Laboratory, SALK Institute, 92037 La Jolla, CA, USA;(3) Eleanor Roosevelt Institute for Cancer Research, 80206 Denver, CO, USA;(4) Howard Hughes Medical Center, Harvard Medical School, 02115 Boston, MA, USA
Abstract:Summary Multiple endocrine neoplasia type 1 (MEN1) is characterized by neoplasia of the parathyroids, the pancreas, and the pituitary. Tumorigenesis involves unmasking of a recessive mutation at the MEN1 locus, which has been mapped to the centromeric part of chromosomal region 11q. In order to localize the MEN1 gene further and to make its isolation possible, a number of new markers were isolated. Two radiation-reduced somatic cell hybrids were identified that only contained markers close to and flanking the MEN1 region. DNA from these hybrids was used for the construction of a cosmid library, and clones containing human inserts were isolated. In addition, cosmid clones were isolated for locus expansion of 7 other markers that were mapped to the 11q12–13.2 region. The 33 newly isolated clones together with 25 previously published markers from this region were analyzed in a panel of radiation-reduced somatic cell hybrids. From the hybridization pattern, the region was divided into 11 parts. New restriction fragment length polymorphisms were identified in 7 of the newly isolated cosmid clones and in one plasmid. These were then used to sublocalize meiotic cross-overs more precisely in two MEN1 families, thus refining the mapping of the disease gene.
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