11q13 allelotype analysis in 27 northern American MEN1 kindreds identifies two distinct founder chromosomes

M R Emmert-Buck; L V Debelenko; S Agarwal; M B Kester; P Manickam; Z Zhuang; S C Guru; S E Olufemi; A L Burns; S C Chandrasekharappa; I A Lubensky; L A Liotta; M C Skarulis; A M Spiegel; S J Marx; F S Collins

doi:10.1006/mgme.1997.2649

11q13 allelotype analysis in 27 northern American MEN1 kindreds identifies two distinct founder chromosomes

Mol Genet Metab. 1998 Feb;63(2):151-5. doi: 10.1006/mgme.1997.2649.

Authors

M R Emmert-Buck¹, L V Debelenko, S Agarwal, M B Kester, P Manickam, Z Zhuang, S C Guru, S E Olufemi, A L Burns, S C Chandrasekharappa, I A Lubensky, L A Liotta, M C Skarulis, A M Spiegel, S J Marx, F S Collins

Affiliation

¹ Laboratory of Pathology, National Cancer Institute, Bethesda, Maryland 20892, USA.

PMID: 9562970
DOI: 10.1006/mgme.1997.2649

Abstract

We analyzed constitutional and tumor DNA from 27 MEN1 kindreds not known to be related to each other. Disease allele haplotypes were constructed for each pedigree based on shared alleles from two or more affected members and from determination of allelic loss patterns in their tumors. Analysis of disease allele haplotypes showed unexpected linkage disequilibrium at marker PYGM. Further haplotype analysis indicated this could be explained by the presence of two founder chromosomes, one in four families, the other in three. A shared disease haplotype was not observed among two MEN1 kindreds with the prolactinoma phenotype of MEN1.

MeSH terms

Alleles*
Chromosomes, Human, Pair 11 / genetics*
Founder Effect*
Genetic Markers
Haplotypes
Humans
Multiple Endocrine Neoplasia Type 1 / genetics*
North America
Pedigree
Polymerase Chain Reaction
Polymorphism, Genetic

Substances

Genetic Markers