Close Linkage with the RET Proto-oncogene and Boundaries of Deletion
Mutations in Autosomal Dominant Hirschsprung Disease
Y. Luo , I. Ceccherini , B. Pasini , I. Matera , M.P. Bicocchi,
V. Barone, R. Bocciardi, H. Kaariainen , D. Weber, M. Devoto,
G. Romeo
Human Molecular Genetics , 2(11), 1803--1808 (1993 Nov)
Abstract
Tight linkage with the RET proto-oncogene (Zmax = 3.41 at theta =
0.00), analysis of recombinants and detection of a familial
microdeletion in a large pedigree restrict the mapping of the
Hirschsprung (HSCR) gene previously localized on proximal 10q. The
molecular characterization of the familial microdeletion and of 3
additional cytogenetically visible de novo deletions, isolated in
somatic cell hybrids, identify a smallest region of overlap of 250
Kb. This contains the RET proto-oncogene where missense mutations
causing multiple endocrine neoplasia type 2A (MEN 2A) phenotype were
recently found. The pentagastrin test (which detects preclinical
forms of MEN 2A or B) is negative in adult HSCR patients with
deletions of the RET gene. This represents a good candidate for the
search of mutations causing HSCR.
