Length and Loss of Heterozygosity of an Intron 1 Polymorphic Sequence of egfr Is Related to Cytogenetic Alterations and Epithelial Growth Factor Receptor Expression
2000
Overexpression of epithelial growth factor receptor (EGFR) is correlated
with a poor prognosis and reduced steroid receptor expression.
Recently, it was demonstrated that the length of a CA repeat in the
intron 1 of EGFR correlated with the expression of EGFR
in vitro . We investigated 112 cases of cancerous and
noncancerous breast tumor samples for loss of heterozygosity (LOH) in
intron 1 of the egfr gene and determined the
intratumoral EGFR content and genetic alterations by comparative
genomic hybridization. Heterozygous tumors with short CA repeats
showed elevated EGFR expression in contrast to tumors with longer CA
repeats. Tumors with LOH in intron 1 of egfr revealed
higher EGFR expression when the longer allele was lost compared with
loss of the shorter allele. Additionally, tumors with a loss of
the long allele showed more chromosomal alterations, especially a
higher frequency of amplifications. We conclude that the CA repeat
status in intron 1 of the egfr gene also modulates the
intratumoral EGFR content in vivo . Furthermore, LOH at
the CA repeat is associated with genetically advanced tumors.
Therefore, allele-specific gene expression due to LOH of the CA repeat
could be assumed to be an important event in invasive breast cancer
development.
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