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Abstract
The process of embryo attachment and implantation is
accompanied by dramatic cellular and functional changes in
the endometrium whose control and mechanisms are not
clearly understood. cDNA cloning of differentially
expressed genes, specifically at implantation sites in the
rabbit endometrium, was used to identify genes controlling
functional and remodeling changes. Tissue from the
endometrium of day 6
(preimplantation) and day 8
(implantation initiation) pregnant rabbits was used to
screen for differentially expressed genes by combined cDNA
subtraction/suppressive hybridization. Twenty-nine
differentially expressed genes were identified encoding
protein modification enzymes, signaling proteins,
structural proteins, and enzymes. One of these is a novel
member of the E2 ubiquitin-conjugating enzyme family we
have designated UBCi (i for implantation), which displayed
dramatic nucleotide and deduced amino acid sequence
conservation between rabbits, humans, and mice. In situ
hybridization indicated UBCi expression exclusively in the
luminal epithelium of the endometrium while glandular
epithelium, trophoblast, and myometrium were negative.
Expression was specific for epithelial cells at
implantation sites and was not detected in non-implant
site endometrium. UBCi mRNA was detected in both the
mesometrial and antimesometrial epithelial cells of the
implantation sites, sites undergoing both differentiation
and/or apoptosis. These results identify a group of
differentially expressed genes in the endometrium
including UBCi and provide new focal targets for studying
processes controlling cellular remodeling during
implantation. The important roles of ubiquitination in
controlling the activities and turnover of key signaling
proteins suggest potential roles in controlling critical
aspects of implantation.
Key words:
Implantation
Uterus
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