Korean J Pathol.
2000 Dec;34(12):961-971.
Molecular Cloning of Novel Genes Related to the Craniofacial Development of Human Embryo
- Affiliations
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- 1Department of Oral Pathology, Kangnung National University College of Dentistry, Kangnung 210-702, Korea.
- 2Department of Oral Pathology, Wonkwang University College of Dentistry.
- 3Department of Pathology, Seoul National University College of Medicine.
Abstract
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In order to obtain novel genes for craniofacial development of human, molecular
cloning and sequencing were performed and followed by in situ hybridization in tissue
sections. Subtracted cDNA library of craniofacial tissue from 8 weeks old human
embryo was made by the subtraction with cDNA of RHEK cells. A total of 231 clones
were obtained and their partial sequence data disclosed that 214 clones were
nonredundant in Genebank search. We have done in situ hybridization screening on the
craniofacial sections of a 10 weeks old human fetus, and found significant positive
reaction in 30 clones. Depending on the cell type of similar developmental origin, the
positive reactions could be divided into four groups: first group showed an intense
positive reaction in neural tube, ganglion, and a part of peripheral nerve tissue, second
group relatively diffuse positive reaction in neural tube, cartilage, epithelium, and muscle,
third group localized positive reaction in nerve, and muscle, and fourth group positive
reaction in almost all kinds of cells of craniofacial tissues. Although every clone showed
different expression patterns in the craniofacial development, some of them showed
intense mRNA expressions in the characteristic cell type. Because this study also aimed
to test a screening methods to find out novel genes related to craniofacial development
by the subtracted cDNA library and in situ hybridization, the intense positive reaction of
a certain clone by in situ hybridization may indicate its role in the developmental
processes. We presumed that 30 clones selected in this study are possibly important
new genes for the development of human craniofacial structure.