MouseÀÇ Ä¡¾Æ ¹ßÀ°½Ã Runx2ÀÇ ¹ßÇö ¾ç»ó
EXPRESSION PATTERN OF RUNX2 IN MURINE TOOTH DEVELOPMENT
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±èÅÂ¿Ï ( Kim Tae-Wan ) - °æºÏ´ëÇб³ Ä¡°ú´ëÇÐ ¼Ò¾ÆÄ¡°úÇб³½Ç
·ùÇö¸ð ( Ryoo Hyun-Mo ) - °æºÏ´ëÇб³ ÀÇ°ú´ëÇÐ »ýÈÇб³½Ç
³²¼øÇö ( Nam Soon-Hyeun ) - °æºÏ´ëÇб³ Ä¡°ú´ëÇÐ ¼Ò¾ÆÄ¡°úÇб³½Ç
±è¿µÁø ( Kim Young-Jin ) - °¸ª´ëÇб³ Ä¡°ú´ëÇÐ ¼Ò¾ÆÄ¡°úÇб³½Ç
±èÇöÁ¤ ( Kim Hyun-Jung ) - °æºÏ´ëÇб³ Ä¡°ú´ëÇÐ ¼Ò¾ÆÄ¡°úÇб³½Ç
KMID : 0358920040310040651
Abstract
Runx2´Â runt gene family¿¡ ¼ÓÇÏ´Â Àü»çÁ¶Àý ÀÎÀÚ·Î½á »ÀÀÇ Çü¼º°ú °ñ¾Æ¼¼Æ÷ÀÇ ºÐÈ¿¡ Áß¿äÇÑ ¿ªÇÒÀ» ´ã´çÇÏ°í ÀÖ´Ù. Runx2-haploinsufficency´Â ¼â°ñÀÇ ÀúÇü¼º ¹× µÎ°³ ºÀÇÕÀÇ Áö¿¬À» Ư¡À¸·Î ÇÏ´Â ¼â°ñµÎ°³ ÀÌÇü¼ºÁõÀ» ÀÏÀ¸Å°¸ç, Ä¡¾Æ¿¡ À־ ¹ý¶ûÁúÀÇ ÀúÇü¼º, ¿µ±¸Ä¡ ¸ÍÃâÁö¿¬ µîÀ» º¸ÀδÙ. ÀÌ¿¡, Ä¡¾ÆÀÇ ¹ßÀ° ¹× ¸ÍÃâ¿¡ ¹ÌÄ¡´Â Runx2ÀÇ ¿µÇâÀ» ¾Ë¾Æº¸±â À§ÇØ in situ hybridization ¹æ¹ýÀ¸·Î Å»ý 1, 4, 7, 14. 21ÀÏ µÈ ÁãÀÇ ÇÏ¾Ç ¹× Á¦1´ë±¸Ä¡¸¦ »ç¿ëÇÏ¿© ½ÇÇèÀ» ½Ç½ÃÇÏ¿´´Ù. Runx2-full length´Â Å»ý 1ÀÏ°ú 4ÀÏ¿¡ Ä¡³¶ ¹× ÁÖÀ§Á¶Á÷¿¡ º¸ÀÌÁö¸¸ Runx2-type¥±´Â º¸ÀÌÁö ¾Ê¾Ò´Ù. Runx2-full length´Â Å»ý 7ÀÏ¿¡ Ä¡°ü ±³ÇÕ¸é ºÎÀ§ÀÇ ¹ý¶û¸ð¼¼Æ÷¿¡ ¹ßÇöÇÏ¿´°í, 1ÁÖÀÏ ÈÄÀÎ Å»ý 14ÀÏ¿¡´Â ¹é¾Ç¹ý¶û°æ°è »ó¹æÀÇ Ä¡°üÀÎ Á¢¸é ¹ý¶û¸ð¼¼Æ÷¿¡¼ ¹ßÇöµÇ¾ú´Ù. ÀÌ¿¡ ¹ÝÇØ Runx2-type¥±´Â ¹ý¶û¸ð¼¼Æ÷¿¡¼ ¹ßÇöÇÏÁö ¾Ê¾Ò´Ù. ¶ÇÇÑ Å»ý 21ÀÏ¿¡¼´Â µÎ°¡Áö À̼ºÁúü°¡ ¸ðµÎ ÇϾǰñ¿¡¼ ¹ßÇöÀ» º¸¿´´Ù. ÀÌ·± °á°ú¸¦ Á¾ÇÕÇغ¼ ¶§, Runx2-full length´Â Ä¡¾ÆÀÇ ¸ÍÃâ°ú ¿¬°üÀÌ ÀÖÀ¸¸ç, ¹ý¶û¸ð¼¼Æ÷ÀÇ ºÐÈ ¹× ÀÌ·Î ÀÎÇÑ ¹ý¶ûÁúÇü¼º¿¡ ¿µÇâÀ» ÁÖÁö¸¸ Runx2-type¥±´Â ÇϾǰñÀÇ Çü¼º¿¡¸¸ ¿µÇâÀ» ¹ÌÄ¡´Â °ÍÀ¸·Î »ç·áµÈ´Ù.
Runx2 is a transcription factor in homologous with Drosophila runt gene and it is essential for bone formation during embryogenesis and a critical gene for osteoblast differentiation and osteoblast function. Runx2-haploinsufficency causes cleidocranial dysplasia (CCD). CCD is an autosomal-dominant inherited disorder characterized by hypoplastic clevicle and delayed ossification in fontanelles and wormian bones. Dental defects are possibly shown to CCD patients : multiple supernumerary teeth, irregular and compressed permanent tooth crowns, hypoplastic and hypomineralized defects in enamel and dentin, an excess of epithelial root remnants, the absence of cellular cementum, and abnormally shaped roots. In addition, delayed eruption of the secondary dentition is a constant finding.
The aim of this study is to evaluate the role of Runx2 in the tooth development and eruption through analyzing the expression pattern of Runx2 by in situ hybridization during crown (late bell stage) and root formation of tooth, using postnatal day 1, 4, 7, 14 and 21 mice mandibular molar teeth. mRNA of Runx2-full length is expressed in dental follicle and surrounding tissue at postnatal day1 and 4. At post-natal day 7, it is expressed in ameloblasts of occlusal surface of enamel and bone area surrounding the tooth. In comparison with previous stage, at postnatal day 14, it is expressed in ameloblasts of proximal surface of enamel. At postnatal day 21 it¡¯s expression is observed only in bone area. mRNA of Runx2-type¥± is not expressed At postnatal day 1 and 7. At postnatal day 14 and 21, it¡¯s expression is observed in the bone area.
In this study, we suggest that Runx2 have a relation of ameloblasts differentiation and an important role to tooth eruption made by dental follicle during intraosseous eruption stage. Also we can confirm that Runx2 has a role to bone formation.
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Ä¡³¶;¼â°ñµÎ°³ ÀÌÇü¼ºÁõ;Ä¡¾Æ¹ßÀ°;Ä¡¾Æ¸ÍÃâ
Runx2;Dental follicle;Cleidocranial Dysplasia;Tooth Development;Tooth Eruption
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