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c-Met Expression in Colorectal Carcinoma and Adenomas: Correlation with Clinicopathologic Parameters
±èÁø, ±èÁ¤À±, ÀÌ¿øÁø, Á¶¼ºÁø, ¹Îº´¿í, ¾öÁØ¿ø, Á¶¹Î¿µ, ¼¼º¿Á, ¹®È«¿µ, ȲÁ¤¿õ,
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±èÁø ( Kim Jin )
°í·Á´ëÇб³ ÀÇ°ú´ëÇÐ ¿Ü°úÇб³½Ç
±èÁ¤À± ( Kim Chung-Yun )
°í·Á´ëÇб³ ÀÇ°ú´ëÇÐ ¿Ü°úÇб³½Ç
ÀÌ¿øÁø ( Lee Won-Jin )
°í·Á´ëÇб³ ÀÇ°ú´ëÇÐ ¿Ü°úÇб³½Ç
Á¶¼ºÁø ( Cho Seong-Jin )
ÇѸ²´ëÇб³ ÀÇ°ú´ëÇÐ Çغκ´¸®Çб³½Ç
¹Îº´¿í ( Min Byung-Wook )
°í·Á´ëÇб³ ÀÇ°ú´ëÇÐ ¿Ü°úÇб³½Ç
¾öÁØ¿ø ( Um Jun-Won )
°í·Á´ëÇб³ ÀÇ°ú´ëÇÐ ¿Ü°úÇб³½Ç
Á¶¹Î¿µ ( Cho Min-Young )
°í·Á´ëÇб³ ÀÇ°ú´ëÇÐ ¿Ü°úÇб³½Ç
¼¼º¿Á ( Seo Seong-Ok )
°í·Á´ëÇб³ ÀÇ°ú´ëÇÐ ¿Ü°úÇб³½Ç
¹®È«¿µ ( Moon Hong-Young )
°í·Á´ëÇб³ ÀÇ°ú´ëÇÐ ¿Ü°úÇб³½Ç
ȲÁ¤¿õ ( Whang Jeong-Woong )
°í·Á´ëÇб³ ÀÇ°ú´ëÇÐ ¿Ü°úÇб³½Ç
KMID : 0356720040200040205
Abstract
Purpose: Hepatocyte growth factor (HGF) stimulates proliferation, migration, and morphogenesis of epithelial cells by specifically binding to its receptor c-met. Abnomalities of the c-met oncogene have been studied in cancers of many organs including thyroid, lung, pancreas, and stomach. However, little is known about the clinical significance of c-met oncogene abnormalities in colorectal carcinomas. In this study, we investigated over- expression of the c-met protein in colorectal adenomas and adenocarcinomas, and analyzed the clinicopathologic significance of this over-expression.
Methods: Expression of the c-met protein localized in colorectal adenoma and adenocarcinoma tissues was analyzed by using immunohistochemistry. The results were compared with clinicopathologic parameters to find clinical correlation.
Results: c-met protein was detected in 42.5% (17/40) of colorectal cancers and in 10.0% (4/40) of colorectal adenomas (P= 0.001). In colorectal cancer, the proportion of expression of c-met protein was 0% (0/40) in stage I, 47.6% (10/40) in stage II, 53.8% (7/40) in stage III and, 0% (0/40) in stage IV. c-met protein expression was 18.8% (3/40) in tumors with invasion into the muscularis propria (MP), and 58.3% (14/40) in tumors with invasion beyond the MP. The depth of tumor invasion was a statistically significant factor (P=0.022) for c-met expression.
Conclusions: The c-met protein expression was related to the depth of invasion of colorectal cancer and showed a significant difference in its rate of expression between adenoma and adenocarcinomas. J Korean Soc Coloproctol 2004;20:205-210
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Proto-oncogene protein c-met;Colorectal neoplasms;Adenoma
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