Han-Il Lee
Catholic University of Daegu
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International Journal of Colorectal Disease | 2007
Chang-Ho Jeon; Han-Il Lee; Im-Hee Shin; Jong-Wook Park
Background and aimColorectal cancer (CRC) is one of the most rapidly increasing cancers in Korea, but no comprehensive analysis has been performed to speculate the genetic basis of CRC development. We investigated the presence of adenomatous polyposis coli gene (APC), Kirsten-ras (K-ras), p53, microsatellite instability (MSI), and melanoma antigen gene (MAGE) alterations in CRC and correlated the results obtained with clinical data.Materials and methodsWe collected 78 cancer tissues from CRC patients. Genetic analyses were performed on APC, K-ras, p53, and MSI (BAT 25 and BAT 26), and in addition, MAGE expression was tested by reverse transcription polymerase chain reaction. Correlations between genetic markers and clinical factors were analyzed after reviewing medical records.ResultThe positive rates for alterations of APC, K-ras, p53, MSI, and MAGE in 78 tissue samples were 33.3, 29.5, 34.6, 9.0, and 68.4%, respectively. Mutations were frequently detected in codons 1291 and 1450 of APC, in codon 12 of K-ras and in codons 248, 282, and 176 of p53. APC mutations were frequently noted in early-stage cancer, whereas MSI was observed in right-sided and multiple cancers. No associations were found between the presence of alterations in APC, K-ras, p53, MSI, and MAGE.InterpretationIn Koreans, positive rates of alterations in APC and p53 were slightly lower than those of APC and p53 in Caucasians, and the genetic alterations including MAGE expression are involved in 92.1% of CRCs. The lack of multiple mutations and of a relation between mutation rates and clinical stage suggest that genetic alterations might have independent influences on CRC development in Koreans.
Cancer Research and Treatment | 2012
Sangbong Jung; Han-Il Lee; Hoon-Kyu Oh; Im-Hee Shin; Chang-Ho Jeon
Purpose Although the incidence of microsatellite instability (MSI) accounts for 10-15% of cases of colorectal cancer, its clinical application for all colorectal cancers has widened. We attempted to identify clinical and pathological parameters that may be helpful in selection of patients with MSI-high (MSI-H). Materials and Methods A total of 120 resected colorectal cancers were enrolled retrospectively for this MSI study. Polymerase chain reaction (PCR) and denaturing high performance liquid chromatography and/or real time PCR methods with five markers and immunohistochemistry (IHC) for MLH1 and MSH2 were performed for analysis of cancer and blood specimens. Clinico-pathologic parameters, including IHC, were investigated in order to determine their usefulness as predictive factors of MSI. Results Among 120 cases of colorectal cancer, MSI was observed in 15 cases (12.5%), including 11 cases of MSI-H and four cases of MSI-low. Patients with MSI were younger, less than 50 years old, had a family history of cancer, Rt. sided colon cancer and/or synchronous multiple colorectal cancer, mucinous histologic type, and serum carcinoembryonic antigen group in the normal range. Results of multivariate analysis showed Bethesda guidelines, Rt. sided and/or synchronous multiple colorectal cancer, and negative expression of IHC for MLH1, which was consistently associated with MSI-H. MSI-H colorectal tumors have met at least one of these three parameters and their sensitivity and specificity were 100% and 72.5%, respectively. Conclusion Bethesda guidelines, tumor location, and negative expression of MLH1 protein are important parameters for selection of patients with colorectal cancers for MSI testing. MSI testing is recommended for patients showing any of these three parameters.
The Korean journal of internal medicine | 2004
Jin-Hyang Shin; Soyeon Kim; Chang-Min Woo; Young-Sup Kim; Ji-Young Kim; Jung-Hyun Seo; Wan-Suk Lee; Sung-Hwa Bae; Hun-Mo Ryoo; Han-Il Lee; Im-Hee Shin; Min-Kyoung Kim; Kyung-Hee Lee; Myung-Soo Hyun
Journal of The Korean Society of Coloproctology | 2004
Dong-Ryul Lee; Han-Il Lee; Ho-Gak Kim; Eun Young Kim; Hyun-Mo Ryoo; Sang-Mo Yun; Jin-Cheon Kim
Journal of The Korean Society of Coloproctology | 2004
Han-Il Lee; Tae-Soon Lee; Soon-Jai Jung; Kihyuk Park; Dong-Rak Choi; Dae-Hyun Joo; Sung-Hwan Park; Yong-Oon Yoo; Ki-Ho Park; Young-Hwan Lee; Jin-Cheon Kim
Journal of The Korean Society of Coloproctology | 2003
Han-Il Lee; Dong-Rak Choi; Dae-Hyun Joo; Kihyuk Park; Sung-Hwan Park; Yong-Oon Yu; Ki-Ho Park; Im-Hee Shin; Dong-Gun Shin; Jong-Ki Kim; Chang-Ho Cho; Jin-Cheon Kim
Korean journal of gastrointestinal endoscopy | 2002
Joong-Goo Kweon; Eun-Young Kim; Chang-Hyeong Lee; Ho-Gak Kim; Jyung-Dong Bae; Han-Il Lee; Chang-Ho Cho; Hyun-Soo Kim
The Korean journal of internal medicine | 2000
Han-Il Lee; Young-Kil Park; Cho Nk; Young-Jin Yuh; Sung Rok Kim
한국간담췌외과학회지 | 1997
Yang-Il Kim; Dae-Hyun Joo; Yong-Oon Yoo; Han-Il Lee; Sung-Hwan Park; Ki-Ho Park
The Korean journal of internal medicine | 1997
Young-Sook Park; Kwan Jae Lee; Tae-Yeob Kim; Min-Hye Kim; Han-Il Lee; Kim Sy; Hoh Cs; H K Min