• Toxicological Research
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• 제7권1호
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• pp.1-12
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• 1991

The phenotyping of cytochrome P-450 in hepatic mivrosomes induced by phenytoin in the rats was carried out by using several monoclonal antibodies (MAbs) against specific P-450 isozymes. Phenytoin (180 mg/kg) was administered intrapritoneally for three consecutive days to the male Sprague-Dawley rats(100-120g). Solid phase radio-immunoassay showed higher binding affinity of MAb PB 2-66-3 and PCN 2-13-1 to the microsomes from phenytoin treated rats than those to from untreated rats, which was comparable to the level in phenobarbital induced rat hepatic microsomes.

• Asian Pacific Journal of Cancer Prevention
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• 제14권5호
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• pp.2699-2701
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• 2013

The RAS family genes encode small GTP-binding cytoplasmic proteins. Activated KRAS engages multiple effector pathways, notably the RAF-mitogen-activated protein kinase, phosphoinositide-3-kinase (PI3K) and RalGDS pathways. In the clinical field, K-ras oncogene activation is frequently found in human cancers and thus may serve as a potential diagnostic marker for cancer cells in circulation. This mini-review aims to summarise information on Ras-induced oncogenesis and the clinical significance of K-ras.

• 한국환경성돌연변이발암원학회지
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• 제24권2호
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• pp.85-90
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• 2004

Nickel(II) compounds are carcinogenic metals which induce genotoxicity and oxidative stress through the generation of reactive oxygen species. In search of new molecular pathways toward understanding the molecular mechanism of nickel(II)-induced carcinogensis, we performed mRNA differential display analysis using total RNA extracted from nickel(II) acetate-treated normal rat kidney cells (NRK-52E). Cells were exposed for 3 days to 160 and 240 uM nickel(II) concentrations. cDNAs corresponding to mRNAs for which expression levels were altered by nickel(II) were isolated, sequenced, and followed by a GenBank Blast homology search. Specificity of differential expression of cDNAs was determined by RT-PCR and Western blot analysis. Two of them (SH3BGRL3 and FHIT) were down-regulated and one (metallothionein) was up-regulated by nickel(II) treatment. The expression of these mRNAs were nickel(II) concentration-dependent. The levels of FHIT and metallothionein proteins were also consistent with the results for mRNAs. Overall, although the fundamental questions related to function of these genes in nickel(II)-mediated carcinogenicity are not answered, our study suggests that they can be interesting candidates for studies of molecular mechanisms of nickel(II) carcinogenesis.

• Journal of Nutrition and Health
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• 제25권2호
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• pp.116-122
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• 1992

This study determined hepatic microsomal lipid peroxide values glucose 6-phosphatase NA-DPH-cytochrome P450 reductase and cytosolic glutathione S-transferase activites to examine the effects of methyl group deficiency on hepatic lipid peroxidation in rats treated with diethylni-trosamine(DEN) and 2-acetylamionfluorene(AAF) Weanling sprague Dawley male rats were fed the diet with methyl group supplemented or deficient. Two weeks after feeding rate were injected with a single of 200mg/kg body weight DEN intraperitoneally and after four weeks 0.02% AAF containing diets were fed for two weeks. Animals were sacrificed at 6th week. Microsomal lipid peroxide values were tended to increase in methyl group deficiency(MD). Especially in case of carcinogen tratments lipid peroxide values were increased significantly in MD. Microsomal glucose 6-phophatase activities were decreased by MD and carcinogens and in MD with carcinogen group (MD+C) the enzyme activites were the lowest Glucose 6-phosphatase activities were negatively correlated with lipid peroxidation. Microsomal NADPH-cytochrome P450 reductase activities were the highest in MD+C and correlated positively with lipid peroxidation. Cytosolic glutathione S-transferase activities were the highest in MD+C Methyl group deficiency induces lipid peroxidation especially in case of being exposed to carcinogens. Therefore the results suggest that lipid peroxidation may be one of the meachanisms of carcinogensis by methyl group deficiency.

• Toxicological Research
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• 제17권
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• pp.293-297
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• 2001

The international pharmaceutical and regulatory communities had been recognizing the limited utility of conventional rodent carcinogenicity study particularly on the second species, mouse, after intense investigation of carcinogenicity data base worldwide, and a new scheme for carcinogenicity testing for pharmaceuticals was proposed at the Expert Working Group on Safety in the International Conference on Harmonization (ICH) in 1996. CB6F 1-Tg rasH2 mouse carrying human prototype c-Ha-ras gene with its own promoter/enhancer is one oj the new carcinogenicity assay model for human cancer risk assessment. Studies have been conducted since 1992 to validate the transgenic (Tg) mice for rapid carcinogenicity test-ing, short term (26 weeks) studies with genotoxic (by Salmonella), non-genotoxic carcinogens, genotoxic non-carcinogens, non-genotoxic non-carcinogens revealed relatively high concordance oj the response of the Tg mouse with classical bioassay across classes of carcinogenic agents. Mechanistic basis for carcinogensis in the model are being elucidated in terms of the role of overexpression and/or point mutation of the transgene. This report review the initial studies of validation of the model and preliminary results of on-going ILSI HESI ACT project will be presented.

• Asian Pacific Journal of Cancer Prevention
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• 제16권8호
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• pp.3307-3312
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• 2015

The papillary patterned lesion of thyroid may be challenging with many diagnostic pitfalls. Tumor stroma plays an important part in the determination of the tumor phenotype. CD34 is thought to be involved in the modulation of cell adhesion and signal transduction as CD34(+) fibrocytes are potent antigen-presenting cells. Smooth muscle actin (SMA) positivity could be diagnostic for fibroblast activation during tumorigenesis. We aimed to examine the expression of CD34 and alphaSMA in the stroma of papillary thyroid hyperplasia, papillary thyroid carcinoma and papillary tumors of uncertain malignant potential in order to elucidate their possible differential distribution and roles. A total number of 54 cases with papillary thyroid lesions were studied by routine H&E staining, CD34 and ASMA immunostaining. ASMA was not expressed in benign papillary hyperplastic lesions while it was expressed in papillary carcinoma, indicating that tumors have modulated stroma. Although the stroma was not well developed in papillary lesions with equivocal features of uncertain potentiality, CD34 was notable in such cases with higher incidence in malignant cases. So ASMA as well as CD34 could predict neoplastic behavior, pointing to the importance of the stromal role. Differences between groups suggest that the presence of CD34 + stromal cells is an early event in carcinogensis and is associated with neoplasia, however ASMA+ cells are more likely to be associated with malignant behavior and metastatic potential adding additional tools to the light microscopic picture helping in diagnosis of problematic cases with H&E.

• 한국환경성돌연변이발암원학회지
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• 제9권1호
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• pp.1-12
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• 1989

특정 발암원의 조직특이성 암유발기전을 연구하기 위하여 DMBA의 구강투여 또는 NMU의 동맥주입에 의하여 유암이 유도되는 실험모델을 대상으로 선택하였다. 본 실험에서는 화학적 발암원의 유암유발기전에 미치는 숙주인 흰쥐의 연령효과를 아울러 비교분석하였으며, 특히 발암원의 조직내 활성화, 불활화 및 해독 그리고 DNA 손상과 수성등의 변화를 구명하였다. 유암의 발생율은 1년생 흰쥐보다 생후 50일 흰쥐에서 현저하게 높았다. 특정조직의 선택적 발암기전을 설명하는 기전의 일환으로 조직 DNA의 특정 발암원에 의한 공유결합성 지표(covalent binding index, CBI)를 발암원의 활성화 기전 지표로는 cytochrome P450의 함량을 반면 불확화의 지표로는 glutathione S-transferase와 peroxide의 활성을 비교하였다. 조직의 CBI는 생후 50일군의 유선조직이 DMBA나 NMU에 대하여 간조직보다 유의하게 높았으며 시험관내 CBI 실험에서는 생후 50일군 유선조직의 microsome 분획의 발암원 활성화능이 보다 높음을 관찰하였다. 또한 T.C.D.D. 의존성 cytochrome P450 함량도 생후 50일군에서 가장 높았다. 그러나 불활화 효소들은 연령 변화에 따라 유의한 변화를 보여주지 않았다. 상기의 결과들은 DMBA나 NMU와 같은 발암물질이 특정조직, 특히 유선조직에 생후 50일군에서 유암을 선택적으로 유발하는 기전은 표적 조직의 높은 발암원 활성화능, 낮은 불활화등 그리고 효율이 낮은 DNA 수선능이 연계적으로 작동함으로써 이루어지고 있음을 보여주고 있다.

• Journal of Oral Medicine and Pain
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• 제30권3호
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• pp.301-317
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• 2005

전 세계적으로 구강암의 빈도는 점점 증가 추세이며, 특히 한국인의 있어 혀(tongue)는 구강암이 가장 호발하는 장소이다. 구강암은 발암 단계에서부터 과증식 병소(hyperplastic lesion), 이형성(dysplasia) 및 상피내암(carcinoma in situ) 을 거쳐 악성 암종으로 발전하는 다단계 발암과정을 보이며, 분자 생물학적 변이가 구강암을 진행시킴이 널리 알려져 있다. 또한, 구강암은 일반적으로 암세포의 증식 및 고사(apoptosis)의 억제가 중요한 역할을 하고 있다 알려져 있다. 그리고, Bcl-2 family 는 세포 고사에 주요한 역할을 하고 있음이 알려져 있다. 그러나, 이들과 관련한 구강암 발생과정의 변화에 대해서는 널리 연구된 바가 없다. 본 연구는 백서에서 발암 물질인 4-NQO로 구강암을 유도시키고, 구강암 발생 다단계별로 Bcl-2 family의 mRNA 변화를 RT-PCR을 이용해 살펴보았다. Bcl-2 family는 크게 3군, 즉 1) anti-apoptotic, 2) pro-apoptotic, 그리고 3) BH3 only protein으로 분류할 수 있으며, 본 연구에서 anti-apoptotic molecules인 Bcl-w는 모든 군에서 발현이 감소되었으며, Bcl-2는 발현이 증가 되었다. pro-apoptotic molecules에서는 Bad가 제 3군 (편평세포암종)에서 발현이 증가 되었고, 나머지는 감소하였다. BH-3 only protein에서는 Bmf가 제 2군에서, BBC3가 제 3군에서 발현이 증가하였고, 나머지는 모든 군에서 감소하였다. 결론적으로, 4-NQO로 유도된 백서의 발암단계에서, Bcl-2 family의 mRNA 양상은 다양하게 관찰되었으나, Bad 및 BBC3 mRNA가 제 3군에서, Bmf mRNA가 제 2군에서의 발현이 특별함을 알 수 있어, 다단계 발암과정에서의 구강암을 진단하는데 유용하리라 사료된다.

• 대한약리학회지
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• 제29권2호
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• pp.275-282
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• 1993

Microsomal epoxide hydrolase (mEH)은 epoxide형 중간대사물을 해독화하는 효소이다. 본 실험실에서는 thiazole 또는 pyrazine을 rat에 투여할 때 mEH mRNA수준이 증가되고 mEH가 유도증가한다는 것을 밝힌바 있다(Carcinogenesis, Kim et al, 1993). 본 연구에서는 Thiazole처리를 한 rat의 간 microsome 분획으로 부터 DEAE-cellulose column chromatography를 이용하여 mEH를 순수분리하였고, 이를 SDS-PAGE분석 및 N 말단 amino acid 서열분석으로 확인하였다. Pyrazine처리를 한 rat의 간 microsome분획에서는 mEH와 더불어 이와 관련된 43 kDa 단백질이 함께 정제되었다. 정제된 thiazole 유도성 mEH를 토끼에 주사하여 항체를 생산하였고, 이 항체를 이용한 immunoblot 분석을 하였을 때 간 microsome 분획의 mEH가 thiazole투여군에서는 대조군에 비하여 10배, pyrazine 투여군에서 7배 증가하였다. Pyrazine처치한 rat의 간 microsome 분획에서는 mEH 관련성 43 kDa 단백질이 동시 유도증가하는 것을 면역화학적 반응으로도 확인하였다. 이때 Pyrazine으로 유도된 rat의 간 microsome 분획 또는 정제분획에 존재하는 43 kDa 단백질과 mEH의 비율은 1 : 15로 나타났다. 정제된 mEH와 43 kDa 단백질의 N 말단 amino acid 서열을 분석하였을때 43 kDa 단백질의 N 말단이 mEH와 동일하게 나타나 관련 단백질임을 확인하였다. 이러한 mEN 유도현상에 종차가 있는지를 알아보기 위하여 thiazole과 pyrazine을 각각 rabbit에 투여하였을 때 rabbit에서 는 mEH의 유도증가가 일어나지 않았으며, pyrazine 투여군에서 43 kDa 단백질의 증가는 관찰 되었다. 본 연구는 thiazole 또는 pyrazine 투여후 mEH 발현이 유도증가되며, pyrazine 투여 후에는 mEH 및 이와 관련된 43 kDa 단백질이 동시유도되고, 이러한 mEH 유도발현에 rat와 rabbit간에는 종차가 있음을 보여준다.