• Asian Pacific Journal of Cancer Prevention
• /
• 제13권9호
• /
• pp.4669-4675
• /
• 2012

Objective: Nude mice with orthotopic transplantation of human ovarian epithelial cancer were used to investigate screening criteria for paraneoplastic normal ovarian tissue and the security of the freezing and thawing for ovarian tissue transplantation. Methods: Expression of CK-7, CA125, P53, survivin, MMP-2/TIMP-2 in paraneoplastic normal ovarian tissues were detected by RT-PCR as well as immunohistochemistry. The tissues of the groups with all negative indicators of RT-PCR, all negative indicators of immunohistochemistry, negative expression of CK-7, CA125 and survivin, positive expression of CK-7, CA125 and survivin, cancer tissues and normal ovarian tissues of nude mice were used for freezing and thawing transplantation, to analyze overt and occult carcinogenesis rates after transplantation. Results: When all indicators or the main indicators, CK-7, CA125 and survivin, were negative, tumorigenesis did not occur after transplantation. In addition the occult carcinogenesis rate was lower than in the group with positive expression of CK-7, CA125 and survivin (P<0.01). After subcutaneous and orthotopic transplantation of ovarian tissues, rates did not change (P>0.05). There was no statistical significance among rates after transplantation of ovarian tissues which were obtained under different severity conditions (P>0.05). Conclusion: Negative expression of CK-7, CA125 and survivin can be treated as screening criteria for security of ovarian tissues for transplantation. Immunohistochemical methods can be used as the primary detection approach. Both subcutaneous and orthotopic transplantation are safe. The initial severity does not affect the carcinogenesis rate after tissue transplantation. Freezing and thawing ovarian tissue transplantation in nude mice with human epithelial ovarian carcinoma is feasible and safe.

• 한국균학회지
• /
• 제23권4호통권75호
• /
• pp.285-297
• /
• 1995

영지의 균사체를 분획화하여 ${\beta}-glucan$성 다당류인 ganoderan을 분리한 결과, 12%의 균체외성, 13%의 세포질성, 그리고 75%의 세포벽성 분획으로 각각 수획되었다. 각각의 분획들은 추출 부위와는 상관없이 포도당을 가장 많이 포함하고 있었으며, ${\beta}-glucan$의 특정을 지닌 다당류이었다. Ganoderan의 구성당 및 구성 아미노산은 균사체 추출부위에 따라 상이한 비율을 나타내었다. 이들의 생리적 활성을 검색한 결과, 항 보체 활성은 균체외성이며 수용성인 EXO-WS 분획이 38%로 가장 우수하였으며, 세포벽에서 추출한 알칼리 가용성이며 수용성인 CW-AS-WS 분획이 37%를 나타내었다. 항암활성은 CW-AS-WS 분획이 가장 우수하였으며 94%의 종양 억제율을 보였다. CW-AS-WS 는 평균 분자량 20kD로 80% 의 포도당으로 이루어진 ${\beta}-glucan$성 다당류이다.

• 대한한방종양학회지
• /
• 제9권1호
• /
• pp.1-14
• /
• 2003

Objective : Ikiyangeumhaedoc-tang(IYHT) has an effect of nourishing Yin(陰) and Jin(津), and has been used to cancer patient effectively. In order to prove the anticancer's and antimetastic effect of IYHT experimentally, studies were done. Methods : We evaluated the cytotoxic activity on HT-1080 cells as well as inhibitory effect on activity of DNA topoisomerase Ⅰ, cell adhesion, cell invasion and proliferation of HUVEC cells induced by bFGF and measured the expression of mRNA(uPA, MMP2, TIMP2), p-ERK protein, recovery effect of gap junctional intercellular communication by $H_{2}O_2$ and survival time of ICR mice bearing sacoma-180. Results : IYHT showed the inhibitory effect on DNA topoisomerase Ⅰ in the concentration of $100{\mu}g/ml,\;500{\mu}g/ml$ and the dosage-dependent inhibitory effect on the adhesion of HT-1080. The concentration of 1mg/ml of IYHT inhibited 15% of adhesion compared with control. IYHT decreased the expression of uPA, but not in MMP2, TIMP2 by RT-PCR and inhibited the expression of p-ERK effectively in the concentration of more than $500{\mu}g/ml.$ IYHT recovered the inhibited gap junctional intercellular communication by $H_{2}O_2$ to the level of 60% of normal control in the concentration of $400{\mu}g/ml$ but, did not extended the mean survival time of sarcoma 180-bearing mouse. Conclusions : It was concluded that IYHT could be applied usefully for prevention and treatment of human cancer, And also experimental study for the evaluation of molecular biological study and antimetastatic research would be recommended in the near future.

• Asian Pacific Journal of Cancer Prevention
• /
• 제16권7호
• /
• pp.3035-3042
• /
• 2015

Background: Isorhamnetin (Iso), a novel and essential monomer derived from total flavones of Hippophae rhamnoides that has long been used as a traditional Chinese medicine for angina pectoris and acute myocardial infarction, has also shown a spectrum of antitumor activity. However, little is known about the mechanisms of action Iso on cancer cells. Objectives: To investigate the effects of Iso on A549 lung cancer cells and underlying mechanisms. Materials and Methods: A549 cells were treated with $10{\sim}320{\mu}g/ml$ Iso. Their morphological and cellular characteristics were assessed by light and electronic microscopy. Growth inhibition was analyzed by MTT, clonogenic and growth curve assays. Apoptotic characteristics of cells were determined by flow cytometry (FCM), DNA fragmentation, single cell gel electrophoresis (comet) assay, immunocytochemistry and terminal deoxynucleotidyl transferase nick end labeling (TUNEL). Tumor models were setup by transplanting Lewis lung carcinoma cells into C57BL/6 mice, and the weights and sizes of tumors were measured. Results: Iso markedly inhibited the growth of A549 cells with induction of apoptotic changes. Iso at $20{\mu}g/ml$, could induce A549 cell apoptosis, up-regulate the expression of apoptosis genes Bax, Caspase-3 and P53, and down-regulate the expression of Bcl-2, cyclinD1 and PCNA protein. The tumors in tumor-bearing mice treated with Iso were significantly smaller than in the control group. The results of apoptosis-related genes, PCNA, cyclinD1 and other protein expression levels of transplanted Lewis cells were the same as those of A549 cells in vitro. Conclusions: Iso, a natural single compound isolated from total flavones, has antiproliferative activity against lung cancer in vitro and in vivo. Its mechanisms of action may involve apoptosis of cells induced by down-regulation of oncogenes and up-regulation of apoptotic genes.

• 대한미생물학회지
• /
• 제14권1호
• /
• pp.89-97
• /
• 1979

암환자(癌患者)에서 세포성면역반응(細胞性免疫反應)이 대체적(大體的)으로 억제(抑制)되었다는 사실(事實)은 여러 항원(抗原)에 대(對)한 피부반응(皮膚反應)의 감소(減少), 임파구(淋巴球)의 mitogen에 대(對)한 임파아구형성반응저하(淋巴芽球形成反應低下) 및 임파구(淋巴球)와 면양적혈구(緬羊赤血球)(SRBC)와의 자연로젤형성(自然로젤形成)의 감소(減少) 등에 의(依)하여 구명(究明)되었다. 그러나 이와 같은 현상(現象)에 대(對)한 기전(機轉)의 설명(說明)은 많은 연구(硏究)에도 불구(不句)하고 아직 미흡(未洽)하다. 본(本) 실험(實驗)에서 저자(著者)는 간암(肝癌) 및 폐암환자(肺癌患者)로부터 무균적(無菌的)으로 채취(採取)한 복수(腹水) 및 늑막액(肋膜液)을 마우스에 SRBC로 면역(免疫)하기 2일전(日前), 항원조사(抗原注射)와 동시(同時) 또는 항원주사(抗原注射) 2일(日)에 투여(投與)하여 마우스의 SRBC에 대(對)한 세포성(細胞性) 및 체액성면역반응(體液性免疫反應)에 미치는 영향(影響)을 실험(實驗)하였다. 그 결과(結果) SRBC로 면역(免疫)하기 전(前)에 암성삼출액(癌性渗出液)을 투여(投與)받은 마우스군(群)의 면역반응(免疫反應)은 대조군(對照群)의 면역반응(免疫反應)에 비(比)하여 유의성(有意性)있는 감소(減少)를 보인데 비(比)하여, 암성삼출액(癌性渗出液)을 SRBC와 동시(同時) 및 항원주사(抗原注射) 후(後)에 투여(投與)받은 마우스군(群)의 면역반응(免疫反應)은 대조군(對照群)의 그것과 유의(有意)한 차이(差異)가 없었다. 따라서 이상(以上)의 본(本) 실험결과(實驗結果)는 암성삼출액(癌性渗出液)이 면역억제인자(免疫抑制因子)를 가지고 있으며 이 억제인자(抑制因子)는 면역계(免疫系)의 afferent arc을 억제(抑制)함을 강력(强力)히 시사(示唆)한 증거(證據)라고 사료(思料)된다.

• 한국미생물·생명공학회지
• /
• 제31권4호
• /
• pp.355-361
• /
• 2003

사람 분변으로부터 대식세포 활성 증강효능이 있는 유산균을 선별하여 이를 동정한 결과 P. pentosaceus 동정되었으며, 이 균주를 P. pentosaceus EROM101로 명명하였다. P. pentosaceus EROM101의 면역증강 및 항암활성을 알아보기 위하여 실험동물에게 3주간 생균 및 파쇄액을 경구 투여한 뒤 대식세포와 비장세포의 활성화를 측정하였으며, 동시에 소장점막상피세포에서 생산되는 IgA의 함량을 측정하였다. P. pentosaceus EROM101의 경구 투여는 대식세포 및 비장세포의 분열을 촉진하여 면역증강 기능이 있는 것으로 나타났다. 특히, 생균보다 파쇄액에서 활성이 더 뛰어난 것으로 나타나, P. pentosaceus EROM101은 장내에서 생균으로 서식하여 지속적으로 면역증강 기능을 나타내는 것이 아닌 세포 구성물에서 면역증강활성이 있는 것으로 사료되었다. 또한, 소장점막상피세포에서 IgA의 분비량에서도 대조군보다 약 4배이상의 IgA 생산량을 증가시켜 장관면역 활성화 기능이 있는 것으로 판단되었다. 또한 P. pentosaceus EROM101 파쇄액이 Sarcoma 180 복수암세포를 이식해 준 실험동물 내에서 복수암성장을 억제하였으나, Sarcoma 180 세포열에 대한 세포독성을 나타내지 않아 면역증강에 의해서 항암 활성이 나타난 것으로 추측되었다. 이상의 연구결과에서 P. pentosaceus EROM101은 면역증강 능력이 있으며, 동시에 항암 활성을 기대할 수 있을 것으로 사료된다.

• Archives of Pharmacal Research
• /
• 제28권5호
• /
• pp.626-635
• /
• 2005

Liposome as a carrier of topotecan (TPT), a promising anticancer drug, has been reported in attempt to improve the stability and antitumor activity of TPT. However, the biodistr ibution pattern of TPT liposome in vivo and PEG-modified liposome containing TPT have not been studied systemically. In this paper, the in vitro stability and in vivo biodistribution behavior of several liposomes containing TPT with different lipid compositions and PEG-modification were studied. Compared with the 'fluid' liposome (S-Lip) composed of soybean phosphatidylcholine (SPC), the 'solid' liposome (H-Lip) composed of hydrogenated soybean phosphatidylcholine HSPC decreased the leaking efficiency of TPT from liposome and enhanced the stability of liposome in fetal bovine serum (FBS) or human blood plasma (HBP). The results of biodistribution studies in S$_{180}$ tumor-bearing mice showed that liposomal encapsulation increased the concentrations of total TPT and the ratio of lactone form in plasma. Compared with free TPT, S-Lip and H-Lip resulted in 5- and 19- fold increase in the area under the curve (AUC$_{0\rightarrow\propto}$), respectively. PEG- modified H-Lip (H-PEG) showed 3.7-fold increase in AUC$_{0\rightarrow\propto}$ compared with H-Lip, but there was no significant increase in t$_{1/2}$ and AUC$_{0\rightarrow\propto}$ for PEG-modified S-Lip (S-PEG) compared with S-Lip. Moreover, the liposomal encapsulation changed the biodistribution behavior, and H-Lip and H-PEG dramatically increased the accumulation of TPT in tumor, and the relative tumor uptake ratios were 3.4 and 4.3 compared with free drug, respectively. There was also a marked increase in the distribution of TPT in lung when the drug was encapsulated into H-Lip and H-PEG. Moreover, H-PEG decreased the accumulation of TPT in bore marrow compared with unmodified H-Lip. All these results indicated that the membrane fluidity of liposome has an important effect on in vitro stability and in vivo biodistribution pattern of liposomes containing TPT, and PEG-modified 'solid' liposome may be an efficient carrier of TPT.

• Radiation Oncology Journal
• /
• 제18권4호
• /
• pp.329-336
• /
• 2000

목적 : 마우스 간암에서 방사선과 각종 항암제와의 복합요법을 시행하여, 방사선 감수성을 증가시킬 수 있는 약물을 탐색하고자 하였다. 방법 : C3H/HeJ마우스에 마우스 간암인 HCa-1을 이식하고, 평균 직경 8 mm에 이르렀을 때, 방사선 조사(25 Gy), 항암 약물(5-Fu, 150 mg/kg; adriamycln, 8 mg/kg; paclltaxel, 40 mg/kg; gemcltablne, 50 mg/kg), 또는 방사선과 항암 약물의 복합 치료를 시행하였다 치료에 대한 종양 반응은 종양 성장 지연과 항진 요인으로 분석하였다. 항진 효과를 보인 약물에 대하여 그 기전 연구는 조직 절편에서 apoptotic 수준을 평가하고, 또한 조절물질의 발현을 분석하였다. p53, Bcl-2, Bax, Bcl-XL, Bcl-XS, p21$^{WAF1/CIP1}$의 발현 분석은 westeblotting으로 하였다. 결과 : Gemcltabine 만이 방사선 감수성을 증가시키는 것으로 나타났다(항진요인:1.6). Gemcltabine과 방사선의 복합 치료는 apoptosis 유도에서는 부가적 수준만을 보였다. 조절울질의 발현 양상은 방사선 단독에 비하여 방사선과 gemcitabine의 병용시 p21$^{WAF1/CIP1}$의 증가가 유의하게 관찰되었다. 결론 : Gemcitabiue은 마우스 간암에서 방사선 감수성을 증가시키는 것으로 나타났다. 이를 조절하는 요소로서 p21$^{WAF1/CIP1}$ 이 관여할 것으로 생각 된다.

• 대한수의학회지
• /
• 제45권1호
• /
• pp.85-91
• /
• 2005

Much of the interest on the chemopreventive properties of herbs and plants has been raised, whereas little is regarding to anti-tumor effect of farming and aquatic products. In the present study, the anti-tumor effect of hot-water extract of a seaweed, BLC (Sargassum fulvellum) and BLC/HEN egg was investigated using MCF-7 cells in vitro and in vivo systems. We found that the BLC extract and BLC/HEN egg inhibited cell proliferation in a dose-dependent manner, which might be mediated through up-regulation of p53. Furthermore, this test compound can directly induce apoptosis in MCF-7 cells, which might be mediated through up-regulation of a pro-apoptotic Bax protein and down-regulation of a anti-apoptotic Bcl-2 protein, not by immune system. Nude mice bearing established breast tumors (with exogenous estradiol) were treated with BLC extract and BLC/HEN egg. Treatment BLC extract and BLC/HEN egg caused a 42% and 71% inhibition of tumor growth, respectively. Both agents caused a significant inhibition of volume and weight growth of estrogen independent human breast tumors established from MCF-7 cells. Our results suggested that BLC extract and BLC/HEN egg have the efficacious effect of human breast cancer not only in vitro but also in vivo.

• 대한약리학회지
• /
• 제26권1호
• /
• pp.91-100
• /
• 1990

Benzylacyclouridines (BAU and BBAU)는 uridine phosphorylase (UrdPase)의 선택적이고 강력한 상경억제제이다. 보고된 바에 의하면 (Cancer Res., 44: 1852, 1984) Benzylacyclouridines가 5-fluoro-2'-deoxyuridine (FdUrd)의 인체 암세포에 대한 독성을 증가시켜 준다고 하였지만, L5187Y 세포를 사용한 본 실험에서는 Benzylacyclouridines가 FdUrd를 포함하여 5-fluorouridine (FUra) 모두에 대해 조금도 세포 독성을 증가시키지 못하였을 뿐만아니라, 오히려 세포를 그들 독성으로부터 투여량에 비례하여 보호하였다. 복강내 주사에 의한 생체실험에서도 Benzylacyclouridines는 5-fluorinated pyrimidine에 의한 L5187Y를 지닌 쥐(mouse)의 life-span을 연장시켜 주지 못하였다. 본 실험에서 Benzylacyclouridines가 기대했던 fluorinated pyrimidine 항암제의 효과를 증진시키지 못한 이유는 nucleosides의 anabolism이 UrdPase와 orotate phosphoribosyltransferase이 의한 sequential 작용에 의하던가 또는 Benzylacyclouridines에 의한 nucleosides의 수송억제에 의하던가, 아니면 두가지 다 복합적으로 작용한 결과로 생각된다.