• 한국자원식물학회:학술대회논문집
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• 한국자원식물학회 2019년도 춘계학술대회
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• pp.93-93
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• 2019

In this study, we evaluated the anti-cancer activity and potential molecular mechanism of 70% ethanol extracts of branches from Taxillus yadoriki parasitic to Neolitsea sericea (TN-NS-B) against human lung cancer cells, A549. TY-NS-B dose-dependently suppressed the growth of A549 cells. TY-NS-B decreased ${\beta}$-catenin protein level, but not mRNA level in A549 cells. The downregulation of ${\beta}$-catenin protein level by TY-NS-B was attenuated in the presence of MG132. Although TY-NS-B phosphorylated ${\beta}$-catenin protein, the inhibition of $GSK3{\beta}$ by LiCl did not blocked the reduction of ${\beta}$-catenin by TY-NS-B. In addition, TY-NS-B decreased ${\beta}$-catenin protein in A549 cells transfected with Flag-tagged wild type ${\beta}$-catenin or Flag-tagged S33/S37/T41 mutant ${\beta}$-catenin construct. Our results suggested that TN-NS-B may downregulate ${\beta}$-catenin protein level independent on GSK3${\beta}$-induced ${\beta}$-catenin phosphorylation. Based on these findings, TY-NS-B may be a potential candidate for the development of chemopreventive or therapeutic agents for human lung cancer.

• The Korean Journal of Physiology and Pharmacology
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• 제18권1호
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• pp.61-66
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• 2014

Lung cancer is still the number one cause of death from cancer worldwide. The clinical effect of platinum-based chemotherapy for non-small cell lung cancer is constrained by the resistance to drug. To overcome chemo-resistance, various modified treatment including combination therapy has been used, but overall survival has not been improved yet. In this study, chemo-resistant lung cancer cells, A549/Cis and H460/Cis, were developed by long-term exposure of cells to cisplatin and the proliferative capability of these resistant cells was verified to be reduced. We found cytotoxic effect of epigallocatechin gallate (EGCG), a major catechin derived from green tea, on both the parental lung cancer cells, A549 and H460, and their cisplatin resistant cells, A549/Cis and H460/Cis. ELISA and Western blot analysis revealed that EGCG was able to increase interlukine-6 (IL-6) production per cell, whereas its downstream effector Signal transducers and activators of transcription 3 (STAT3) phosphorylation was not changed by EGCG, indicating that IL-6/STAT3 axis is not the critical signaling to be inhibited by EGCG. We next found that EGCG suppresses the expression of both Axl and Tyro 3 receptor tyrosine kinases at mRNA and protein level, explaining the cytotoxic effect of EGCG on lung cancer cells, especially, regardless of cisplatin resistance. Taken together, these data suggest that EGCG impedes proliferation of lung cancer cells including their chemo-resistant variants through downregulation of Axl and Tyro 3 expression.

• 동의생리병리학회지
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• 제19권4호
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• pp.1050-1054
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• 2005

Recently, arsenic compounds were considered as novel agents for treatment of acute promyelocytic leukemia and malignant tumors. However, it showed severe toxicity effect on normal tissue at the same time. In this study, to investigate the possible molecular mechanism (s) of arsenic compounds as candidate of anti-cancer drugs, we compared the abilities of two arsenic compounds, tetraarsenic oxide $(AS_4O_6)$ and arsenic trioxide (diarsenic oxide, $As_2O_3$), to induce cell growth inhibition as well as apoptosis induction in A549 human non-small cell lung cancer cells. Both $As_4O_6\;and\;As_2O_3$ treatment declined the cell growth and viability of A549 cells in a concentration-dependent manner, which was associated with induction of G1 arrest of the cell cycle and apoptotic cell death. However, $As_4O_6$ induced growth inhibition and apoptosis in A549 cells at much lower concentrations than $As_2O_3.\;As_4O_6$ down-regulated the levels of anti-apoptotic Bcl-2 protein, however, the levels of Bax, a pro-apoptotic protein, were up-regulated in a dose-dependent manner. In conclusion, $As_4O_6$ might be a new arsenic compound which may induce apoptosis in A549 cells by modulation the Bcl-2 family and deserves further evaluation.

• Journal of Microbiology and Biotechnology
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• 제30권6호
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• pp.885-892
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• 2020

Chemotherapy regimens for non-small cell lung cancer (NSCLC) have various adverse effects on the human body. For this reason, probiotics have received attention regarding their potential value as a safe and natural complementary strategy for cancer prevention. This study analyzed the anticancer effects of aqueous extracts of probiotic bacteria Bifidobacterium bifidum (BB), Bifidobacterium longum (BL), Bifidobacterium lactis (BLA), Bifidobacterium infantis 1 (BI1), and Bifidobacterium infantis 2 (BI2) on NSCLC cell lines. When the aqueous extracts of probiotic Bifidobacterium species were applied to the NSCLC cell lines A549, H1299, and HCC827, cell death increased considerably; in particular, the aqueous extracts from BB and BLA markedly reduced cell proliferation. p38 phosphorylation induced by BB aqueous extract increased the expression of cleaved caspase 3 and cleaved poly (ADP-ribose) polymerase (PARP), consequently inducing the apoptosis of A549 and H1299 cells. When the p38 inhibitor SB203580 was applied, phosphorylation of p38 decreased, and the expression of cleaved caspase 3 and cleaved PARP was also inhibited, resulting in a reduction of cell death. In addition, BB aqueous extracts reduced the secretion of MMP-9, leading to inhibition of cancer cell invasion. By contrast, after transfection of short hairpin RNA shMMP-9 (for a knockdown of MMP-9) into cancer cells, BB aqueous extracts treatment failed to suppress the cancer cell invasiveness. According to our results about their anticancer effects on NSCLC, probiotics consisting of Bifidobacterium species may be useful as adjunctive anticancer treatment in the future.

• Tuberculosis and Respiratory Diseases
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• 제44권6호
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• pp.1271-1284
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• 1997

연구배경 : 종양괴사인자(tumor necrosis factor ; TNF)는 다양한 생물학적 기능을 가지고 있는 바, 그 중 생체 외에서 증명된 뚜렷한 항암 효과로 말미암아 최근 항암 유전자요법의 중요한 대상으로 관심을 모으고 있다. 현재 유전자 이입의 기술적 문제로 생체 외에서 암세포에 유전자 이입을 시행한 후 이를 다시 환자의 생체내로 이식하는 방법이 연구의 주종을 이루고 있다. 그러나 저자들의 과거의 연구를 포함한 여러 연구에서 TNF가 이입된 암세포는 TNF에 대해 내성을 보이는 것으로 증명되었고 이에는 새로이 방어 단백질을 합성하는 것이 관여할 것이라는 시사가 있었다. 이 획득내성의 기전을 밝히는 것이 종양생물학의 이해를 넓히고 보다 효과적인 항암 유전자요법을 개발하기위한 매우 중요한 과제로 생각된다.

• Asian Pacific Journal of Cancer Prevention
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• 제15권6호
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• pp.2511-2515
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• 2014

Objective: Lung cancer is one of the malignant tumors with greatest morbidity and mortality around the world. The keys to targeted therapy are discovery of lung cancer biomarkers to facilitate improvement of survival and quality of life for the patients with lung cancer. Translationally controlled tumor protein (TCTP) is one of the most overexpressed proteins in human lung cancer cells by comparison to the normal cells, suggesting that it might be a good biomarker for lung cancer. Materials and Methods: In the present study, the targeted efficacy of dihydroartemisinin (DHA) on TCTP expression in the A549 lung cancer cell model was explored. Results and Conclusions: DHA could inhibit A549 lung cancer cell proliferation, and simultaneously up-regulate the expression of TCTP mRNA, but down-regulate its protein expression in A549 cells. In addition, it promoted TCTP protein secretion. Therefore, TCTP might be used as a potential biomarker and therapeutic target for non-small cell lung cancers.

• Tuberculosis and Respiratory Diseases
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• 제49권1호
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• pp.60-71
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• 2000

배경 및 목적 : Cathepsin D는 리소솜에 위치하는 단백분해효소로서 종양의 침윤, 전이, 증식에 관여할 것으로 생각되며, 이러한 작용을 통해 예후에도 중요한 역할을 할 것으로 추정된다. 폐암에서의 Cathepsin D의 예후인자로서의 역할은 아직 확립되지 않고 논란이 많은 실정이다. 이 연구의 목적은 비소세포폐암에서 Cathepsin D 발현의 예후적인 중요성을 알고자 하였다. 방법 : 비소세포 폐암환자 중 치료 목적으로 수술적 처치를 시행한 총 54명의 환자를 대상으로 하여 적출한 폐조직의 면역조직화학적 염색으로 Cathepsin D의 발현을 관찰하고 생존기간 및 TNM 병기와의 관계를 보았다. 결과 : 종양세포에서의 Cathepsin D의 발현은 총 54례 중 18례에서 관찰되어 33.3%의 발현율을 보였으나, 발현군과 비발현군 사이에 조직학적 분화도, 암의 크기. 영역 림프절 침범, 병리조직적 병기(surgical-pathologic stage, p-stage)는 통계적인 유의한 차이를 보이지 않았다. 간질세포에서는 29례(53.7%)에서 중둥도에서 다량(moderate to massive)의 Cathepsin D가 발현되는 것이 관찰되었고, 발현양상과 병리조직적 병기사이에 통계적으로 유의한 관련성이 있었으나(p=0.031), 각각의 조직학적 분화도, 암의 크기, 영역 림프절 침범과는 관계가 없었다. 종양세포와 세포에서의 Cathepsin D 의 발현은 생존율로 표현한 예후와의 유의한 관련성이 없었다. 예후와 관련된 변수를 사용한 다변량 분석결과 영역림프절 침범이 유일한 독립적 예후인자가 되었으며 Cathepsin D는 예후 인자로서의 의미는 없었다. 결론 : 비소세포폐암의 간질세포내 Cathepsin D 발현양상은 병리조직적 병기와 유의한 관련성을 나타내어 종양 진행과의 관련 가능성을 제사하였으나, 다른 임상병리인자들 및 예후와의 관련성은 없었다. 종양세포내에서의 Cathepsin D 발현은 병리조직적 병기를 포함한 임상병리 인자들 및 예후와 관계가 없었다.

• Asian Pacific Journal of Cancer Prevention
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• 제14권7호
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• pp.4229-4233
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• 2013

Abraxane (nab-paclitaxel) is a member of the group of nano chemotherapeutics. It is approved for metastatic breast cancer and non small cell lung cancer. Trials for several cancer types including gynecological cancers, head and neck, and prostatic cancer are being studied. In this study, the antiproliferative and apoptotic effect of abraxane was evaluated on HeLa cell line originated from human cervix carcinoma. Three different doses ($D_1$=10 nM, $D_2$=50 nM, $D_3$=100 nM) were administered to HeLa cells for 24, 48 and 72 h. The 50 nM dose of abraxane decreased DNA synthesis from 4.62-0.08%, mitosis from 3.36-1.89% and increased apoptosis from 10.6-30% at 72 h. Additionally, tripolar metaphase plates were seen in mitosis preparations. In this study, abraxane effected cell kinetic parameters significantly. This results are consistent with other studies in the literature.

• Journal of Applied Biological Chemistry
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• 제61권2호
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• pp.119-124
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• 2018

두충(Eucommia ulmoides Oliver)잎 아세톤 추출물의 in vitro 항암 및 항산화 활성을 조사하였다. 두충잎 아세톤 추출물의 수율은 $1.13{\pm}0.033%$ (w/w)이었고, 총 페놀성 화합물 함량은 $36.7{\pm}1.96mg$ gallic acid equivalents/g-추출물로 나타났다. 세포증식을 절반 억제하는 추출물의 농도인 $GI_{50}$값은 사람의 암세포인 비소세포폐암세포(A549)에서 $53.4{\mu}g/mL$, 결장암세포(SNU-C4)에서 $53.8{\mu}g/mL$ 및 자궁경부암세포(HeLa)에서 $88.3{\mu}g/mL$이었고, 사람의 정상세포인 배아 폐 상피세포(L132)에서는 $153.9{\mu}g/mL$로 나타났다. 두충잎 아세톤 추출물은 사람의 정상세포에는 낮은 독성을 나타내면서 농도에 비례하여 사람의 비소세포폐암세포(A549)와 결장암세포(SNU-C4)의 증식을 효과적으로 억제하였다. DPPH 유리라디칼을 절반 소거하는 추출물의 농도인 $EC_{50}$값은 2 mg/mL 정도로 높게 나타났고, 환원력의 $EC_{50}$값은 $275.8{\mu}g/mL$, 지질과산화를 절반 저해하는 농도인 $EC_{50}$값은 $257.9{\mu}g/mL$이었다. 유근피 아세톤 추출물은 농도에 비례하여 우수한 환원력 및 지질과산화 억제활성을 보여주었다.

• Tuberculosis and Respiratory Diseases
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• 제72권2호
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• pp.124-131
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• 2012

Background: DNA damage-inducible 1 (Ddi1), one of the ubiquitin-like and ubiquitin-associated family of proteins, may function in the regulation of the ubiquitin-proteasome pathway, which has been validated as a target for antineoplastic therapy. We investigated Ddi1 expression in human lung cancer tissues and evaluated the relationship of this expression pattern with clinicopathological factors in patients with non-small-cell lung cancer (NSCLC). Methods: Ddi1 expression was examined by immunohistochemistry in tumor tissues from 97 patients with stage I NSCLC, who had undergone curative surgical resection at two tertiary referral hospitals from 1993~2004. None of the patients received preoperative chemotherapy and/or radiation therapy. Results: Thirty-nine (40.2%) of the 97 cases were positive for Ddi1. Ddi1 expression was dominantly seen in cytoplasm rather than in the nuclei of cancer cells in all histological types, whereas adjacent nontumoral lung tissue showed negative Ddi1 staining in most cases. Ddi1 expression tended to increase in well-differentiated tumors but without statistical significance. Positive Ddi1 expression was associated with a tendency for better disease-free survival and disease-specific survival, although the difference was not significant. Conclusion: Ddi1 expression is a property of NSCLC. Because Ddi1 could be a potential target for cancer therapy, more research is needed to evaluate its role in NSCLC.