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http://dx.doi.org/10.3746/jfn.2010.15.2.137

Diallyl Sulfides (DAS) and Diallyl Disulfides (DADS) Exhibit a Suppressive Effect on the Proliferation and Migration of Vascular Smooth Muscle  

Kim, Min-Ju (National Research Laboratory for Clinical Nutrigenetics/Nutrigenomics, Department of Food and Nutrition, Yonsei University)
Kwak, Jung-Hyun (National Research Laboratory for Clinical Nutrigenetics/Nutrigenomics, Department of Food and Nutrition, Yonsei University)
Baek, Seung-Han (Department of Biology, College of Natural Science, Yonsei University)
Yeo, Hyun-Yang (Research Institute National Cancer Center, Colorectal Cancer Branch)
Song, Ju-Hyun (National Research Laboratory for Clinical Nutrigenetics/Nutrigenomics, Department of Food and Nutrition, Yonsei University)
Cho, Bong-Jun (Interdisciplinary Course of Science for Aging Graduate School, Yonsei University)
Kim, Oh-Yoen (National Research Laboratory for Clinical Nutrigenetics/Nutrigenomics, Department of Food and Nutrition, Yonsei University)
Publication Information
Preventive Nutrition and Food Science / v.15, no.2, 2010 , pp. 137-142 More about this Journal
Abstract
Previous studies report that organo-sulfur compounds derived from garlic inhibited smooth muscle cell (SMC) proliferation and induced apoptosis of cancer cells. Recently, lipid-soluble compounds such as diallyl sulfides (DAS) and diallyl disulfides (DADS) have been reported to more effectively suppress tumor cell proliferation. However, there were few studies on the suppressive effects of lipid-soluble garlic sulfur compounds on the proliferation and migration of vascular smooth muscle cells (VSMC). Therefore, this study investigated the effect of DAS and DADS on VSMC proliferation/migration induced by oleic acid (OA), a principal fatty acid in circulating triglyceride of blood stream. Assays performed include a tetrazole (MTT) assay, a wound healing assay and a Western blots. VSMC proliferations were enhanced by OA in a dose-dependent manner at concentrations of $10{\sim}50\;{\mu}M$ and inhibited by DAS and DADS compared to non-treated control. OA-induced proliferations were also attenuated by DAS and DADS. OA-induced cell migrations were 2.5 times higher than non-treated control, and they were significantly attenuated by DAS (32% at $150\;{\mu}M$ and 50% at $200\;{\mu}M$) and DADS (40% at $150\;{\mu}M$ and 46% at $200\;{\mu}M$). OA-induced cell migration was also attenuated by PD98059 (ERK inhibitor), SB203580 (P38 inhibitor) and particularly by LY204002 (PI3K inhibitor) and SP600125 (JNK2 inhibitor). Additionally, Western blot assays showed that OA-induced JNK1/2-phosphorylation was down-regulated after treatment with DAS and DADS. In conclusion, the findings of our study support the idea that DAS and DADS may have a suppressive effect on the proliferation and migration of OA-induced VSMC and that this effect may be partly associated with PI3K and JNK2 pathways.
Keywords
diallyl sulfides; diallyl disulfides; vascular smooth muscle cell; proliferation; migration;
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1 Zhu L, Sun G, Zhang H, Zhang Y, Chen X, Jiang X, JiangX, Krauss S, Zhang J, Xiang Y, Zhang CY. 2009. PGC-1$\alpha$ is a key regulator of glucose-induced proliferation and migration in vascular smooth muscle cells. PLoS One 4:e4182.   DOI   ScienceOn
2 Zhang Y, Liu C, Zhu L, Jiang X, Chen X, Qi X, LiangX, Jin S, Zhang P, Li Q, Wang D, Liu X, Zeng K, ZhangJ, Xiang Y, Zhang CY. 2007. PGC-1$\alpha$ inhibits oleic acid induced proliferation and migration of rat vascular smooth muscle cells. PLos One 11: e1137.
3 Lu G, Greene EL, Nagai T, Egan BM. 1998. Reactive oxygen species are critical in the oleic acid-mediated mitogenic signaling pathway in vascular smooth muscle cells.Hypertension 32: 1003-1010.   DOI   ScienceOn
4 Lima TM, Kanunfre CC, Pompeia C, Verlengia R, CuriR. 2002. Ranking the toxicity of fatty acids on Jurkat and Raji cells by flow cytometric analysis. Toxicol In Vitro 16: 741-747.   DOI   ScienceOn
5 Lu G, Morinelli TA, Meier KE, Rosenzweig SA, EganBM. 1996. Oleic acid-induced mitogenic signaling in vascular smooth muscle cells. A role for protein kinase C. Circ Res 79: 611-618.   DOI   ScienceOn
6 Thejass P, Kuttan G. 2007. Inhibition of angiogenic differentiation of human umbilical vein endothelial cells by diallyl disulfide (DADS). Life Sci 80: 515-521.   DOI   ScienceOn
7 Jo HJ, Song JD, Kim KM, Cho YH, Kim KH, Park YC.2008. Diallyl disulfide induces reversible G2/M phase arrest on a p53-independent mechanism in human colon cancer HCT-116 cells. Oncol Rep 19: 275-280.
8 Ispanovic E, Haas TL. 2006. JNK and PI3K differentially regulate MMP-2 and MT1-MMP mRNA and protein in response to actin cytoskeleton reorganization in endothelial cells. Am J Physiol Cell Physiol 291: C579-C588.   DOI   ScienceOn
9 Ciapaite J, van Bezu J, van Eikenhorst G, Bakker SJ,Teerlink T, Diamant M, Heine RJ, Krab K, WesterhoffHV, Schalkwijk CG. 2007. Palmitate and oleate have distinct effects on the inflammatory phenotype of human endothelial cells. Biochim Biophys Acta 1771: 147-154.   DOI   ScienceOn
10 Kavurma MM, Khachigian LM. 2003. ERK, JNK, and p38 MAP kinases differentially regulate proliferation and migration of phenotypically distinct smooth muscle cell subtypes. J Cell Biochem 89: 289-300.   DOI   ScienceOn
11 Artwohl M, Lindenmair A, Roden M, Waldhausl WK,Freudenthaler A, Klosner G, Ilhan, Luger AA, Baumgartner-Parzer SM. 2009. Fatty acids induce apoptosis in human smooth muscle cells depending on chain length, saturation, and duration of exposure. Atherosclerosis 202:351-362.   DOI   ScienceOn
12 Arunkumar A, Vijayababu MR, Kanagaraj P, BalasubramanianK, Aruldhas MM, Arunakaran J. 2005. Growth suppressing effect of garlic compound diallyl disulfide on prostate cancer cell line (PC-3) in vitro. Biol Pharm Bull28: 740-743.   DOI   ScienceOn
13 Ferri N, Yokoyama K, Sandilek M, Paoletti R, Apitz-CastroR, Gelb MH, Corsini A. 2003. Ajoene, a garlic compound, inhibits protein prenylation and arterial smooth muscle cell proliferation. Bri J Pharmacol 138: 811-818.   DOI   ScienceOn
14 Tan H, Ling H, He J, Yi L, Zhou J, Lin M, Su Q. 2008. Inhibition of ERK and activation of p38 are involved in diallyl disulfide induced apoptosis of leukemia HL-60 cells. Arch Pharm Res 31: 786-793.   과학기술학회마을   DOI   ScienceOn
15 Knowles LM, Milner JA. 2001. Possible mechanism by which allyl sulfides suppress neoplastic cell proliferation. J Nutr 131: 1061S-1066S.   DOI
16 Wu XJ, Hu Y, Lamy E, Mersch-Sundermann V. 2009.Apoptosis induction in human lung adenocarcinoma cells by oil-soluble allyl sulfides: triggers, pathways and modulators. Environ Mol Mutagen 50: 266-275.   DOI   ScienceOn
17 Greene EL, Lu G, Zhang D, Egan BM. 2001. Signaling events mediating the additive effects of oleic acid and angiotensin II on vascular smooth muscle cell migration. Hypertension 37: 308-312.   DOI   ScienceOn
18 Nigam N, Shukla Y. 2007. Preventive effects of diallyl sulfide on 7,12-dimethylbenz[a]anthracene induced DNA alkylation damage in mouse skin. Mol Nutr Food Res 51:1324-1328.   DOI   ScienceOn
19 Thejass P, Kuttan G. 2007. Inhibition of angiongenic differentiation of human umbilical vein endothelial cells by diallyl disulfide (DADS). Life Sci 80: 515-521.   DOI   ScienceOn
20 Kwok CF, Shih KC, Hwu CM, Ho LT. 2000. Linoleic acid and oleic acid increase the endothelin-1 binding and action in cultured rat aortic smooth muscle cells. Metabolism 49: 1386-1389.   DOI   ScienceOn
21 Doran AC, Meller N, McNamara CA. 2008. Role of smooth muscle cells in the initiation and early progression of atherosclerosis. Arterioscler Thromb Vasc Biol 28: 812-819.   DOI   ScienceOn
22 Dirsch VM, Gerbes AL, Vollmar AM. 1998. Ajoene, a compound of garlic, induces apoptosis in human promyeloleukemic cells, accompanied by generation of reactive oxygen species and activation of nuclear fator-${\kappa}B$. Mol Pharm 53: 402-407.   DOI
23 Yun MR, Lee JY, Park HS, Heo HJ, Park JY, Bae SS,Hong KW, Sung SM, Kim CD. 2006. Oleic acid enhances vascular smooth muscle cell proliferation via phosphatidylinositol 3-kinase/Akt signaling pathway. Pharmacol Res 54: 97-102.   DOI   ScienceOn
24 Suzuki LA, Poot M, Gerrity RG, Bornfeldt KE. 2001.Diabetes accelerates smooth muscle accumulation in lesions of atherosclerosis: lack of direct growth-promoting effects of high glucose levels. Diabetes 50: 851-860.   DOI   ScienceOn
25 Miron T, Wilchek M, Sharp A, Nakagawa Y, Naoi M,Nozawa Y, Akao Y. 2008. Allicin inhibits cell growth and induces apoptosis through the mitochondrial pathway in HL60 and U937 cells. J Nutr Biochem 19: 524-535.   DOI   ScienceOn