Subscribe to RSS
Download PDF
DOI: 10.1055/s-2007-981527
© Georg Thieme Verlag KG Stuttgart · New York
A Novel Polyacetylene Significantly Inhibits Angiogenesis and Promotes Apoptosis in Human Endothelial Cells through Activation of the CDK Inhibitors and Caspase-7
Publication History
Received: November 14, 2006
Revised: April 23, 2007
Accepted: April 23, 2007
Publication Date:
11 June 2007 (online)
Abstract
A novel bioactive polyacetylene compound, 1,2-dihydroxy-5(E)-tridecene-7,9,11-triyne (compound 1), was identified from the Bidens pilosa extract using an ex vivo primary human umbilical vein endothelium cell (HUVEC) bioassay-guided fractionation protocol. Our results demonstrate that compound 1 (at 2.5 μg/mL) possessed significant anti-angiogenic effects, as manifested by an inhibition of HUVEC proliferation, migration, and the formation of tube-like structures in collagen gel. Moreover, compound 1 induced HUVECs to undergo cell death in a concentration- and time-dependent manner. The mechanisms underlying these pharmacological effects include reduced expression of cell cycle mediators such as CDK4, cyclins D1 and A, retinoblastoma (Rb) and vascular endothelial growth factor receptor 1 (VEGFR-1), and promotion of caspase-mediated activation of CDK inhibitors p21(Cip1) and p27(Kip). Moreover, apoptotic induction in HUVECs mediated by compound 1 was found to be in part through overexpression of FasL protein, down-regulation of anti-apoptotic Bcl-2, and activation of caspase-7 and poly(ADP-ribose) polymerase. This study demonstrates the potent anti-angiogenic and apoptotic activities of compound 1, suggesting that phytocompounds such as polyacetylenes deserve more attention regarding their potential as candidates for anti-angiogenic therapeutics.
Key words
Bidens pilosa - Compositae - polyacetylenes - HUVEC - angiogenesis - apoptosis - CDK inhibitors
- Supporting Information for this article is available online at
- Supporting Information .
References
- 1 Folkman J. Angiogenesis in cancer, vascular, rheumatoid and other disease. Nat Med. 1995; 1 27-31.
- 2 Folkman J, Shing Y. Angiogenesis. J Biol Chem. 1992; 267 10 931-4.
- 3 Boehm T, Folkman J, Browder T, O'Reilly M S. Antiangiogenic therapy of experimental cancer does not induce acquired drug resistance. Nature. 1997; 390 404-7.
- 4 Chang S L, Chang C L, Chiang Y M, Hsieh R H, Tzeng C R, Wu T K. et al . Polyacetylenic compounds and butanol fraction from Bidens pilosa can modulate the differentiation of helper T cells and prevent autoimmune diabetes in non-obese diabetic mice. Planta Med. 2004; 70 1045-51.
- 5 Chang J S, Chiang L C, Chen C C, Liu L T, Wang K C, Lin C C. Antileukemic activity of Bidens pilosa L. var. minor (Blume) Sherff and Houttuynia cordata Thunb. Am J Chin Med. 2001; 29 303-12.
- 6 Rojas J J, Ochoa V J, Ocampo S A, Munoz J F. Screening for antimicrobial activity of ten medicinal plants used in Colombian folkloric medicine: a possible alternative in the treatment of non-nosocomial infections. BMC Complement Altern Med. 2006; 6 2.
- 7 Ubillas R P, Mendez C D, Jolad S D, Luo J, King S R, Carlson T J. et al . Antihyperglycemic acetylenic glucosides from Bidens pilosa . Planta Med. 2000; 66 82-3.
- 8 Chiang Y M, Chuang D Y, Wang S Y, Kuo Y H, Tsai P W, Shyur L F. Metabolite profiling and chemopreventive bioactivity of plant extracts from Bidens pilosa . J Ethnopharmacol. 2004; 95 409-19.
- 9 Wu L W, Chiang Y M, Chuang H C, Wang S Y, Yang G W, Chen Y H. et al . Polyacetylenes function as anti-angiogenic agents. Pharm Res. 2004; 21 2112-9.
- 10 Chiang Y M, Lo C P, Chen Y P, Wang S Y, Yang N S, Kuo Y H. et al . Ethyl caffeate suppresses NF-κB activation and its downstream inflammatory mediators, iNOS, COX-2, and PGE2 in vitro or in mouse skin. Br J Pharmacol. 2005; 146 352-63.
- 11 Jaffe E A, Nachman R L, Becker C G, Minick C R. Culture of human endothelial cells derived from umbilical veins. Identification by morphologic and immunologic criteria. J Clin Invest. 1973; 52 2745-56.
- 12 Boukamp P, Petrussevska R T, Breitkreutz D, Hornung J, Markham A, Fusenig N E. Normal keratinization in a spontaneously immortalized aneuploid human keratinocyte cell line. J Cell Biol. 1988; 106 761-71.
- 13 Yang S, Graham J, Kahn J W, Schwartz E A, Gerritsen M E. Functional roles for PECAM-1 (CD31) and VE-cadherin (CD144) in tube assembly and lumen formation in three-dimensional collagen gels. Am J Pathol. 1999; 155 887-95.
- 14 Montesano R, Orci L, Vassalli P. In vitro rapid organization of endothelial cells into capillary-like networks is promoted by collagen matrices. J Cell Biol. 1983; 97 1648-52.
- 15 Rucker G, Kehrbaum S, Sakulas H, Lawong B, Goeltenboth F. Acetylenic glucosides from Microglossa pyrifolia . Planta Med. 1992; 58 266-9.
- 16 Lin C M, Chang H, Chen T H, Wu I H, Chiu J H. Wogonin inhibits IL-6-induced angiogenesis via down-regulation of VEGF and VEGFR-1, not VEGFR-2. Planta Med. 2006; 72 1305-10.
- 17 Sherr C J, Roberts J M. Inhibitors of mammalian G1 cyclin-dependent kinases. Genes Dev. 1995; 9 1149-63.
- 18 Matsushime H, Quelle D E, Shurtleff S A, Shibuya M, Sherr C J, Kato J Y. D-type cyclin-dependent kinase activity in mammalian cells. Mol Cell Biol. 1994; 14 2066-76.
- 19 Resnitzky D, Gossen M, Bujard H, Reed S I. Acceleration of the G1/S phase transition by expression of cyclins D1 and E with an inducible system. Mol Cell Biol. 1994; 14 1669-79.
- 20 Levkau B, Koyama H, Raines E W, Clurman B E, Herren B, Orth K. et al . Cleavage of p21Cip1/Waf1 and p27Kip1 mediates apoptosis in endothelial cells through activation of Cdk2: role of a caspase cascade. Mol Cell. 1998; 1 553-63.
- 21 Polyak K, Kato J Y, Solomon M J, Sherr C J, Massague J, Roberts J M. et al . p27Kip1, a cyclin-Cdk inhibitor, links transforming growth factor-beta and contact inhibition to cell cycle arrest. Genes Dev. 1994; 8 9-22.
- 22 Matsuoka S, Edwards M C, Bai C, Parker S, Zhang P, Baldini A. et al . p57KIP2, a structurally distinct member of the p21CIP1 Cdk inhibitor family, is a candidate tumor suppressor gene. Genes Dev. 1995; 9 650-62.
1 These authors contributed equally to this article.
Lie-Fen Shyur, Ph.D.
Agricultural Biotechnology Research Center
Academia Sinica
Taipei
Taiwan
Republic of China
Phone: +886-2-2651-5028
Email: lfshyur@ccvax.sinica.edu.tw
- www.thieme-connect.de/ejournals/toc/plantamedica