Biomed Pap Med Fac Univ Palacky Olomouc Czech Repub. 2015, 159(1):053-059 | DOI: 10.5507/bp.2013.096

The anti-atherosclerotic effects of puerarin on induced-atherosclerosis in rabbits

Lidao Baoa, Ying Zhangb, Guomin Weib, Yi Wanga, Ruilian Maa, Rui Chenga, Xianhua Rena, Agula Bc
a Department of Pharmacy, Affiliated Hospital of Inner Mongolia Medical University, Hohhot 010059, P. R. China
b Department of Respiratory Medicine, Binzhou People's Hospital, Binzhou 256610, P. R. China
c College of Traditional Mongolia Medicine, Inner Mongolia Medical University, Hohhot 010110, P. R. China

Background: Cardiovascular disease is a major health issue worldwide, which has been well treated by the extracts of traditional herbs. Radix Puerariae, the dried root of the leguminous plant Pueraria lobata (Willd.) Ohwi, is a delicious vegetable in some southern provinces of China. Puerarin has also been widely used to treat human diseases, but few controlled studies are available.

Aim: To determine the anti-atherosclerotic effects of puerarin on fat diet-induced atherosclerosis (AS) in rabbits.

Methods: An AS model was established by feeding 60 rabbits a high-fat diet and randomly dividing them into 6 groups: (1) normal control, (2) a model group (3) the statin, simvastatin and groups (4), (5) and (6) received 3 different amounts of puerarin. The fasting sera of all animals were collected before and after 90 days treatment to determine the levels of total cholesterol (TC), triglyceride (TG), low density lipoprotein-cholesterol (LDL-C) and high density lipoprotein-cholesterol (HDL-C). The aortas were pathomorphologically examined. PCNA and PDGF-A protein levels were assessed by Western blot.

Results: On the 90th day, the levels of TC, TG and LDL-C were significantly lower in high- and middle-dose puerarin groups and simvastatin group than in the model group (P<0.05), and the HDL-C level was higher. The percentages of plaque area to the total aortic area differed significantly for high- and middle-dose puerarin groups, simvastatin group and model group (P<0.05). Whole blood viscosity increased in the high-fat diet groups, while those in the treatment groups (except for the low-dose puerarin group) were significantly lower than those in the model group (P<0.05). PCNA and PDGF-A protein expression levels of rabbit aorta were low in the normal group. Protein expression levels in the groups fed the high-fat diet were significantly increased (P<0.05), but those in the high-dose puerarin group and simvastatin group were significantly decreased compared with the model group (P<0.05).

Conclusions: Puerarin inhibits the formation and development of AS plaque and suppresses the migration and reproduction of vascular smooth muscle cells by decreasing PCNA and PDGF-A expressions in the rabbit. This is encouraging in terms of cardiovascular disease prevention/treatment.

Keywords: puerarin, rabbit, atherosclerosis, proliferation cell nuclear antigen, platelet-derived growth factor

Received: July 7, 2013; Accepted: December 19, 2013; Prepublished online: January 27, 2014; Published: March 9, 2015  Show citation

ACS AIP APA ASA Harvard Chicago Chicago Notes IEEE ISO690 MLA NLM Turabian Vancouver
Bao, L., Zhang, Y., Wei, G., Wang, Y., Ma, R., Cheng, R., Ren, X., & Agula, B. (2015). The anti-atherosclerotic effects of puerarin on induced-atherosclerosis in rabbits. Biomedical papers159(1), 053-059. doi: 10.5507/bp.2013.096
Share...
Download citation
  • BibTeX (.bib)
  • Bookends (.ris)
  • EasyBib (.ris)
  • EndNote (.enw)
  • EndNote 8 (.xml)
  • ISI WoS (.isi)
  • Medlars (.medlars)
  • Mendeley (.ris)
  • MODS (.xml)
  • Papers (.ris)
  • RefWorks (.txt)
  • RefManager (.ris)
  • RIS (.ris)
  • MS Word (.xml)
  • Zotero (.ris)
    • Open full article

    References

    1. LaRosa JC, Grundy SM, Waters DD, Shear C, Barter P, Fruchart JC, Gotto AM, Greten H, Kastelein JJ, Shepherd J, Wenger NK. Intensive Lipid Lowering with Atcrvastatin in Patients with stable coronary disease. N Eng J Med 2005;352:1425-35. Go to original source... Go to PubMed...
    2. Pan D, Yang J, Lu F, Xu D, Zhou L, Shi A, Cao K. Platelet- derived growth factor BB modulates PCNA protein synthesis partially through the transforming growth factor beta signaling pathway in vascular smooth muscle cells. Biochem Cell Biol 2007;85:606-15. Go to original source... Go to PubMed...
    3. Keramati AR, Singh R, Lin A, Faramarzi S, Ye ZJ, Mane S, Tellides G, Lifton RP, Mani A. Wild-type LRP6 inhibits, whereas atherosclerosis-linked LRP6R611C increases PDGF-dependent vascular smooth muscle cell proliferation. Proc Natl Acad Sci U S A 2011;108:1914-8. Go to original source... Go to PubMed...
    4. Qi H, Li L, Huang C, Li W, Wu C. Optimization and physicochemical characterization of thermosensitive poloxamer gel containing puerarin for ophthalmic use. Chem Pharm Bull (Tokyo) 2006;54:1500-7. Go to original source... Go to PubMed...
    5. Zhu YM, Ni C, Zhu L, Shen YL, Chen YY. [Effect and mechanism of puerarin on high glucose-induced hypo-responses in vascular contraction]. Zhongguo Ying Yong Sheng Li Xue Za Zhi 2011;27:62-5. Go to PubMed...
    6. Wang Q, Xu X. [Progresses in research of hemolysis induced by puerarin injection]. Zhongguo Zhong Yao Za Zhi 2011;36:1402-5. Go to PubMed...
    7. Tian F, Xu LH, Zhao W, Tian LJ, Ji XL. The optimal therapeutic timing and mechanism of puerarin treatment of spinal cord ischemia-reperfusion injury in rats. J Ethnopharmacol 2011;134:892-6. Go to original source... Go to PubMed...
    8. Li DZ, Hu YF, Yang KP. [Protective effect of puerarin on endothelial dysfunction of heat shock protein 60 induced specific immunity in apolipoprotein E-null mice]. Zhongguo Zhong Xi Yi Jie He Za Zhi 2006;26 Suppl:4-6.
    9. Chen R, Xue J, Xie M. Puerarin prevents isoprenaline-induced myocardial fibrosis in mice by reduction of myocardial TGF-beta1 expression. J Nutr Biochem 2012;23:1080-5. Go to original source... Go to PubMed...
    10. Liu JM, Ma L, He WP. [Therapeutic effect of puerarin therapy on sudden deafness]. [Clinical Trial Comparative Study Randomized Controlled Trial]. Di Yi Jun Yi Da Xue Xue Bao 2002;22:1044-5. Go to PubMed...
    11. Liu R, Xing D, Lu H, Wu H, Du L. Pharmacokinetics of puerarin and ginsenoside Rg1 of CBN injection and the relation with platelet aggregation in rats. Am J Chin Med 2006;34:1037-45. Go to original source... Go to PubMed...
    12. Zhang S, Ji G, Liu J. Reversal of chemical-induced liver fibrosis in Wistar rats by puerarin. J Nutr Biochem 2006;17:485-91. Go to original source... Go to PubMed...
    13. Nakamura K, Nishihata T, Jin JS, Ma CM, Komatsu K, Iwashima M, Hattori M. The C-glucosyl bond of puerarin was cleaved hydrolytically by a human intestinal bacterium strain PUE to yield its aglycone daidzein and an intact glucose. Chem Pharm Bull (Tokyo) 2011;59:23-7. Go to original source... Go to PubMed...
    14. Lv Y, Hughes TC, Hao X, Mei D, Tan T. Preparation of monomeric and polymeric beta-cyclodextrin functionalized monoliths for rapid isolation and purification of puerarin from Radix puerariae. J Sep Sci 2011; doi: 10.1002/jssc.201100282 Go to original source...
    15. Luo CF, Yuan M, Chen MS, Liu SM, Zhu L, Huang BY, Liu XW, Xiong W. Pharmacokinetics, tissue distribution and relative bioavailability of puerarin solid lipid nanoparticles following oral administration. Int J Pharm 2011;410:138-44. Go to original source... Go to PubMed...
    16. Dong P, Ma CJ, Wendusu B, Wang B, Han XM, Wang Y, Song MD, Du GE. [Effects of Eerdun-wurile in a Rabbit Model of Atherosclerosis]. Chinese Archives of Traditional Chinese Medicine 2011;28:1012-5.
    17. Tavridou A, Efthimiadis A, Efthimiadis I, Manolopoulos VG. Simvastatin-induced changes in circulating oxidized low-density lipoprotein in different types of dyslipidemia. Heart Vessels 2010;25:288-93. Go to original source... Go to PubMed...
    18. Feaver RE, Gelfand BD, Wang C, Schwartz MA, Blackman BR. Atheroprone hemodynamic regulates fibronectin deposition to create positive feedback that sustains endothelial inflammation. Circ Res 2010;106:1703-11. Go to original source... Go to PubMed...
    19. Dzau VJ, Braun-Dullaeus RC, Sedding DG. Vascular Proliferation and Atherosclerosis: New Perspectives and Therapeutic Strategies. Nat Med 2002;8:1249-56. Go to original source... Go to PubMed...
    20. Kappert K, Sparwel J, Sandin A, Seiler A, Siebolts U, Leppänen O, Rosenkranz S, Ostman A. Cultured VSMCs and in Restenosis Antioxidants Relieve Phosphates Inhibition and Reduce PDGF Signaling in Cultured VSMCs and in Restenosis. Arterioscler Thromb Vasc Biol 2006;26:2644-51. Go to original source... Go to PubMed...
    21. Brown XQ, Bartolak-Suki E, Williams C, Walker ML, Weaver VM, Wong JY. Effect of substrate stiffness and PDGF on the behavior of vascular smooth muscle cells: implications for atherosclerosis. J. Cell Physiol 2010;225:115-22. Go to original source... Go to PubMed...
    22. Li L, Blumenthal DK, Terry CM, He Y, Carlson ML, Cheung AK. PDGF-Induced Proliferation in Human Arterial and Venous Smooth Muscle Cells: Molecular Basis for Differential Effects of PDGF Isoforms. J Cell Biochem 2011;112:289-98. Go to original source... Go to PubMed...

    Return to the content