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Article Navigation >  Journal of Pharmaceutical Practice and Service  > 2011  >  29(3): 193-196

ZHOU Yu, HU Li-na, LUO Jian-fei, YU Shi-chong, WU Qiu-ye. Synthesis and PTP1B activity of enzyme inhibition of mangiferin derivates[J]. Journal of Pharmaceutical Practice and Service, 2011, 29(3): 193-196.
Citation: ZHOU Yu, HU Li-na, LUO Jian-fei, YU Shi-chong, WU Qiu-ye. Synthesis and PTP1B activity of enzyme inhibition of mangiferin derivates[J]. Journal of Pharmaceutical Practice and Service, 2011, 29(3): 193-196.
shu

Synthesis and PTP1B activity of enzyme inhibition of mangiferin derivates

  • 1.

    NO. 82 Hospital of PLA, Huaian 223001,China

  • 2.

    Department of Organic Chemistry,School of Pharmacy,Second Military Medical University,Shanghai 200433,China

  • Received Date: 2011-01-06
  • Rev Recd Date: 2011-03-10
  • Objective To synthetize and conduct PTP1B inhibitory activity experiment of series of novel mangiferin derivates. Methods Different benzyl groups were introduced to mangiferin framework by nucleophilic substitution reaction. All the compounds were screened against protein tyrosine phosphatase 1B(PTP1B)with the colorimetrie assay. Results Eight compounds were synthesized and all the compounds exhibited PTP1B inhibitory activity to some extent. Conclusions Derivates of mangiferin remarkably enhanced the activity compared with mangiferin itself. In addition, the benzylated derivates with chloro atom had better inhibitory activity than other substitution groups. Furthermore,the para position of the benzyl was a better place for introducing substituent than meta and ortho position.
  • [1] Pardo-Andreu GL, Rene D, Alberto J, et al. Mangifera indica L, extract (Vimang) inhibits 2-deoxyribose damage induced by Fe (Ⅲ) plus ascorbate[J].Phytother Res, 2006, 20(2):120.
    [2] 彭志刚,罗 军,赖永熔,等.芒果苷对K562胞端粒酶活性和细胞周期的影响[J].中药药理与临床,2007, 23(1): 13.
    [3] Rivera DG, Balmaseda IH, Leon AA, et al. Anti-allergic properties of Manglfera indica L. extract (Vimang) and contribution of its glueosylxanthone mangiferin[J]. J Pham Pharmacol, 2006, 58(3): 385.
    [4] Gottlieb M, Leal-Campanario R, Campos-Esparza MR, et al. Neuroprotection by two polyphenols following excitotoxicity and experimental ischemia[J]. Neurobiology of Disease, 2006, 23(2): 374.
    [5] Hu HG, Liao HL, Zhang J, et al. First identification of xanthone sulfonamides as potent acyl-CoA: cholesterol acyltransferase (ACAT) inhibitors[J]. Bioorg Med Chem Lett, 2010, 20(10): 3094.
    [6] Miura T, Ichiki H, Iwamoto N, et al. Antidiabetic activity of the rhizoma of Anemarrhena asphodeloides and active components, mangiferin and its glucoside[J]. Biol Pharm Bull, 2001, 24(9): 1009.
    [7] Miura T, Ichiki H, Hashimoto I, et al. Antidiabetic activity of a xanthone compound, mangiferin[J]. Phytomedicine, 2001, 8(2): 85.
    [8] Pei Z, Liu G, Lubben TH, et al. Inhibition of protein tyrosine phosphatase 1B as a potential treatment of diabetes and obesity[J]. Curr Pharm Des, 2004, 10(28): 3481.
    [9] Dadke S, Chernoff J. Protein-tyrosine phosphatase 1B as a potential drug target for obesity[J]. Curr Drug Targets Immune Endocr Metabol Disord, 2003, 3(4): 299.
    [10] Kim HO, Blaskovich MA. Recent discovery and development of protein tyrosine phosphatase inhibitors[J]. Expert Opin Ther Patents, 2002, 12(6): 871.
    [11] Elchebly M, Payette P, Michaliszyn E, et al. Increased insulin sensitivity and obesity resistance in mice lacking the protein tyrosine phosphatase-1B gene[J]. Science, 1999, 283(5407): 1544.
    [12] Klaman LD, Boss O, Peroni OD, et al. Increased energy expenditure, decreased adiposity, and tissue-specific insulin sensitivity in protein-tyrosine phosphatase 1B-deficient mice[J]. Mol Cell Biol, 2000, 20(15): 5479.
    [13] 廖洪利,陈 军,杨 倩.芒果苷衍生物的制备[J].药学实践杂志,2010, 27(5): 49.
    [14] Goldstein BJ, Bittner-Kowalezyk A, White MF, et al. Tyrosine dephosphorylation and deactivation of insulin receptor substrate-1 by protein-tyrosine phosphatase 1B: Possible facilitation by the formation of a ternary complex with the GRB2 adaptor protein[J]. J Biol Chem, 2000, 275: 4283.
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Synthesis and PTP1B activity of enzyme inhibition of mangiferin derivates

  • 1. NO. 82 Hospital of PLA, Huaian 223001,China
  • 2. Department of Organic Chemistry,School of Pharmacy,Second Military Medical University,Shanghai 200433,China
  • Received Date: 2011-01-06
  • Rev Recd Date: 2011-03-10

Abstract: Objective To synthetize and conduct PTP1B inhibitory activity experiment of series of novel mangiferin derivates. Methods Different benzyl groups were introduced to mangiferin framework by nucleophilic substitution reaction. All the compounds were screened against protein tyrosine phosphatase 1B(PTP1B)with the colorimetrie assay. Results Eight compounds were synthesized and all the compounds exhibited PTP1B inhibitory activity to some extent. Conclusions Derivates of mangiferin remarkably enhanced the activity compared with mangiferin itself. In addition, the benzylated derivates with chloro atom had better inhibitory activity than other substitution groups. Furthermore,the para position of the benzyl was a better place for introducing substituent than meta and ortho position.

ZHOU Yu, HU Li-na, LUO Jian-fei, YU Shi-chong, WU Qiu-ye. Synthesis and PTP1B activity of enzyme inhibition of mangiferin derivates[J]. Journal of Pharmaceutical Practice and Service, 2011, 29(3): 193-196.
Citation: ZHOU Yu, HU Li-na, LUO Jian-fei, YU Shi-chong, WU Qiu-ye. Synthesis and PTP1B activity of enzyme inhibition of mangiferin derivates[J]. Journal of Pharmaceutical Practice and Service, 2011, 29(3): 193-196.
shu

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