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  • Desoxypeganine

    Desoxypeganine

    Desoxypeganine
    产品编号 CFN91939
    CAS编号 495-59-0
    分子式 = 分子量 C11H12N2 = 172.23
    产品纯度 >=98%
    物理属性 Powder
    化合物类型 Alkaloids
    植物来源 The herbs of Peganum harmala
    ChemFaces的产品在影响因子大于5的优秀和顶级科学期刊中被引用
    提供自定义包装
    产品名称 产品编号 CAS编号 包装 QQ客服
    Desoxypeganine CFN91939 495-59-0 1mg QQ客服:215959384
    Desoxypeganine CFN91939 495-59-0 5mg QQ客服:215959384
    Desoxypeganine CFN91939 495-59-0 10mg QQ客服:215959384
    Desoxypeganine CFN91939 495-59-0 20mg QQ客服:215959384
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    ChemFaces的产品在许多优秀和顶级科学期刊中被引用

    Cell. 2018 Jan 11;172(1-2):249-261.e12.
    doi: 10.1016/j.cell.2017.12.019.
    IF=36.216(2019)

    PMID: 29328914

    Cell Metab. 2020 Mar 3;31(3):534-548.e5.
    doi: 10.1016/j.cmet.2020.01.002.
    IF=22.415(2019)

    PMID: 32004475

    Mol Cell. 2017 Nov 16;68(4):673-685.e6.
    doi: 10.1016/j.molcel.2017.10.022.
    IF=14.548(2019)

    PMID: 29149595

    ACS Nano. 2018 Apr 24;12(4): 3385-3396.
    doi: 10.1021/acsnano.7b08969.
    IF=13.903(2019)

    PMID: 29553709

    Nature Plants. 2016 Dec 22;3: 16206.
    doi: 10.1038/nplants.2016.205.
    IF=13.297(2019)

    PMID: 28005066

    Sci Adv. 2018 Oct 24;4(10): eaat6994.
    doi: 10.1126/sciadv.aat6994.
    IF=12.804(2019)

    PMID: 30417089
    我们的产品现已经出口到下面的研究机构与大学,并且还在增涨
  • Siksha O Anusandhan University (India)
  • Uniwersytet Jagielloński w Krakowie (Poland)
  • University of Medicine and Pharmacy (Romania)
  • S.N.D.T. Women's University (India)
  • University of Illinois at Chicago (USA)
  • Universidade do Porto (Portugal)
  • Leibniz Institute of Plant Biochemistry (Germany)
  • University of Toronto (Canada)
  • Cancer Research Initatives Foundation(CARIF) (Malaysia)
  • Vin?a Institute of Nuclear Sciences (Serbia)
  • Florida International University (USA)
  • Istanbul University (Turkey)
  • University of Leipzig (Germany)
  • Melbourne University (Australia)
  • More...
  • 国外学术期刊发表的引用ChemFaces产品的部分文献
  • Horticulturae2024, 10(4), 382.
  • Applied Biological Chemistry2022, 65(85).
  • Universiti Tunku Aboul Rahman2023, 6263.
  • Front Microbiol.2022, 13:835463.
  • Antimicrob Agents Chemother.2020, AAC.01921-20.
  • PLoS One.2017, 12(3):e0173585
  • J Pharm Biomed Anal.2017, 140:274-280
  • Nutrients.2022, 14(19):4170.
  • Phytomedicine.2022, 100:154036.
  • Egyptian Pharmaceutical Journal2024, epj_205_23.
  • PLoS One.2020, 15(2):e0220084.
  • Nutr Res Pract.2023, 17(4):670-681.
  • Universidade Estadual Paulista2017, 11449
  • Sci Adv.2018, 4(10)
  • Crystals2020, 10(3), 206.
  • Cell Physiol Biochem.2019, 52(6):1255-1266
  • Sci Rep.2023, 13(1):21690.
  • Journal of Functional Foods2022, 98:105271.
  • Chinese Pharmacological Bulletin2019, 35(8):1120-1125
  • J Cell Biochem.2022, 123(7):1222-1236.
  • Phytochemistry Letters2017, 449-455
  • Yakugaku Zasshi.2018, 138(4):571-579
  • Molecules.2019, 24(6):E1177
  • ...
  • 生物活性
    Description: Desoxypeganine is a cholinesterase inhibitor, acting preferentially on butyrylcholinesterase, and as a selective inhibitor of monoamine oxidase A but not monoamine oxidase B.Desoxypeganine is being developed for its potential utility in the pharmacological treatment of alcohol abuse to reduce craving and depression in alcohol abusers, and might also be useful as a smoking cessation aid.
    Targets: MAO
    In vivo:
    Int J Clin Pharmacol Ther. 2009 Jul;47(7):483-90.
    Randomized, crossover, single-blind, placebo-controlled, human pharmacology clinical trial with desoxypeganine, a new cholinesterase and selective MAO-A inhibitor: multiple-dose pharmacokinetics.[Pubmed: 19640356]
    Desoxypeganine, a naturally occurring alkaloid, is being developed for its potential utility in the pharmacological treatment of alcohol abuse to reduce craving and depression in alcohol abusers, and might also be useful as a smoking cessation aid. During the preclinical development it was characterized as a cholinesterase inhibitor, acting preferentially on butyrylcholinesterase, and as a selective inhibitor of monoamine oxidase A but not monoamine oxidase B. The aim of the present human pharmacology clinical trial was to assess the oral bioavailability, pharmacokinetic profile and tolerability of Desoxypeganine, administered in a multiple-dose regimen to healthy volunteers.
    METHODS AND RESULTS:
    Eighteen healthy adult volunteers of both sexes received placebo, 50 mg and 100 mg Desoxypeganine (b.i.d. for 3 days) in a single-blind, crossover, randomized manner. Main pharmacokinetic parameters after single and multiple doses were estimated. Clinical tolerability and clinical laboratory safety, including effect on QTc interval, were assessed. Non-compartmental estimations of Cmax, AUC, tmax, t1/2 and MRT at 12-h intervals are given. No significant dose effect was observed in tmax, t1/2 and MRT. Cmax and AUC are approximately double with the dose of 100 mg comparing with the dose of 50 mg. A significant increase (p < 0.05) on Cmax and AUC was also obtained with the highest dose administered in comparison with the lowest one, revealing a slight but clinically insignificant accumulation. Steady state of drug concentration was reached in both genders during the study period. Plasma protein binding of Desoxypeganine amounted to approximately 18%. No severe adverse events were recorded and none of the subjects suffered from any adverse event that led to withdrawal from the study. Most frequently recorded adverse event was dizziness. No significant effects of Desoxypeganine on vital signs, laboratory parameters or QTc interval were observed.
    CONCLUSIONS:
    The present clinical trial describes the pharmacokinetic profile of two doses of Desoxypeganine, administered orally in multiple dose to healthy volunteers. The drug was well tolerated without any severe clinical, clinical laboratory, or ECG adverse events being recorded.
    Methods Find Exp Clin Pharmacol. 2008 Mar;30(2):141-7.
    Phase I clinical trial with desoxypeganine, a new cholinesterase and selective MAO-A inhibitor: tolerance and pharmacokinetics study of escalating single oral doses.[Pubmed: 18560630 ]
    Desoxypeganine (DOP) is a natural alkaloid that has been characterized as a cholinesterase inhibitor and a selective inhibitor of monoamine oxidase A. DOP has been investigated for its potential utility in the pharmacological treatment of alcohol abuse and as a smoking cessation aid. The aim of this clinical trial was to evaluate the tolerance and single-dose pharmacokinetic profile of DOP in healthy human volunteers.
    METHODS AND RESULTS:
    The study was an open-label, dose-escalation, phase I clinical trial involving the administration of increasing single oral doses of DOP (50, 100, 150 and 200 mg). The study was conducted according to the Declaration of Helsinki and Good Clinical Practice. Eighteen healthy adult volunteers (8 males and 10 females, age ranging 20-30 years) were recruited. DOP was administered sequentially, escalating in single doses of 50, 100, 150 and 200 mg in four experimental sessions with a washout period of at least 1 week between them. Progress to the next dose was allowed only if the previous dose was tolerated. Pharmacokinetic parameters were determined using noncompartmental methods. Clinical and analytical safety was assessed throughout the study, and QTc intervals were measured at regular intervals. The main pharmacokinetic parameters and renal excretion are described. No serious adverse events were registered, and none of the subjects discontinued the study because of lack of tolerance. All the adverse events recorded were mild to moderate and increased with the dose. The ECG measurements revealed that even at a higher dose, the QTc interval remained below the safety threshold.
    CONCLUSIONS:
    In summary, this first phase I study indicates that DOP has linear and dose-proportional pharmacokinetics, satisfactory oral bioavailability and plasma half-life and renal excretion. Also, DOP has shown an adequate safety profile that allows the continuation of clinical development.
    制备储备液(仅供参考)
    1 mg 5 mg 10 mg 20 mg 25 mg
    1 mM 5.8062 mL 29.0309 mL 58.0619 mL 116.1238 mL 145.1547 mL
    5 mM 1.1612 mL 5.8062 mL 11.6124 mL 23.2248 mL 29.0309 mL
    10 mM 0.5806 mL 2.9031 mL 5.8062 mL 11.6124 mL 14.5155 mL
    50 mM 0.1161 mL 0.5806 mL 1.1612 mL 2.3225 mL 2.9031 mL
    100 mM 0.0581 mL 0.2903 mL 0.5806 mL 1.1612 mL 1.4515 mL
    * Note: If you are in the process of experiment, it's need to make the dilution ratios of the samples. The dilution data of the sheet for your reference. Normally, it's can get a better solubility within lower of Concentrations.
    部分图片展示
    产品名称 产品编号 CAS编号 分子式 = 分子量 位单 联系QQ
    常山乙素; Febrifugine CFN92302 24159-07-7 C16H19N3O3 = 301.3 20mg QQ客服:3257982914
    异常山乙素; Isofebrifugine CFN92303 32434-44-9 C16H19N3O3 = 301.3 20mg QQ客服:2056216494
    Desoxypeganine; Desoxypeganine CFN91939 495-59-0 C11H12N2 = 172.23 5mg QQ客服:2159513211
    骆驼蓬碱; Vasicine CFN97052 6159-55-3 C11H12N2O = 188.2 10mg QQ客服:3257982914
    鸭嘴花酚碱; Vasicinol CFN99009 5081-51-6 C11H12N2O2 = 204.2 5mg QQ客服:2056216494
    脱氧鸭嘴花碱酮; Deoxyvasicinone CFN98882 530-53-0 C11H10N2O = 186.2 5mg QQ客服:2159513211
    鸭嘴花碱酮; Vasicinone CFN98773 486-64-6 C11H10N2O2 = 202.2 5mg QQ客服:2159513211
    鸭嘴花碱酮; Vasicinolone CFN97406 84847-50-7 C11H10N2O3 = 218.2 5mg QQ客服:1413575084
    薏苡素; Coixol CFN98889 532-91-2 C8H7NO3 = 165.1 20mg QQ客服:2056216494
    2,7-二羟基-2H-1,4-苯并嗪-3(4H)-酮; 2,7-Dihydroxy-2H-1,4-benzoxazin-3(4H)-one CFN97184 69804-59-7 C8H7NO4 = 181.1 5mg QQ客服:1413575084

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