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  • 草乌甲素

    Bulleyaconitine A

    草乌甲素
    产品编号 CFN99720
    CAS编号 107668-79-1
    分子式 = 分子量 C35H49NO10 = 643.8
    产品纯度 >=98%
    物理属性 Powder
    化合物类型 Alkaloids
    植物来源 The roots of Aconitum kusnenzoffii Reichb.
    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
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    产品名称 产品编号 CAS编号 包装 QQ客服
    草乌甲素 CFN99720 107668-79-1 10mg QQ客服:2056216494
    草乌甲素 CFN99720 107668-79-1 20mg QQ客服:2056216494
    草乌甲素 CFN99720 107668-79-1 50mg QQ客服:2056216494
    草乌甲素 CFN99720 107668-79-1 100mg QQ客服:2056216494
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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
  • Subang Jaya Medical Centre (Malaysia)
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  • University of Helsinki (Finland)
  • University of Malaya (Malaysia)
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  • John Innes Centre (United Kingdom)
  • University of Queensland (Australia)
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  • Korea Food Research Institute(KFRI) (Korea)
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  • 国外学术期刊发表的引用ChemFaces产品的部分文献
  • Sains Malaysiana2022, 51(4):1143-1154
  • Food Chem.2017, 221:1135-1144
  • J Ethnopharmacol.2020, 269:113752.
  • Acta horticulturae2017, 1158:257-268
  • Microchemical Journal2018, 137:168-173
  • Natural Product Communications2020, doi: 10.1177.
  • Geroscience.2024, 01207-y.
  • J Cell Mol Med.2023, jcmm.18071.
  • Integr Cancer Ther.2018, 17(3):832-843
  • Mol Neurobiol.2021, 58(8):3665-3676.
  • FEBS J.2022, 10.1111:febs.16676.
  • Biomolecules.2020, 10(2):E184
  • Molecules.2020, 25(21):5087.
  • Phytomedicine.2015, 22(11):1027-36
  • J Integr Plant Biol.2023, 13564.
  • Plant Foods Hum Nutr.2020, 10.1007
  • Cell Signal.2022, 99:110433.
  • Neurochem Int.2023, 167:105537.
  • Molecules.2019, 24(21):E3834
  • Molecules.2019, 24(12):E2286
  • Int J Mol Sci.2018, 19(2)
  • Asian J Beauty Cosmetol2021, 19(1): 57-64.
  • Exp Biol Med (Maywood).2019, 244(16):1463-1474
  • ...
  • 生物活性
    Description: Bulleyaconitine A is an analgesic and antiinflammatory drug, it has several potential targets, including voltage-gated Na+ channels. It displays long-acting local anesthetic properties in vitro and in vivo, it has been approved for the treatment of chronic pain and rheumatoid arthritis in China, it has the suppressive effect on some immune function of Balb/c mice.
    Targets: NO | Sodium Channel
    In vitro:
    Anesthesiology. 2007 Jul;107(1):82-90.
    Bulleyaconitine A isolated from aconitum plant displays long-acting local anesthetic properties in vitro and in vivo.[Pubmed: 17585219]
    Bulleyaconitine A (BLA) is an active ingredient of Aconitum bulleyanum plants. Bulleyaconitine A has been approved for the treatment of chronic pain and rheumatoid arthritis in China, but its underlying mechanism remains unclear.
    METHODS AND RESULTS:
    The authors examined (1) the effects of Bulleyaconitine A on neuronal voltage-gated Na channels in vitro under the whole cell patch clamp configuration and (2) the sensory and motor functions of rat sciatic nerve after single Bulleyaconitine A injections in vivo. Bulleyaconitine A at 10 microm did not affect neuronal Na currents in clonal GH3 cells when stimulated infrequently to +50 mV. When stimulated at 2 Hz for 1,000 pulses (+50 mV for 4 ms), Bulleyaconitine A reduced the peak Na currents by more than 90%. This use-dependent reduction of Na currents by Bulleyaconitine A reversed little after washing. Single injections of Bulleyaconitine A (0.2 ml at 0.375 mm) into the rat sciatic notch not only blocked sensory and motor functions of the sciatic nerve but also induced hyperexcitability, followed by sedation, arrhythmia, and respiratory distress. When Bulleyaconitine A at 0.375 mm was coinjected with 2% lidocaine (approximately 80 mm) or epinephrine (1:100,000) to reduce drug absorption by the bloodstream, the sensory and motor functions of the sciatic nerve remained fully blocked for approximately 4 h and regressed completely after approximately 7 h, with minimal systemic effects.
    CONCLUSIONS:
    Bulleyaconitine A reduces neuronal Na currents strongly at +50 mV in a use-dependent manner. When coinjected with lidocaine or epinephrine, Bulleyaconitine A elicits prolonged block of both motor and sensory functions in rats with minimal adverse effects.
    In vivo:
    Exp Neurol. 2015 Nov;273:263-72.
    Bulleyaconitine A depresses neuropathic pain and potentiation at C-fiber synapses in spinal dorsal horn induced by paclitaxel in rats.[Pubmed: 26376216 ]
    Paclitaxel, a widely used chemotherapeutic agent, often induces painful peripheral neuropathy and at present no effective drug is available for treatment of the serious side effect.
    METHODS AND RESULTS:
    Here, we tested if intragastrical application of Bulleyaconitine A (BLA), which has been approved for clinical treatment of chronic pain in China since 1985, could relieve the paclitaxel-induced neuropathic pain. A single dose of BLA attenuated the mechanical allodynia, thermal hyperalgesia induced by paclitaxel dose-dependently. Repetitive administration of the drug (0.4 and 0.8 mg/kg, t.i.d. for 7 d) during or after paclitaxel treatment produced a long-lasting inhibitory effect on thermal hyperalgesia, but not on mechanical allodynia. In consistency with the behavioral results, in vivo electrophysiological experiments revealed that spinal synaptic transmission mediated by C-fiber but not A fiber was potentiated, and the magnitude of long-term potentiation (LTP) at C-fiber synapses induced by the same high frequency stimulation was ~50% higher in paclitaxel-treated rats, compared to the naïve rats. Spinal or intravenous application of BLA depressed the spinal LTP, dose-dependently. Furthermore, patch clamp recordings in spinal cord slices revealed that the frequency but not amplitude of both spontaneous excitatory postsynaptic current (sEPSCs) and miniature excitatory postsynaptic currents (mEPSCs) in lamina II neurons was increased in paclitaxel-treated rats, and the superfusion of BLA reduced the frequency of sEPSCs and mEPSCs in paclitaxel-treated rats but not in naïve ones.
    CONCLUSIONS:
    Taken together, we provide novel evidence that BLA attenuates paclitaxel-induced neuropathic pain and that depression of spinal LTP at C-fiber synapses via inhibiting presynaptic transmitter release may contribute to the effect.
    Anesth Analg. 2008 Oct;107(4):1397-405.
    Use of bulleyaconitine A as an adjuvant for prolonged cutaneous analgesia in the rat.[Pubmed: 18806059]
    Bulleyaconitine A (BLA) is an analgesic and antiinflammatory drug isolated from Aconitum plants. BLA has several potential targets, including voltage-gated Na+ channels. We tested whether BLA elicited long-lasting cutaneous analgesia, when co-injected with lidocaine and epinephrine, as a model for prolonged infiltration anesthesia.
    METHODS AND RESULTS:
    The local anesthetic properties of BLA were assessed by the patch-clamp technique in HEK293t cells expressing Nav1.7 and Nav1.8 neuronal Na+ channels, both crucial for nociception. Drug solutions (0.6 mL) were injected subcutaneously via rat shaved dorsal skin. Inhibition of the cutaneous trunci muscle reflex was evaluated by pinpricks. Skin cross-sections were stained with hematoxylin and eosin or with antibodies against PGP9.5. BLA at 10 microM interacted minimally with resting or inactivated Nav1.7 and Nav1.8 Na+ channels when infrequently stimulated to +50 mV for 3 ms. However, when stimulated at 2 Hz for 1000 pulses, their peak Na+ currents were >90% reduced by BLA. This use-dependent inhibition was not significantly reversed after 15-min washing. Complete nociceptive blockade after injection of lidocaine (0.5%)/epinephrine (1:200,000) lasted for approximately 1 h in rats; full recovery occurred after approximately 6 h. Co-injection of 0.125 mM BLA with lidocaine/epinephrine increased the duration of complete nociceptive blockade to 24 h. Full recovery occurred after approximately 6 days. Skin histology including peripheral nerve fibers appeared unaffected by BLA.
    CONCLUSIONS:
    BLA inhibits Nav1.7 and Nav1.8 Na+ currents in a use-dependent manner. Co-injection of BLA at
    制备储备液(仅供参考)
    1 mg 5 mg 10 mg 20 mg 25 mg
    1 mM 1.5533 mL 7.7664 mL 15.5328 mL 31.0655 mL 38.8319 mL
    5 mM 0.3107 mL 1.5533 mL 3.1066 mL 6.2131 mL 7.7664 mL
    10 mM 0.1553 mL 0.7766 mL 1.5533 mL 3.1066 mL 3.8832 mL
    50 mM 0.0311 mL 0.1553 mL 0.3107 mL 0.6213 mL 0.7766 mL
    100 mM 0.0155 mL 0.0777 mL 0.1553 mL 0.3107 mL 0.3883 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
    雪上一枝蒿甲素; Bullatine A CFN90228 1354-84-3 C22H33NO2 = 343.51 20mg QQ客服:1457312923
    多根乌头碱; Karacoline CFN93074 39089-30-0 C22H35NO4 = 377.52 10mg QQ客服:2056216494
    关附甲素; Guan-fu base A CFN91495 1394-48-5 C24H31NO6 = 429.5 5mg QQ客服:2056216494
    翠雀花定; Delgrandine CFN89550 145237-05-4 C41H43NO12 = 741.77 5mg QQ客服:2056216494
    14-Dehydrodelcosine; 14-Dehydrodelcosine CFN89547 1361-18-8 C24H37NO7 = 451.55 5mg QQ客服:1457312923
    8-去乙酰基滇乌碱; Acoforestinine CFN99502 110011-77-3 C35H51NO10 = 645.79 20mg QQ客服:1457312923
    8-去乙酰滇乌碱; 8-Deacetylyunaconitine CFN89329 93460-55-0 C33H47NO10 = 617.73 5mg QQ客服:1413575084
    滇乌头碱; Yunaconitine CFN99503 70578-24-4 C35H49NO11 = 659.77 20mg QQ客服:3257982914
    3-乙酰滇乌碱; 3-Acetylyunaconitine CFN89362 80787-51-5 C37H51NO12 = 701.80 5mg QQ客服:1457312923
    草乌甲素; Bulleyaconitine A CFN99720 107668-79-1 C35H49NO10 = 643.8 20mg QQ客服:1457312923

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