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  • 人参皂苷Rf

    Ginsenoside Rf

    人参皂苷Rf
    产品编号 CFN99976
    CAS编号 52286-58-5
    分子式 = 分子量 C42H72O14 = 801.01
    产品纯度 >=98%
    物理属性 Powder
    化合物类型 Triterpenoids
    植物来源 The roots of Panax ginseng C. A. Mey.
    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
    人参皂苷Rf CFN99976 52286-58-5 10mg QQ客服:215959384
    人参皂苷Rf CFN99976 52286-58-5 20mg QQ客服:215959384
    人参皂苷Rf CFN99976 52286-58-5 50mg QQ客服:215959384
    人参皂苷Rf CFN99976 52286-58-5 100mg 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
  • Imperial College London (United Kingdom)
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  • Macau University of Science and Technology (China)
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  • 国外学术期刊发表的引用ChemFaces产品的部分文献
  • Int J Mol Sci.2022, 23(5):2796.
  • Int J Mol Sci.2019, 20(3):E651
  • Legume Science2021, 3(4): e101.
  • LWT-Food Sci Technol2020, 109163
  • Sci Rep.2023, 13(1):21690.
  • Viruses.2017, 9(10)
  • J Adv Res.2021, 35:245-257.
  • Geroscience.2024, 01207-y.
  • Biochemistry.2018, 57(40):5886-5896
  • Life Sci.2022, 298:120488.
  • J Pain Res.2022, 15:3469-3478.
  • Bio-protocol2018, 9(14):e3301
  • Appl. Sci.2022, 12(17), 8646.
  • J Biochem Mol Toxicol.2022, e23211.
  • Chin J Pharm Anal.2019, 39(7):1217-1228
  • Biomed Pharmacother.2019, 111:262-269
  • Molecules.2021, 26(12):3652.
  • Sci Rep.2016, 6:25094
  • Pest Manag Sci.2019, 75(9):2530-2541
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  • Pharmaceuticals (Basel).2024, 17(1):108.
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  • ...
  • 生物活性
    Description: Ginsenoside Rf is a trace component of ginseng root, which has antinociception, analgesia, anti-inflammatory, and anti-cancer activities, it induces G2/Mphase cell cycle arrest and apoptosis in human osteosarcoma MG-63 cells through the mitochondrial pathway. Rf can act through a novel G protein-linked receptor in the nervous system by inhibiting N-type Ca2+ channel. Rf significantly reduces the production of IL-1β, IL-6, TNF-α, NO, and ROS, and suppresses TNF-α/LPS-induced NF-κB transcriptional activity.
    Targets: Bcl-2/Bax | CDK | Caspase | TNF-α | NO | ROS | IL Receptor | NF-kB | P450 (e.g. CYP17) | GABA Receptor | Calcium Channel
    In vitro:
    Oncol Rep. 2014 Jan;31(1):305-13.
    Induction of G2/M phase cell cycle arrest and apoptosis by ginsenoside Rf in human osteosarcoma MG‑63 cells through the mitochondrial pathway.[Pubmed: 24173574]
    Ginsenosides, extracted from the traditional Chinese herb ginseng, are a series of novel natural anticancer products known for their favorable safety and efficacy profiles. The present study aimed to investigate the cytotoxicity of ginsenoside Rf to human osteosarcoma cells and to explore the anticancer molecular mechanisms of ginsenoside Rf.
    METHODS AND RESULTS:
    Five human osteosarcoma cell lines (MG-63, OS732, U-2OS, HOS and SAOS-2) were employed to investigate the cytotoxicity of ginsenoside Rf by MTT and colony forming assays. After treatment with ginsenoside Rf, MG-63 cells which were the most sensitive to ginsenoside Rf, were subjected to flow cytometry to detect cell cycle distribution and apoptosis, and nuclear morphological changes were visualized by Hoechst 33258 staining. Caspase-3, -8 and -9 activities were also evaluated. The expression of cell cycle markers including cyclin B1 and Cdk1 was detected by RT-PCR and western blotting. The expression of apoptotic genes Bcl-2 and Bax and the release of cytochrome c were also examined by western blotting. Change in the mitochondrial membrane potential was observed by JC-1 staining in situ. Our results demonstrated that the cytotoxicity of ginsenoside Rf to these human osteosarcoma cell lines was dose-dependent, and the MG-63 cells were the most sensitive to exposure to ginsenoside Rf. Additionally, ginsenoside Rf induced G2/M phase cell cycle arrest and apoptosis in MG-63 cells. Furthermore, we observed upregulation of Bax and downregulation of Bcl-2, Cdk1 and cyclin B1, the activation of caspase-3 and -9 and the release of cytochrome c in MG-63 cells following treatment with ginsenoside Rf.
    CONCLUSIONS:
    Our findings demonstrated that ginsenoside Rf induces G2/M phase cell cycle arrest and apoptosis in human osteosarcoma MG-63 cells through the mitochondrial pathway, suggesting that ginsenoside Rf, as an effective natural product, may have a therapeutic effect on human osteosarcoma.
    Mol Pharmacol. 2002 Apr;61(4):928-35.
    Functional expression of a novel ginsenoside Rf binding protein from rat brain mRNA in Xenopus laevis oocytes.[Pubmed: 11901233]
    We have shown that ginsenoside Rf (Rf) regulates voltage-dependent Ca(2+) channels through pertussis toxin (PTX)-sensitive G proteins in rat sensory neurons.
    METHODS AND RESULTS:
    These results suggest that Rf can act through a novel G protein-linked receptor in the nervous system. In the present study, we further examined the effect of Rf on G protein-coupled inwardly rectifying K(+) (GIRK) channels after coexpression with size-fractionated rat brain mRNA and GIRK1 and GIRK4 (GIRK1/4) channel cRNAs in Xenopus laevis oocytes using two-electrode voltage-clamp techniques. We found that Rf activated GIRK channel in a dose-dependent and reversible manner after coexpression with subfractions of rat brain mRNA and GIRK1/4 channel cRNAs. This Rf-evoked current was blocked by Ba(2+), a potassium channel blocker. The size of rat brain mRNA responding to Rf was about 6 to 7 kilobases. However, Rf did not evoke GIRK current after injection with this subfraction of rat brain mRNA or GIRK1/4 channel cRNAs alone. Other ginsenosides, such as Rb(1) and Rg(1), evoked only slight induction of GIRK currents after coexpression with the subfraction of rat brain mRNA and GIRK1/4 channel cRNAs. Acetylcholine and serotonin almost did not induce GIRK currents after coexpression with the subfraction of rat brain mRNA and GIRK1/4 channel cRNAs. Rf-evoked GIRK currents were not altered by PTX pretreatment but were suppressed by intracellularly injected guanosine-5'-(2-O-thio) diphosphate, a nonhydrolyzable GDP analog.
    CONCLUSIONS:
    These results indicate that Rf activates GIRK channel through an unidentified G protein-coupled receptor in rat brain and that this receptor can be cloned by the expression method demonstrated here.
    In vivo:
    Life Sci. 2003 Jan 3;72(7):759-68.
    Ginsenoside Rf potentiates U-50,488H-induced analgesia and inhibits tolerance to its analgesia in mice.[Pubmed: 12479975]
    In the present study, the effect of ginsenoside Rf (Rf), a trace component of Panax ginseng on U-50,488H (U50), a selective kappa opioid-induced analgesia and its tolerance to analgesia was studied using the mice tail-flick test. In addition, the possible mechanism by which Rf may affect U50-induced analgesia was investigated.
    METHODS AND RESULTS:
    Intraperitoneal administration of U50 (40 mg/kg) produced analgesia. Rf (10(-14)-10(-10) mg/kg) on co treatment dose-dependently potentiated the U50 (40 mg/kg)-induced analgesia. Rf (10(-12)-10(-2) mg/ml) did not alter the binding of [3H] naloxone, a opioid ligand and [3H]PN200-110, a dihydropyridine ligand to mice whole brain membrane. Twice daily administration of U50 (40 mg/kg) for six days induced tolerance to its analgesia. Chronic treatment (day 4-day 6) of Rf (10(-14)-10(-10) mg/kg) to U50-tolerant mice, dose-dependently inhibited the tolerance. The inhibition of tolerance to U50-induced analgesia by Rf was not altered by flumazenil (0.1 mg/kg), a benzodiazepine receptor antagonist and picrotoxin (1 mg/kg), a GABA(A)-gated chloride channel blocker on chronic treatment.
    CONCLUSIONS:
    In conclusion, these findings for the first time demonstrated that ginsenoside Rf potentiates U50-induced analgesia, inhibits tolerance to its analgesia, and suggests that Rf affects U50-induced analgesia via non-opioid, non-dihydropyridine-sensitive Ca(+2) and non-benzodiazepine-GABA(A)ergic mechanisms in mice.
    制备储备液(仅供参考)
    1 mg 5 mg 10 mg 20 mg 25 mg
    1 mM 1.2484 mL 6.2421 mL 12.4842 mL 24.9685 mL 31.2106 mL
    5 mM 0.2497 mL 1.2484 mL 2.4968 mL 4.9937 mL 6.2421 mL
    10 mM 0.1248 mL 0.6242 mL 1.2484 mL 2.4968 mL 3.1211 mL
    50 mM 0.025 mL 0.1248 mL 0.2497 mL 0.4994 mL 0.6242 mL
    100 mM 0.0125 mL 0.0624 mL 0.1248 mL 0.2497 mL 0.3121 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
    人参皂苷Rh1; Ginsenoside Rh1 CFN99970 63223-86-9 C36H62O9 = 638.88 20mg QQ客服:1413575084
    三七皂苷R2; Notoginsenoside R2 CFN92364 80418-25-3 C41H70O13 = 771.0 20mg QQ客服:3257982914
    20(R)-三七皂苷 R2; 20(R)-Notoginsenoside R2 CFN93373 948046-15-9 C41H70O13 = 771.0 5mg QQ客服:215959384
    三七皂苷T5; Notoginsenoside T5 CFN92824 769932-34-5 C41H68O12 = 753.0 5mg QQ客服:3257982914
    人参皂苷Rg2; Ginsenoside Rg2 CFN99968 52286-74-5 C42H72O13 = 785.02 20mg QQ客服:2056216494
    人参皂苷Rf; Ginsenoside Rf CFN99976 52286-58-5 C42H72O14 = 801.01 20mg QQ客服:2159513211
    20-葡萄糖人参皂苷R; 20-O-Glucoginsenoside Rf CFN95036 68406-27-9 C48H82O19 = 963.2 5mg QQ客服:1413575084
    (20R)-人参皂苷Rh1; (20R)-Ginsenoside Rh1 CFN92796 80952-71-2 C36H62O9 = 638.9 20mg QQ客服:3257982914
    20R-人参皂苷Rg2; 20R-Ginsenoside Rg2 CFN90412 80952-72-3 C42H72O13 = 785.02 20mg QQ客服:2159513211
    20(S)-原人参三醇; (20S)-Protopanaxatriol CFN90564 34080-08-5 C30H52O4 = 476.4 20mg QQ客服:2056216494

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