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    Dimesna 16208-51-8

    簡要描述:Dimesna 16208-51-8
    Dimesna is an uroprotective agent used to decrease urotoxicity.

    • 產(chǎn)品型號:abs47027812
    • 廠商性質(zhì):生產(chǎn)廠家
    • 更新時間:2025-12-31
    • 訪  問  量:763

    詳細介紹

    品牌absinCAS16208-51-8
    分子式C4H8Na2O6S4純度98%
    分子量326.34貨號abs47027812
    規(guī)格100mg供貨周期現(xiàn)貨
    主要用途used to decrease urotoxicity.應用領域化工,生物產(chǎn)業(yè),農(nóng)林牧漁,制藥/生物制藥,綜合

    Dimesna 16208-51-8

    產(chǎn)品描述
    描述

    Dimesna is an uroprotective agent used to decrease urotoxicity.

    純度
    98%
    儲存/保存方法
    Store at -20℃ for one year(Powder);Store at 2-4℃ for two weeks;Store at -20℃ for six months after dissolution.
    基本信息
    別名
    地美si鈉;BNP-7787
    外觀
    白色粉末
    可溶性/溶解性
    DMSO :60 mg/mL (183.9 mM)

    Water :60 mg/mL (183.9 mM)
    生物活性
    In vitro(體外研究)
    Dimesna modulates paclitaxel-induced hyperpolymerization of MTP in a dose-dependent manner, and mesna, an in vivo metabolite of Dimesna, protects against time-dependent cisplatin-induced inactivation of MTP. Dimesna -mediated prevention or mitigation of cisplatin-induced nephrotoxicity may involve aminopeptidase N (APN) inhibition by certain Dimesna -derived esna-disulfide heteroconjugates and appears correlated to the presence of a glycinate moiety and/or an anionic group. Two general mechanisms for Dimesna -mediated nephroprotection of cisplatin-induced nephrotoxicity involving the gamma-glutamyl transpeptidase (GGT), APN and cysteine-conjugated-β-lyase (CCBL) nephrotoxigenic pathway are proposed which acting in a concerted and/or synergistic manner, and thereby prevent or mitigate cisplatin-induced renal toxicity. Mesna and its dimer, Dimesna, are coadministered for mitigation of ifosfamide- and cisplatin-induced toxicities, respectively. Dimesna is selectively reduced to mesna in the kidney, producing its protective effects. In vitro screens of uptake and efflux transporters reveal renal organic anion transporters OAT1, OAT3, and OAT4 are responsible for kidney-specific uptake of Dimesna. Uptake of Dimesna by OAT1, OAT3, and OAT4 is determined to be saturable with KM of 636 μM, 390 μM and 590 μM, respectively.
    In vivo(體內(nèi)研究)
    Tumors of urinary bladder induced by cyclophosphamide (CP) in rats can be significantly reduced by Dimesna administration in a dose-related manner.
    參考文獻
    參考文獻
    • 1. Parker AR, et al. Mol, Cancer Ther, 2010, 9(9), 2558-2567.

    • 2. Hausheer FH, et al. Cancer Chemother Pharmacol, 2010, 65(5), 941-951.

    研究領域
    研究領域
    Drug DiscoverySmall Molecule DrugLead Compound Discovery
    Dimesna 16208-51-8溫馨提示:本產(chǎn)品僅作科研實驗使用,不支持臨床等研究

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