SIGMA 420875-1L 二氧化硅 制备 7631-86-9
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SIGMA 420875-1L 二氧化硅 制备 7631-8

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  • ¥463
  • Sigma-Aldrich
  • 进口
  • 420875-1L
  • 2025年08月28日
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    • 详细信息
    • 文献和实验
    • 技术资料
    • 保存条件

      常温

    • 保质期

      根据瓶身LOT号查询

    • 英文名

      LUDOX® AM colloidal silica

    • 库存

      有现货

    • 供应商

      浙江羽翔生物科技有限公司

    • CAS号

      7631-86-9

    • 规格

      1L

    属性

    描述

    colloidal

    质量水平

    200

    表单

    liquid

    浓度

    30 wt. % suspension in H2O

    表面积

    198-250 m2/g

    pH值(酸碱度)

    8.6-9.3

    密度

    1.21 g/mL at 25 °C

    SMILES字符串

    O=[Si]=O

    InChI

    1S/O2Si/c1-3-2

    InChI key

    VYPSYNLAJGMNEJ-UHFFFAOYSA-N

    一般描述

    含有钠稳定反离子。

    LUDOX® AM胶态二氧化硅由更密集的硅结构组成,常用于制备聚苯胺分散体。

    应用

    LUDOX® AM胶体二氧化硅可作为硅质来源,用于合成:
    • NaX沸石,水热法。
    • 温石棉型Mg3Si2O5·(OH)4纳米管(MgSi-NTs)。

    它还可用作陶瓷浆料的粘合剂。

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    图标文献和实验
    该产品被引用文献

    Mucin-based stationary phases as tool for the characterization of drug-mucus interaction.

    Journal of chromatography. A (2014-06-05)
    Andrea F G Gargano, Michael Lämmerhofer, Hans Lönn, Peter J Schoenmakers, Tomas Leek
    PMID24894112
    摘要

    Mucin glycoproteins belong to a class of high molecular weight, heavy glycosylated, proteins that together with water, salts and lipids constitute mucous secretions. Particular disease states (e.g. obstructive chronic bronchitis and ovarian tumor) are known to modify the composition and the thickness of those barriers. Therefore, it is important to address whether the absorption of potential drug candidates to be administered is influenced by the presence of interaction with this class of proteins. Typically, the methods adopted to characterize drug-protein interaction are dialysis, ultrafiltration and gel filtration. Besides these, bio-affinity chromatographic methods have demonstrated to be valuable tools offering the advantageous characteristics such as simplicity, efficiency, high-throughput capability and robustness. The present contribution reports on the synthesis and analytical characterization of a new chromatographic stationary phase based on covalently immobilized mucin and explores the use of LC-UV affinity zonal chromatography as a tool to screen drugs for their affinity to mucin. A series of different binding chemistries for the covalent linkage of mucin to silica-based supports as well as distinct immobilization protocols (static and dynamic) have been evaluated in order to optimize surface coverage. Resultant stationary phases have been characterized chromatographically by studying the effect of mobile phase and analyte structure on the distribution and retention of test compounds. As conclusive study, we report the evaluation of the retention characteristics of 41 drug-like compounds (having heterogeneous chemical properties) for their interaction with this novel stationary phase.

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    SIGMA 420875-1L 二氧化硅 制备 7631-86-9
    ¥463