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首页> 外文期刊>Journal of Medicinal Chemistry >Development of Clickable Monophosphoryl Lipid A Derivatives toward Semisynthetic Conjugates with Tumor-Associated Carbohydrate Antigens
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Development of Clickable Monophosphoryl Lipid A Derivatives toward Semisynthetic Conjugates with Tumor-Associated Carbohydrate Antigens

机译:用肿瘤相关的碳水化合物抗原的半合成缀合物的可点击单磷虾脂质的开发衍生物

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摘要

A semisynthetic strategy to obtain monophosphoryl lipid A derivatives equipped with clickable (azide, alkyne, double bond, or thiol precursor) moieties, starting from the native lipid A isolated from Escherichia coli, is presented. These lipid A derivatives can be conjugated with other interesting biomolecules, such as tumor-associated carbohydrate antigens (TACAs). In this way, the immunostimulant activity of monophosphoryl lipid A can significantly improve the immunogenicity of TACAs, thus opening access to potential self-adjuvant anticancer vaccine candidates. A monophosphoryl lipid A-Thomson-Friedenreich (TF) antigen conjugate was obtained to demonstrate the feasibility of this methodology, which stands as a valuable, rapid, and scalable alternative to the highly complex approaches of total synthesis recently reported to the same aim. A preliminary evaluation of the immunological activity of this conjugate as well as of other semisynthetic lipid A derivatives was also reported.
机译:提出了一种半磷虾脂质的半合成策略,其呈现出从从大肠杆菌分离的天然脂质A开始的可点击(叠氮化物,炔烃,双键或硫醇前体)部分的衍生物。 这些脂质可以与其他有趣的生物分子缀合,例如肿瘤相关的碳水化合物抗原(TACA)。 以这种方式,单磷虾脂质A的免疫刺激活性可以显着改善淋巴的免疫原性,从而开口进入潜在的自助抗癌疫苗候选物。 获得单磷虾脂A-Thomson-Friedenreich(TF)抗原缀合物以证明该方法的可行性,它被视为有价值的,快速,可扩展的替代品,这是最近综合的总合成方法的高度复杂的方法。 还报道了对该缀合物的免疫活性以及其他半合成脂质衍生物的初步评价。

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  • 来源
    《Journal of Medicinal Chemistry 》 |2017年第23期| 共12页
  • 作者单位

    Univ Naples Federico II Complesso Univ Monte S Angelo Dept Chem Sci Via Cintia 4 I-80126 Naples Italy;

    Polish Acad Sci L Hirszfeld Inst Immunol &

    Expt Therapy Weigla 12 PL-53114 Wroclaw Poland;

    Univ Naples Federico II Complesso Univ Monte S Angelo Dept Chem Sci Via Cintia 4 I-80126 Naples Italy;

    Polish Acad Sci L Hirszfeld Inst Immunol &

    Expt Therapy Weigla 12 PL-53114 Wroclaw Poland;

    Univ Naples Federico II Complesso Univ Monte S Angelo Dept Chem Sci Via Cintia 4 I-80126 Naples Italy;

    Univ Naples Federico II Complesso Univ Monte S Angelo Dept Chem Sci Via Cintia 4 I-80126 Naples Italy;

    Polish Acad Sci L Hirszfeld Inst Immunol &

    Expt Therapy Weigla 12 PL-53114 Wroclaw Poland;

    Univ Naples Federico II Complesso Univ Monte S Angelo Dept Chem Sci Via Cintia 4 I-80126 Naples Italy;

    Univ Naples Federico II Complesso Univ Monte S Angelo Dept Chem Sci Via Cintia 4 I-80126 Naples Italy;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学 ;
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