首页> 外国专利> Method of forcing the reverse transport of cholesterol from a body part to the liver while avoiding harmful disruptions of hepatic cholesterol homeostasis, and pharmaceutical compositions, and kit related thereto

Method of forcing the reverse transport of cholesterol from a body part to the liver while avoiding harmful disruptions of hepatic cholesterol homeostasis, and pharmaceutical compositions, and kit related thereto

机译:在避免有害地破坏肝胆固醇动态平衡的同时,迫使胆固醇从身体部分逆向转运至肝脏的方法,药物组合物和相关试剂盒

摘要

The present invention provides a pharmaceutical composition, kit, and method of forcing the reverse transport of cholesterol from peripheral tissues to the liver in vivo while controlling plasma LDL concentrations. The method includes the step of administering a therapeutically effective amount of a multiplicity of large liposomes comprised of phospholipids substantially free of sterol for a treatment period. The method optionally includes the step of periodically assaying plasma LDL concentrations with an assay during the treatment period to assess plasma atherogenic lipoprotein concentrations and obtain an atherogenic lipoprotein profile, and adjusting the administration in response to said profile. The large liposomes are dimensioned larger than fenestrations of an endothelial layer lining hepatic sinusoids in the liver so that the liposomes are too large to readily penetrate the fenestrations. The therapeutically effective amounts are in the range of about 10 mg to about 1600 mg phospholipid per kg body weight per dose. A pharmaceutical composition and related kit for mobilizing peripheral cholesterol and sphingomyelin that enters the liver of a subject consisting essentially of liposomes of a size and shape larger than fenestrations of an endothelial layer lining hepatic sinusoids in the liver is also provided.
机译:本发明提供了在控制血浆LDL浓度的同时在体内迫使胆固醇从外周组织向肝脏反向转运的药物组合物,试剂盒和方法。该方法包括在治疗期间内给予治疗有效量的多种由基本上不含固醇的磷脂组成的大脂质体的步骤。所述方法任选地包括以下步骤:在治疗期间用测定法定期测定血浆LDL浓度,以评估血浆动脉粥样硬化脂蛋白浓度并获得动脉粥样硬化脂蛋白谱,并响应于所述谱调节给药。大脂质体的尺寸大于在肝中肝窦的衬里的内皮层的开窗孔的尺寸,因此脂质体太大而无法轻易穿透开窗孔。治疗有效量在每剂量每千克体重约10mg至约1600mg磷脂的范围内。还提供了一种药物组合物和相关试剂盒,该药物组合物和相关试剂盒用于动员进入受试者的肝脏的外周胆固醇和鞘磷脂,所述胆固醇基本上由脂质体组成,所述脂质体的大小和形状大于在肝脏中内衬肝窦的内皮层的窗孔。

著录项

  • 公开/公告号US2002071862A1

    专利类型

  • 公开/公告日2002-06-13

    原文格式PDF

  • 申请/专利权人 ESPERION LUV DEVELOPMENT INC.;

    申请/专利号US20020061503

  • 发明设计人 KEVIN JON WILLIAMS;

    申请日2002-01-31

  • 分类号A61K9/127;G01N33/53;C12Q1/60;

  • 国家 US

  • 入库时间 2022-08-22 00:52:35

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