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Annexin 2–caveolin 1 complex is a target of ezetimibe and regulates intestinal cholesterol transport

机译:Annexin 2–caveolin 1复合物是依泽替米贝的靶标,并调节肠道胆固醇的运输

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摘要

Modulation of cholesterol absorption in the intestine, the primary site of dietary cholesterol uptake in humans, can have profound clinical implications. We have undertaken a reverse genetic approach by disrupting putative cholesterol processing genes in zebrafish larvae by using morpholino (MO) antisense oligonucleotides. By using targeted MO injections and immunoprecipitation (IP) experiments coupled with mass spectrometry, we determined that annexin (ANX)2 complexes with caveolin (CAV)1 in the zebrafish and mouse intestine. The complex is heat stable and unaffected by SDS or reducing conditions. MO targeting of anx2b or cav1, which are both strongly expressed in the larval and adult zebrafish intestinal epithelium, prevents formation of the protein heterocomplex. Furthermore, anx2b MO injection prevents processing of a fluorescent cholesterol reporter and results in reduced sterol mass. Pharmacological treatment of mice with ezetimibe disrupts the heterocomplex in only hypercholesterolemic animals. These data suggest that ANX2 and CAV1 are components of an intestinal sterol transport complex.
机译:肠道中胆固醇的吸收的调节是人类饮食中胆固醇摄入的主要场所,可能具有深远的临床意义。我们通过使用吗啉代(MO)反义寡核苷酸破坏了斑马鱼幼虫中假定的胆固醇加工基因而采取了反向遗传方法。通过使用针对性的MO注射和免疫沉淀(IP)实验与质谱相结合,我们确定斑马鱼和小鼠肠道中膜联蛋白(ANX)2与小窝蛋白(CAV)1形成复合物。该配合物是热稳定的,不受SDS或还原条件的影响。 MO对anx2b或cav1的靶向作用,在幼虫和成年斑马鱼的肠上皮细胞中均强烈表达,可防止蛋白质异源复合物的形成。此外,anx2b MO注射会阻止荧光胆固醇报道分子的加工并导致固醇质量降低。依泽替米贝对小鼠的药理治疗仅会破坏高胆固醇血症动物的异源复合体。这些数据表明,ANX2和CAV1是肠道固醇转运复合物的组成部分。

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