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The TICE Pathway: Mechanisms and Lipid-Lowering Therapies

机译:TICE途径:机制和降脂疗法

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摘要

Besides the well-known hepatobiliary pathway of cholesterol excretion into the feces, transintestinal cholesterol excretion (TICE) is a second major pathway through which cholesterol is disposed from the body. In the process of TICE, cholesterol is taken up from lipoprotein particles at the basolateral side of the enterocyte and translocates towards the apical side of the enterocyte. At the apical side, the ATP-binding cassette transporters G5 and G8 form a heterodimer that transports cholesterol into the intestinal lumen. A substantial amount of the secreted cholesterol is likely reabsorbed by the cholesterol influx transporter Niemann-Pick C1-Like 1 (NPC1L1) since recent data indicate that inhibition of NPC1L1 increases the efficacy of TICE for disposal of cholesterol via the feces. The pathways and proteins involved in intracellular cholesterol trafficking in the enterocyte have not yet been identified. Therefore, in addition to discussing known mediators of TICE, this review will also examine potential candidates involved in cholesterol translocation in the enterocyte. Both the cholesterol reuptake and efflux pathways can be influenced by pharmaceutical means; thus, the TICE pathway is a very attractive target to increase cholesterol excretion from the body and prevent or mitigate atherosclerotic cardiovascular disease.
机译:除了众所周知的胆固醇排泄到粪便的肝胆途径外,肠内胆固醇排泄(TICE)是胆固醇从体内分解出来的第二种主要途径。在TICE的过程中,胆固醇从肠上皮细胞基底外侧的脂蛋白颗粒中吸收,并向肠上皮细胞的顶侧转移。在顶端,ATP结合盒转运蛋白G5和G8形成异二聚体,将胆固醇转运到肠腔中。胆固醇流入转运蛋白Niemann-Pick C1-Like 1(NPC1L1)可能会大量吸收分泌的胆固醇,因为最近的数据表明,抑制NPC1L1可以提高TICE通过粪便处理胆固醇的功效。尚未确定肠细胞中细胞内胆固醇运输涉及的途径和蛋白质。因此,除了讨论TICE的已知介体外,本综述还将研究参与肠上皮细胞胆固醇转运的潜在候选物。胆固醇的再摄取和外排途径均可受药物影响。因此,TICE途径是增加人体胆固醇排泄并预防或减轻动脉粥样硬化性心血管疾病的极具吸引力的目标。

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