Understanding the Liver’s Role in the Clearance of Aβ40

Livers Pub Date : 2024-05-23 DOI:10.3390/livers4020018
Glen P. Lockwood, Nicholas J. Hunt, M. Kockx, Sun Woo Sophie Kang, D. L. Le Couteur, V. Cogger
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Abstract

The clearance of peripheral beta amyloid (Aβ) is a potential target for the treatment of Alzheimer’s disease (AD). The liver has been implicated in the elimination of Aβ from the peripheral circulation. Here, the single-pass uptake of Aβ40 in perfused livers from young and old rats (6 to 10 rats per group) was investigated with the multiple indicator dilution technique. Aβ40 had volumes of distribution between those of the vascular marker Evans Blue and the extracellular marker sucrose. The hepatic extraction of Aβ40 was negligible, explained in part by the small permeability surface area products consistent with a high endothelial barrier to liver uptake. There were no substantial effects of age on any of these results. In vitro experiments with isolated hepatocytes and liver sinusoidal endothelial cells showed only very small amounts of Aβ uptake consistent with low intrinsic clearance. These results indicate that the hepatic clearance of Aβ is capacity-limited, explained by the low-permeability surface area products and hepatocyte uptake. However, this does not preclude an effect of aging in longer-term in vivo studies where age-related changes in liver blood flow and protein binding influence liver clearance.
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了解肝脏在清除 Aβ40 中的作用
清除外周β淀粉样蛋白(Aβ)是治疗阿尔茨海默病(AD)的一个潜在靶点。肝脏参与了外周循环中 Aβ 的清除。在此,我们采用多指标稀释技术研究了年轻和年老大鼠(每组 6 至 10 只)灌注肝脏对 Aβ40 的单次吸收。Aβ40 的分布体积介于血管标记物埃文斯蓝和细胞外标记物蔗糖之间。肝脏对 Aβ40 的萃取可以忽略不计,部分原因是渗透性表面积较小,这与内皮对肝脏摄取的高屏障一致。年龄对上述结果没有实质性影响。用离体肝细胞和肝窦内皮细胞进行的体外实验显示,只有极少量的 Aβ 被吸收,这与低内在清除率一致。这些结果表明,肝脏对 Aβ 的清除能力是有限的,这可以从低渗透表面积产物和肝细胞摄取得到解释。不过,这并不排除长期体内研究中衰老的影响,因为肝脏血流和蛋白质结合中与年龄相关的变化会影响肝脏的清除率。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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