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胆汁色素的体外渗透性和代谢稳定性以及胆红素亲水性和亲脂性修饰的影响。

In vitro permeability and metabolic stability of bile pigments and the effects of hydrophilic and lipophilic modification of biliverdin.

作者信息

Bulmer Andrew C, Blanchfield Joanne T, Coombes Jeff S, Toth Istvan

机构信息

School of Human Movement Studies, Blair Drive, University of Queensland, St. Lucia, Qld, 4067, Australia.

出版信息

Bioorg Med Chem. 2008 Apr 1;16(7):3616-25. doi: 10.1016/j.bmc.2008.02.008. Epub 2008 Feb 8.

Abstract

Bile pigments, including bilirubin and biliverdin are tetrapyrrolic, dicarboxylic acids capable of forming conjugates at their propionic acid groups via ester or amide bonds. They possess substantial antioxidant and anti-mutagenic activities and therefore their intestinal absorption might influence the development of cardiovascular disease and cancer. The aim of this study was to investigate whether altering the physico-chemical properties of bile pigments would improve their permeability in an in vitro assay of absorption. Native and synthetically modified bile pigments were tested for gastrointestinal permeability and metabolic stability using the Caco-2 cell line. In addition, a gross measure of their toxic effects was tested in a red blood cell co-incubation assay. The apparent permeability of unconjugated bilirubin (1), bilirubin ditaurate (2) and biliverdin (3) through Caco-2 cell monolayers was determined to be 10.4+/-1.2x10(-7), 35.2+/-3.4x10(-7) and 37.0+/-1.6x10(-7) cm/s (mean+/-SD), respectively, while biliverdin diglucosamine (4), and biliverdin dioctylamine (5) were impermeable. Unconjugated bilirubin, biliverdin, bilirubin ditaurate and biliverdin diglucosamine did not decompose when incubated in Caco-2 cell homogenates, whereas biliverdin dioctylamine decomposed over time. Only unconjugated bilirubin showed toxicity towards red blood cells (> or = 1000 microM), an effect that was abolished by the addition of 40 g/L serum albumin. The data presented here suggest that bile pigments are absorbed across the Caco-2 cell monolayer and that conjugation of biliverdin to hydrophilic or lipophilic moieties decreases their absorption and can reduce their metabolic stability. In summary, exogenous bilirubin and biliverdin supplements could be absorbed across the intestinal epithelium in vivo and potentially increase circulating concentrations of these antioxidant compounds.

摘要

胆汁色素,包括胆红素和胆绿素,是四吡咯二羧酸,能够通过酯键或酰胺键在其丙酸基团处形成共轭物。它们具有显著的抗氧化和抗诱变活性,因此其肠道吸收可能会影响心血管疾病和癌症的发展。本研究的目的是在体外吸收试验中研究改变胆汁色素的物理化学性质是否会提高其通透性。使用Caco-2细胞系测试天然和合成修饰的胆汁色素的胃肠道通透性和代谢稳定性。此外,在红细胞共孵育试验中测试了它们毒性作用的大致情况。未结合胆红素(1)、胆红素二牛磺酸盐(2)和胆绿素(3)通过Caco-2细胞单层的表观渗透率分别测定为10.4±1.2×10(-7)、35.2±3.4×10(-7)和37.0±1.6×10(-7)cm/s(平均值±标准差),而胆绿素二葡糖胺(4)和胆绿素二辛胺(5)则不可渗透。未结合胆红素、胆绿素、胆红素二牛磺酸盐和胆绿素二葡糖胺在Caco-2细胞匀浆中孵育时不会分解,而胆绿素二辛胺会随时间分解。只有未结合胆红素对红细胞显示出毒性(≥1000 microM),加入40 g/L血清白蛋白后这种作用消失。此处呈现的数据表明胆汁色素可穿过Caco-2细胞单层被吸收,并且胆绿素与亲水性或亲脂性部分的结合会降低其吸收并可能降低其代谢稳定性。总之,外源性胆红素和胆绿素补充剂可能在体内穿过肠上皮被吸收,并可能增加这些抗氧化化合物的循环浓度。

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