Cluster-determinant 36 (CD36) mediates intestinal absorption of dietary astaxanthin and affects its secretion.

Xiaojuan Liu, Junlin Zhang, Zhiqing Chen, Jie Xiao, Aimei Zhou, Yongshui Fu, Yong Cao
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Abstract

The functional activity of dietary astaxanthin is closely related to its absorption, and the absorption of dietary carotenoids mainly mediated by transmembrane transport protein (TTP) has become the mainstream research direction in recent years. However, the main TTP mediating astaxanthin absorption and its potential mechanisms are still unclear. Hence, based on the preliminary screening results, this study aims to elucidate the role of cluster-determinant 36 (CD36) mediating astaxanthin absorption from the perspective of expression levels through in vitro cell model, in situ single-pass intestinal perfusion model and in vivo mice model. The results showed that astaxanthin uptake was significantly increased by 45.13% in CD36 overexpressing cells and decreased by 20.92% in the case of sulfo-N-succinimidyl oleate (SSO) inhibition. A similar trend also appeared in the duodenum and jejunum by in situ model. Moreover, astaxanthin uptake in the small intestine of CD36 knockout mice was significantly reduced by 88.22%. Furthermore, the inhibition or knockout of CD36 suppressed the expression of other transporters (SR-BI and NPC1L1). Interestingly, CD36 was also involved in the downstream secretion pathway, which is manifested by interfering with the expression of related proteins (ERK1/2, MTP, ApoB48, and ApoAI). Therefore, these results indicate the important role of CD36 in astaxanthin transmembrane transport for the first time, providing vital exploration way for the absorption of dietary fat-soluble substances.

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簇决定簇36(CD36)介导膳食虾青素的肠道吸收并影响其分泌。
膳食虾青素的功能活性与其吸收密切相关,主要由跨膜转运蛋白(TTP)介导的膳食类胡萝卜素的吸收已成为近年来的主流研究方向。然而,TTP介导虾青素吸收的主要机制及其潜在机制尚不清楚。因此,基于初步筛选结果,本研究旨在通过体外细胞模型、原位单程肠道灌注模型和体内小鼠模型,从表达水平的角度阐明簇决定簇36(CD36)介导虾青素吸收的作用。结果表明,在过表达CD36的细胞中,虾青素的摄取显著增加了45.13%,而在磺基-N-琥珀酰亚胺油酸酯(SSO)抑制的情况下,虾青质的摄取减少了20.92%。通过原位模型,十二指肠和空肠也出现了类似的趋势。此外,CD36敲除小鼠小肠中的虾青素摄取量显著降低了88.22%。此外,抑制或敲除CD36抑制了其他转运蛋白(SR-BI和NPC1L1)的表达。有趣的是,CD36也参与下游分泌途径,这表现为干扰相关蛋白(ERK1/2、MTP、ApoB48和ApoAI)的表达。因此,这些结果首次表明CD36在虾青素跨膜转运中的重要作用,为日粮脂溶性物质的吸收提供了重要的探索途径。
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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