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利用生物学相关的消化模型评估叶绿酸铁的生物可给性和 Caco-2 细胞摄取率。

Bioaccessibility and Caco-2 cell uptake of iron chlorophyllin using a biologically relevant digestion model.

机构信息

Department of Human Sciences, OSU Interdisciplinary Nutrition Program, The Ohio State University, Columbus, Ohio, USA.

Department of Human Sciences, OSU Interdisciplinary Nutrition Program, The Ohio State University, Columbus, Ohio, USA; Foods for Health Discovery Theme, The Ohio State University, Columbus, Ohio, USA.

出版信息

J Nutr Biochem. 2024 Oct;132:109698. doi: 10.1016/j.jnutbio.2024.109698. Epub 2024 Jul 3.

Abstract

Iron deficiency remains a top nutrient deficiency worldwide. Iron chlorophyllin (IC), a compound structurally analogous to heme, utilizes the protoporphyrin ring of chlorophyll to bind iron. IC has previously been shown to deliver more iron to Caco-2 cells than FeSO, the most common form prescribed for supplementation. However, previous test conditions used digestive conditions outside of those observed in humans. This study sought to assess IC bioaccessibility and Caco-2 cell uptake using physiologically relevant digestive solutions, pH, and incubation time, as compared to other iron sources (i.e., FeSO, and hemoglobin (Hb)). Co-digestion with ascorbic acid (AA) and albumin was also investigated. Following gastric, duodenal, and jejunal digestion, IC-bound iron was less bioaccessible than iron delivered as FeSO, and IC-bound iron was less bioaccessible than Hb-bound iron. IC-bound iron bioaccessibility was not affected by AA and was enhanced 2x when co-digested with a low dose of albumin. However, Caco-2 cell incubation with IC-containing digesta increased cell ferritin 2.5x more than FeSO alone, and less than Hb. IC with AA or with 400 mg albumin also increased cell ferritin more than IC alone, with the greatest increases observed following incubation of digesta containing IC + AA + 400 mg albumin. These results suggest IC can serve as an improved source of iron for supplementation as compared to FeSO These results also support further in vivo investigations of IC-based iron delivery in populations at risk of iron deficiency.

摘要

缺铁仍然是全球范围内最主要的营养缺乏症之一。铁叶绿酸(IC)是一种结构上与血红素类似的化合物,它利用叶绿素的原卟啉环来结合铁。IC 先前已被证明比硫酸亚铁(最常见的补充剂形式)向 Caco-2 细胞输送更多的铁。然而,之前的测试条件使用的消化条件超出了人体观察到的范围。本研究旨在使用生理相关的消化溶液、pH 值和孵育时间来评估 IC 的生物利用度和 Caco-2 细胞摄取率,并与其他铁源(即硫酸亚铁和血红蛋白(Hb))进行比较。还研究了与抗坏血酸(AA)和白蛋白共消化的情况。在胃、十二指肠和空肠消化后,IC 结合的铁比硫酸亚铁提供的铁的生物利用度更低,IC 结合的铁比 Hb 结合的铁的生物利用度更低。AA 对 IC 结合的铁的生物利用度没有影响,但当与低剂量的白蛋白共消化时,IC 结合的铁的生物利用度提高了 2 倍。然而,与单独的 FeSO 相比,IC 含有消化物孵育的 Caco-2 细胞中的铁蛋白增加了 2.5 倍,低于 Hb。含有 AA 或 400mg 白蛋白的 IC 也增加了细胞铁蛋白的含量,比单独的 IC 增加更多,在含有 IC+AA+400mg 白蛋白的消化物孵育后观察到最大的增加。这些结果表明,与 FeSO 相比,IC 可以作为补充铁的改良来源。这些结果还支持进一步研究 IC 基铁输送在缺铁风险人群中的体内应用。

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