In vitro gastrointestinal digestion of marine oil emulsions and liposomal solutions: fate of LC-PUFAs upon lipolysis

IF 5.1 1区 农林科学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Food & Function Pub Date : 2024-10-30 DOI:10.1039/D4FO03161J
Sawsan Amara, Maureen Gerlei, Carole Jeandel, Moulay Sahaka, Frédéric Carrière and Michel Linder
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Abstract

The bioaccessibility and bioavailability of dietary fatty acids depend on the lipid to which they are esterified, the organisation of theses lipids in water and their recognition by lipolytic enzymes. In this work, we studied the release of marine long-chain polyunsaturated fatty acids (LC-PUFA), depending on their presentation either in the form of phospholipids (PL) or triacylglycerol (TAG). Two formulations based on marine PL or TAG extracted from salmon heads (Salmo salar) were prepared. Lipolysis was first tested in vitro by using individual gastrointestinal lipases and phospholipases to identify the enzymes involved in the digestion. Second, the lipolysis of the prepared formulations by a combination of enzymes was tested under in vitro conditions mimicking the physiological conditions found in the GI tract, both in the stomach and in the upper small intestine, in order to evaluate digestibility of TAG and LC-PUFA-containing liposomes. The in vitro results showed that TAG emulsion was hydrolyzed by porcine pancreatic extracts (PPE) and pure pancreatic lipase (PPL) with its cofactor, colipase, and to a lesser extent by pancreatic-lipase-related protein 2 (PLRP2) and a gastric extract (RGE) containing gastric lipase while no hydrolysis was observed with purified pancreatic phospholipase A2 (PLA2) and carboxyl ester hydrolase (CEH). The PL substrate was found to be hydrolysed by PLA2, PPE and PLRP2. Their phospholipase activities on liposomes formulation was dependent on the presence of bile salts. Using a two-step in vitro digestion model, we measured the kinetics of fatty acid release from TAG and PL during the gastric and intestinal phases of digestion. The highest overall lipolysis level was obtained with liposomes (around 75%) during the intestinal phase while they were preserved during the gastric phase. The overall lipolysis level of TAG emulsion was lower (around 33%), while it started already in the gastric phase. In conclusion, liposomes appear as a better delivery system for intestinal absorption of LC-PUFA than TAG. In addition, their resistance to lipolysis under gastric condition can protect LC-PUFA and provide a gastric stable delivery system for other molecules.

Abstract Image

海洋油乳剂和脂质体溶液的体外胃肠道消化:LC-PUFAs 在脂肪分解后的去向。
膳食脂肪酸的生物可及性和生物利用率取决于它们被酯化的脂质、这些脂质在水中的组织结构以及脂肪分解酶对它们的识别。在这项工作中,我们研究了海洋长链多不饱和脂肪酸(LC-PUFA)的释放,这取决于它们以磷脂(PL)或三酰甘油(TAG)的形式呈现。我们制备了两种基于海洋磷脂或从鲑鱼头(Salmo salar)中提取的 TAG 的配方。首先,利用单个胃肠道脂肪酶和磷脂酶对脂肪分解进行体外测试,以确定参与消化的酶。其次,在模拟胃和小肠上部消化道生理条件的体外条件下,用多种酶对制备的制剂进行脂肪分解试验,以评估含 TAG 和 LC-PUFA 脂质体的消化率。体外实验结果表明,猪胰腺提取物(PPE)和纯胰脂肪酶(PPL)及其辅助因子--大肠脂肪酶可水解 TAG 乳液,胰脂肪酶相关蛋白 2(PLRP2)和含有胃脂肪酶的胃提取物(RGE)也可在较小程度上水解 TAG 乳液,而纯化的胰磷脂酶 A2(PLA2)和羧基酯水解酶(CEH)则不水解 TAG 乳液。发现 PL 底物可被 PLA2、PPE 和 PLRP2 水解。它们在脂质体配方上的磷脂酶活性取决于胆盐的存在。利用两步体外消化模型,我们测量了 TAG 和 PL 在胃肠消化阶段释放脂肪酸的动力学。在肠道消化阶段,脂质体的总体脂肪分解水平最高(约 75%),而在胃肠消化阶段,脂质体的总体脂肪分解水平保持不变。TAG乳液的总体脂肪分解水平较低(约33%),但在胃部阶段已经开始。总之,与 TAG 相比,脂质体似乎是肠道吸收 LC-PUFA 的更好输送系统。此外,脂质体在胃部条件下抗脂肪分解的能力可以保护 LC-PUFA,并为其他分子提供稳定的胃部输送系统。
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来源期刊
Food & Function
Food & Function BIOCHEMISTRY & MOLECULAR BIOLOGY-FOOD SCIENCE & TECHNOLOGY
CiteScore
10.10
自引率
6.60%
发文量
957
审稿时长
1.8 months
期刊介绍: Food & Function provides a unique venue for physicists, chemists, biochemists, nutritionists and other food scientists to publish work at the interface of the chemistry, physics and biology of food. The journal focuses on food and the functions of food in relation to health.
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