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Effects of Marine Oils Digested with Human Fluids on Cellular Viability and Stress Protein Expression in Human Intestinal Caco-2 Cells

机译:用人体液体消化的海洋油脂对人肠道Caco-2细胞细胞活力和应激蛋白表达的影响

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摘要

In vitro digestion of marine oils has been reported to promote lipid oxidation, including the formation of reactive aldehydes (e.g., malondialdehyde (MDA) and 4-hydroxy-2-hexenal (HHE)). We aimed to investigate if human in vitro digestion of supplemental levels of oils from algae, cod liver, and krill, in addition to pure MDA and HHE, affect intestinal Caco-2 cell survival and oxidative stress. Cell viability was not significantly affected by the digests of marine oils or by pure MDA and HHE (0–90 μM). Cellular levels of HSP-70, a chaperone involved in the prevention of stress-induced protein unfolding was significantly decreased (14%, 28%, and 14% of control for algae, cod and krill oil, respectively; p ≤ 0.05). The oxidoreductase thioredoxin-1 (Trx-1) involved in reducing oxidative stress was also lower after incubation with the digested oils (26%, 53%, and 22% of control for algae, cod, and krill oil, respectively; p ≤ 0.001). The aldehydes MDA and HHE did not affect HSP-70 or Trx-1 at low levels (8.3 and 1.4 μM, respectively), whilst a mixture of MDA and HHE lowered Trx-1 at high levels (45 μM), indicating less exposure to oxidative stress. We conclude that human digests of the investigated marine oils and their content of MDA and HHE did not cause a stress response in human intestinal Caco-2 cells.
机译:据报道,海洋油的体外消化促进脂质氧化,包括形成反应性醛(例如,丙二醛(MDA)和4-羟基-2-己烯醛(HHE))。我们的目的是研究人的体外消化,除纯MDA和HHE外,补充水平的藻类,鳕鱼肝和磷虾油的添加是否会影响肠道Caco-2细胞的存活和氧化应激。海洋油的消化物或纯MDA和HHE(0–90μM)对细胞活力没有显着影响。 HSP-70(一种参与预防应激诱导的蛋白质解折叠的分子伴侣)的细胞水平显着降低(藻类,鳕鱼和磷虾油分别为对照组的14%,28%和14%; p≤0.05)。与消化的油温育后,参与减少氧化应激的氧化还原酶硫氧还蛋白-1(Trx-1)的含量也较低(藻类,鳕鱼和磷虾油分别为对照组的26%,53%和22%; p≤0.001 )。醛MDA和HHE在低水平(分别为8.3和1.4μM)时不影响HSP-70或Trx-1,而MDA和HHE的混合物在高水平(45μM)时降低Trx-1氧化应激。我们得出的结论是,人类对所研究海洋油的消化物及其MDA和HHE的含量并未在人类肠道Caco-2细胞中引起应激反应。

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