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Seaweed extracts and unsaturated fatty acid constituents from the green alga Ulva lactuca as activators of the cytoprotective Nrf2–ARE pathway

机译:来自绿藻ULVA乳酸的海藻提取物和不饱和脂肪酸成分作为细胞保护NRF2的活化剂是途径

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摘要

Increased amounts of reactive oxygen species (ROS) have been implicated in many pathological conditions, including cancer. The major machinery that the cell employs to neutralize excess ROS is through the activation of the antioxidant-response element (ARE) that controls the activation of many phase II detoxification enzymes. The transcription factor that recognizes the ARE, Nrf2, can be activated by a variety of small molecules, most of which contain an α,β-unsaturated carbonyl system. In the pursuit of chemopreventive agents from marine organisms, we built, fractionated, and screened a library of 30 field-collected eukaryotic algae from Florida. An edible green alga, Ulva lactuca, yielded multiple active fractions by ARE–luciferase reporter assay. We isolated three monounsaturated fatty acid (MUFA) derivatives as active components, including a new keto-type C18 fatty acid (>1), the corresponding shorter chain C16 acid (>2), and an amide derivative (>3) of the C18 acid. Their chemical structures were elucidated by NMR and mass spectrometry. All three contain the conjugated enone motif between C7 and C9, which is thought to be responsible for the ARE activity. Subsequent biological studies focused on >1, the most active and abundant ARE activator isolated. C18 acid >1 induced the expression of ARE-regulated cytoprotective genes, including NAD(P)H:quinone oxidoreductase 1, heme oxygenase 1, thioredoxin reductase 1, both subunits of the glutamate–cysteine ligase (catalytic subunit and modifier subunit), and the cystine/glutamate exchange transporter, in IMR-32 human neuroblastoma cells. Its cellular activity requires the presence of Nrf2 and PI3K function, based on RNA interference and pharmacological inhibitor studies, respectively. Treatment with >1 led only to Nrf2 activation, and not the increase in production of NRF2 mRNA. To test its ARE activity and cytoprotective potential in vivo, we treated mice with a single dose of a U. lactuca fraction that was enriched with >1, which showed ARE-activating effects similar to those observed in vitro. This could be owing to this fraction's ability to stabilize Nrf2 through inhibition of Keap1-mediated Nrf2 ubiquitination and the subsequent accumulation and nuclear translocation of Nrf2. The induction of many ARE-driven antioxidant genes in vivo and most prominently in the heart agreed with the commonly recognized cardioprotective properties of MUFAs. A significant increase in Nqo1 transcript levels was also found in other mouse tissues such as the brain, lung, and stomach. Collectively, this study provides new insight into why consumption of dietary seaweed may have health benefits, and the identified compounds add to the list of chemopreventive dietary unsaturated fatty acids.
机译:活性氧物质(ROS)的增加与包括癌症在内的许多病理状况有关。细胞用来中和过量ROS的主要机制是通过抗氧化剂反应元件(ARE)的激活来控制许多II期解毒酶的激活。识别ARE的转录因子Nrf2可以被多种小分子激活,其中大多数包含α,β-不饱和羰基系统。在追求海洋生物化学预防剂的过程中,我们建立,分离和筛选了由30个现场采集的佛罗里达真核藻类组成的文库。通过ARE-荧光素酶报告基因分析,可食用的绿藻Ulva lactuca可产生多个活性级分。我们分离了三种单不饱和脂肪酸(MUFA)衍生物作为活性成分,包括新的酮型C18脂肪酸(> 1 )和相应的较短链的C16酸(> 2 )。 ,以及C18酸的酰胺衍生物(> 3 )。通过NMR和质谱法阐明了它们的化学结构。所有这三个都在C7和C9之间包含共轭烯酮基序,这被认为是ARE活性的原因。随后的生物学研究集中于> 1 ,这是最活跃和最丰富的ARE激活剂。 C18酸> 1 诱导ARE调节的细胞保护性基因的表达,包括NAD(P)H:醌氧化还原酶1,血红素加氧酶1,硫氧还蛋白还原酶1,均为谷氨酸-半胱氨酸连接酶的两个亚基(催化亚基)和修饰子亚基),以及IMR-32人成神经细胞瘤细胞中的胱氨酸/谷氨酸交换转运蛋白。分别基于RNA干扰和药理抑制剂研究,其细胞活性需要Nrf2和PI3K功能的存在。用> 1 处理仅导致Nrf2激活,而不导致NRF2 mRNA的产生增加。为了在体内测试其ARE活性和细胞保护潜力,我们用富含> 1 的单剂量U. lactuca馏分处理了小鼠,显示出与体外观察到的相似的ARE激活作用。这可能是由于该级分通过抑制Keap1介导的Nrf2泛素化以及随后的Nrf2积累和核易位而稳定了Nrf2的能力。体内和心脏中最显着的许多ARE驱动的抗氧化剂基因的诱导与MUFA的公认心脏保护特性一致。在其他小鼠组织(如脑,肺和胃)中也发现Nqo1转录水平显着增加。总的来说,这项研究提供了新的见解,说明食用食用海藻为何可能对健康有益,并且已鉴定的化合物增加了化学预防性饮食中不饱和脂肪酸的种类。

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