A Comparative Study About the Neuroprotective Effects of EPA-Enriched Phosphoethanolamine Plasmalogen and Phosphatidylethanolamine Against Oxidative Damage in Primary Hippocampal Neurons

s Oxidative stress is involved in the progression of neurodegenerative diseases.Previous evidences showed that plasma-logens could improve neurodegenerative diseases.In this study,we investigated the function of phosphoethanolamine plasmalogens enriched with EPA(EPA-pPE)and phosphatidylethanolamine enriched with EPA(EPA-PE)on oxidative damage prevention after hy-drogen peroxide(H2O2)and tert-butylhydroperoxide(t-BHP)challenge in primary hippocampal neurons.Results showed that neurons pretreated with EPA-pPE and EPA-PE demonstrated the ability to alleviate oxidative damage,which was proved by the in-creased cell viability.Moreover,the shape and number of neurons were more similar to those of the control group.Antioxidant acti-vity,apoptosis,as well as TrkB/ERK/CREB signaling pathway were investigated to explore the mechanisms.The results suggested that EPA-PE was superior to EPA-pPE in regulating mitochondrial apoptosis.EPA-pPE was more prominent than EPA-PE in upre-gulating TrkB/ERK/CREB signaling pathway.Phospholipids with EPA exerted neuroprotective effects via inhibiting oxidative stress,suppressing apoptosis,and regulating TrkB/ERK/CREB signaling pathway.Therefore,the results provide a scientific basis for utili-zation of phospholipids enriched with EPA on the treatment of neurodegenerative disease.

Dietary Lipid Intervention in the Prevention of Brain Aging

As people live longer,the burden of aging-related brain diseases,especially dementia,is increasing.Brain aging increases the risk of cognitive impairment,which manifests as a progressive loss of neuron function caused by the impairment of synaptic plasticity via disrupting lipid homeostasis.Therefore,supplemental dietary lipids have the potential to prevent brain aging.This review summarizes the important roles of dietary lipids in brain function from both structure and mechanism perspectives.Epidemiological and animal studies have provided evidence of the functions of polyunsaturated fatty acids(PUFAs)in brain health.The results of interventions indicate that phospholipids—including phosphatidylcholine,phosphatidylserine,and plasmalogen—are efficient in alleviating cognitive impairment during aging,with plasmalogen exhibiting higher efficacy than phosphatidylserine.Plasmalogen is a recognized nutrient used in clinical trials due to its special vinyl ether bonds and abundance in the postsynaptic membrane of neurons.Future research should determine the dose-dependent effects of plasmalogen in alleviating brain-aging diseases and should develop extraction and storage procedures for its clinical application.

缩醛磷脂的功能及信号传导机制研究进展

缩醛磷脂(plasmalogen)是甘油骨架C-1位置上含有烯醚键的磷脂,作为哺乳动物细胞质膜的结构成分广泛分布于生物电强的组织中。它可以调节质膜的流动,是多不饱和脂肪酸的储存库,并可作为内源抗氧化剂保护细胞氧化应激。同时,缩醛磷脂还与细胞信号传导有关。

胃癌患者血浆缩醛磷脂和糖脂水平变化

目的 :研究胃癌患者血浆缩醛磷脂和糖脂含量变化 ,并探讨其应用价值。方法 :对临床确诊的 36例胃癌患者 (术前和术后 30d)及 38例正常成人分别测定其血浆缩醛磷脂和糖脂中的总唾液酸 (TSA)及脂结合唾液酸(LSA)的含量。结果 :①胃癌患者术前血浆缩醛磷脂含量显著高于术后 30d和正常人对照组 (P <0 0 5 ) ;②胃癌患者术前血浆总唾液酸 (TSA)和脂结合唾液酸 (LSA)含量显著高于术后 30d和正常人对照组 (P <0 0 5 )。结论 :胃癌患者 (术前 )血浆缩醛磷脂和糖脂含量显著增高。

缩醛磷脂提取和制备的实验研究

通过将新鲜猪心切块、绞碎 ,制成组织匀浆后 ,再经一系列过程包括总脂的提取、从总脂提取物中制取磷脂酰乙醇胺、碱水解进一步纯化缩醛磷脂酰乙醇胺以及对获得的缩醛磷脂酰乙醇胺制剂鉴定其纯度。通过Iodinedisappearance法测出缩醛磷脂酰乙醇胺制剂中的含量为 1 5 35mmol/L ,通过Bartell法测出缩醛磷脂酰乙醇胺制剂中无机磷含量为 1 6.1 0mmol/L。因此 ,获得缩醛磷脂酰乙醇胺制剂的纯度为 95 34 %。

内源性缩醛磷脂对大鼠脑缺血损伤的保护作用

目的探察证实内源性缩醛磷脂对大鼠缺血性脑损伤的保护作用。方法采用行为学探测、经典组化和免疫组化技术对模型大鼠的运动和学习记忆以及纹状体组织病理变化进行形态学探察,实验数据采用SPSS软件统计学处理。结果 1运动行为学探测显示缺血大鼠通过平衡木所需时间明显延长(P<0.05),缩醛磷脂干预的大鼠比缺血大鼠所需时间缩短(P<0.05);握力测试中,缺血大鼠抓握时间缩短(P<0.05),治疗组大鼠抓握时间比缺血组延长(P<0.05)。Morris水迷宫实验中,缩醛磷脂干预的大鼠逃避潜伏期与缺血组相比明显缩短(P<0.05),空间探索经过平台次数明显多于缺血组(P<0.05)。2组织学与免疫组织化学探察显示,缺血大鼠纹状体的背外侧区出现明显的损伤区域,损伤区域中神经元几乎完全丢失,而缩醛磷脂干预组的大鼠则有少数体积较小的神经元幸存。结论内源性缩醛磷脂对大鼠脑缺血损伤有保护作用。

阿尔茨海默病患者大脑生物膜性抗氧化物质含量的改变

选用阿尔茨海默病（ＡＤ）患者不同部位的尸解脑组织标本，以同龄非神经系统疾病患者尸解脑组织标本作为对照，测定脑组织中蛋白质、ＤＮＡ、辅酶Ｑ、缩醛磷脂酰乙醇胺和丙二醛含量，研究内源性生物膜性抗氧化物质在ＡＤ发生中的变化。结果显示：蛋白质和ＤＮＡ含量两组间无明显差别；ＡＤ患者大脑皮质额叶和海马区域中辅酶Ｑ含量升高，缩醛磷脂酰乙醇胺含量降低，经诱导后的丙二醛含量明显高于对照组。表明：ＡＤ患者受影响的脑组织中生物膜性抗氧化物质水平发生异常改变，这种表现可能与体内自由基含量的异常变化有关。

胃癌术前血浆缩醛磷脂与总胆固醇水平的比较分析

目的 研究胃癌患者血浆缩醛磷脂含量的变化并与总胆固醇含量变化的相关性进行比较分析。方法 对临床确诊的 3 6例胃癌患者及 3 8例正常成人分别测定其血浆缩醛磷脂和总胆固醇的含量。结果 ①胃癌患者血浆缩醛磷脂含量较正常人对照组明显增加 ,且差异有统计学意义 (P <0 .0 5 )。②胃癌患者血浆总胆固醇含量较正常人对照组亦明显增加 ,差异有统计学意义 (P <0 .0 5 )。③胃癌患者组中 (术前 ) ,血浆缩醛磷脂与总胆固醇呈正相关关系 (r =0 .82 ,且P <0 .0 0 1)。结论 在胃癌患者中 ,血浆缩醛磷脂含量显著增高 。

大肠癌手术前后血浆缩醛磷脂等类脂水平变化

目的 研究大肠癌患者血浆缩醛磷脂、总磷脂、总胆固醇和糖脂含量变化 ,并探讨其应用价值。方法 对临床确诊的 3 4例大肠癌患者 (术前和术后 3 0天 )及 3 6例正常成人分别测定其血浆缩醛磷脂、总磷脂、总胆固醇和糖脂中的总唾液酸 (TSA)及脂结合唾液酸 (LSA)的含量。结果 1.大肠癌患者术前血浆缩醛磷脂含量较术后 3 0天和正常人对照组明显增加 ,差异统计学有意义 (P <0 .0 5 ) ,而大肠癌患者术前血浆总磷脂含量较术后 3 0天和正常人对照组有所减少 ,差异亦有统计学意义 (P <0 .0 5 )。 2 .大肠癌患者术前血浆总胆固醇含量较术后 3 0天和正常人对照组亦明显增加 ,差异有显著性意义 (P <0 .0 5 )。 3 .大肠癌患者术前血浆总唾液酸 (TSA)和脂结合唾液酸 (LSA)含量显著高于术后 3 0天和正常人对照组 ,其差异有统计学意义 (P <0 .0 5 )。结论 大肠癌患者 (术前 )血浆缩醛磷脂、总胆固醇和糖脂含量显著增高 ,而总磷脂的含量是降低的。

缩醛磷脂的分离 纯化和鉴定

目的 研究从猪心中提取和纯化缩醛磷脂 ,并测定其纯度 ,以利于进一步研究其生物学作用。方法 取新鲜猪心切块 ,绞碎 ,制成匀浆后 ,再经一系列过程包括①总脂的提取 ;②通过硅酸柱层析和硅胶薄板层析从总脂提取物中分离出磷脂酰乙醇胺 (PE)、磷脂酰胆碱 (PC)、磷脂酰肌醇 (PI)、磷脂酰丝氨酸 (PS)和鞘磷脂 (SM ) ,并从含PE浓度最高的柱层析液中分离出PE ;③碱水解制备缩醛磷脂酰乙醇胺 (plas PE) ;④通过硅酸柱层析和硅胶薄板层析从碱水解物中进一步纯化和鉴定 plas PE ;⑤分别用Iodinedisappearance法和Bartlett法检测 plas PE制剂中plas PE的含量及无机磷的含量 ,并计算出其纯度。 结果 ①从总脂提取液中分离出下列几种磷脂并经标准品鉴定出为PE、PI+PS、PC和SM ,其Rf值分别为 0 .87、0 .75、0 .54和 0 .37;②从含PE浓度最高的柱层析液中分离出PE ,并经碱水解 ,制备出plas PE ,其在薄板层析板上的Rf值为 0 .81 ;③plas PE制剂中无机磷含量为 3 .1 61 μmol/ml,plas PE含量为 3 .0 0 6μmol/ml,经计算 plas PE的纯度为 95 .1 0 %。 结论 猪心是缩醛磷脂含量丰富的器官 。

3'-甲基-4-二甲氨基偶氯苯对大鼠肝脏磷脂代谢的影响

探讨3'—甲基—4—二甲氨基偶氮苯（3'－Me－DAB）诱发大鼠肝癌过程中肝脏磷脂代谢的变化。用3'－Me－DAB诱发Wistar大鼠肝癌，同时辅以低胆碱饮食，TLC分离磷脂组分，Rouser法测定第6、9、12、16、20周肝脏中总磷脂及各磷脂组分含量。结果：发现诱癌组总磷脂和磷脂酸胆碱（PC）的含量不断下降，且两者变化一致；鞘磷脂（SM）在3'—Me—DAB加普通饮食组（A组）诱癌早期即迅速增高，超过对照组约1倍，并一直维持至肝癌形成，而在3'—Me—DAB加低胆碱饮食组（B组）虽然早期也升高，但当第20周肿瘤发生转移时降至对照组以下；溶血磷脂酰胆碱（LPC）仅在B组晚期出现下降。不含胆碱基因的磷脂组分：磷脂酰乙醇胺（PE）、磷脂酰丝氨酸（PS）和磷脂酰肌醇（PI）在3'—Me—DAB诱癌晚期均降低，B组尤为明显。缩醛磷脂的含量在整个诱癌过程中未见明显变化。结论：3'－Me－DAB诱发大鼠肝癌过程中主要影响PC和SM的代谢，表现为PC降低，SM增高。低胆碱饮食能缯强3'—Me—DAB对大鼠肝脏磷脂代谢的影响。

缩醛磷脂制备及其生物功能研究进展

缩醛磷脂是甘油骨架sn-1位上含有一个烯醚键的磷脂,主要存在于哺乳动物组织中,其能保持膜稳定性,具有潜在信息传导及抗癌和抗氧化作用;且其含量变化也与许多疾病有关。该文介绍缩醛磷脂制备方法及其生物功能研究进展。

Structural and functional roles of ether lipids

Ether lipids, such as plasmalogens, are peroxisome- derived glycerophospholipids in which the hydrocarbon chain at the sn-1 position of the glycerol backbone is attached by an ether bond, as opposed to an ester bond in the more common diacyl phospholipids. This seem- ingly simple biochemical change has profound structural and functional implications. Notably, the tendency of ether lipids to form non-lamellar inverted hexagonal structures in model membranes suggests that they have a role in facilitating membrane fusion processes. Ether lipids are also important for the organization and stability of lipid raft microdomains, cholesterol-rich membrane regions involved in cellular signaling. In addition to their structural roles, a subset of ether lipids are thought to function as endogenous antioxidants, and emerging studies suggest that they are involved in cell differentiation and signaling pathways. Here, we review the biology of ether lipids and their potential signifi- cance in human disorders, including neurological diseases, cancer, and metabolic disorders.

Ether phospholipids govern ferroptosis

Ferroptosis is a cell death modality triggered by excessive lipid peroxidation.Two recent studies(Zou et al.,2020;Cui et al.,2021)not only reveal critical roles of ether-linked phospholipids as an additional source for providing polyunsaturated fatty acid-containing phospholipids in driving ferroptosis but also suggest a context-dependent role of TMEM189-mediated vinyl-ether phospholipid(plasmalogen)synthesis in ferroptosis.

缩醛磷脂对混合细菌感染大鼠阴道炎的改善效果分析

目的探讨缩醛磷脂对混合细菌感染大鼠阴道炎的改善效果及可能机制。方法选取雌性Wistar大鼠经阴道先后注入金黄色葡萄球菌和大肠埃希菌以构建混合感染性大鼠阴道炎模型,接种5 d后取感染成功的80只模型大鼠随机分为模型组、凝胶基质组和缩醛磷脂高、中、低剂量组,每组16只。缩醛磷脂高、中、低剂量组分别接受10、5、2.5 mg/kg的缩醛磷脂凝胶阴道给药,每天1次,连续1周。比较各组大鼠的治疗效果(炎症分值、炎症改善率和转阴率)、阴道相关指标(阴道pH、阴道体质量指数和阴道分泌物计分)、氧化应激指标[丙二醛(MDA)和超氧化物歧化酶(SOD)]及炎症指标[肿瘤坏死因子-α(TNF-α)和白细胞介素-8(IL-8)]水平,收集治疗期间阴道灌洗液检测阴道细菌的负荷情况。结果与模型组比较,凝胶基质组大鼠治疗效果、阴道相关指标、氧化应激指标、炎症指标及阴道细菌负荷无显著变化;与模型组和凝胶基质组相比,缩醛磷脂高、中、低剂量组大鼠的炎症分值、阴道pH、阴道分泌物计分、MDA、TNF-α和IL-8水平及阴道细菌负荷均降低,而炎症改善率、转阴率和SOD水平均升高(P<0.05),且缩醛磷脂高剂量组指标优于中、低剂量组(P<0.05)。结论缩醛磷脂对混合感染性大鼠阴道炎具有一定的改善效果,可能与其改善氧化应激和炎症反应有关。