Postsynaptic Excitation of Prefrontal Cortical Pyramidal Neurons by Hypocretins/Orexins

Hypocretins/orexins are crucial for the regulation of wakefulness by the excitatory actions on multiple subcortical arousal systems. In prefrontal cortex,

Orexin-A和RJR-2403影响脊髓腹角神经元自发动作电位的比较

目的:探究食欲素-A(orexin-A)和α_(4)β_(2)-N型乙酰胆碱受体(α_(4)β_(2)-nAChR)选择性激动剂RJR-2403分别对新生大鼠离体脊髓腹角神经元自发动作电位影响的差异。方法:应用8~12 d新生SD大鼠,麻醉后游离出颈端至骶部的脊髓,保留腰骶膨大节段并制备切片。切片孵育30min,采用木瓜蛋白酶消化19~22 min,转常温孵育45~60 min。沿中央管切取脊髓腹角,使用口径从大到小的巴斯德吸管急性机械分离神经元,静置20 min待细胞贴壁,在倒置显微镜下利用膜片钳记录良好的神经元,联合药理学方法进行功能性研究。在电流钳记录模式下,观察orexin-A和RJR-2403分别对离体脊髓腹角神经元自发放电(动作电位)的影响,并比较多种参数的差异。结果:(1)本研究应用急性分离的脊髓腹角神经元进行膜片钳记录,所记录的神经元胞体完整,形态多样,能发出较多突起且有分支;(2)给予orexin-A前的腹角神经元自发动作电位的频率[(3.55±0.66)Hz]低于给药后[(8.26±3.31)Hz](P<0.01),给药前动作电位幅值[(95.28±7.21)mV]高于给药后[(85.15±5.80)mV](P<0.05),静息电位和动作电位半幅时程无明显变化;(3)应用RJR-2403前,腹角神经元的静息电位[(-66.67±43.38)mV]高于给药后[(-60.48±3.38)mV](P<0.01),给药前放电频率[(2.74±1.60)Hz]低于给药后[(8.94±3.14)Hz](P<0.001),给药前动作电位幅值[(84.96±4.85)mV]高于给药后[(73.77±5.42)mV](P<0.01),给药前半幅时程[(4.34±1.52)ms]低于给药后[(5.39±1.80)ms](P<0.01)。结论:Orexin-A和RJR-2403对脊髓腹角神经元自发动作电位均具有正性调制作用,但对于静息电位、半幅时程存在不同作用,可能源于促代谢型受体和促离子型受体介导的作用差异。

神经肽Orexins的研究进展

orexins是一组神经肽 ,分为orexinA、orexinB (OXA、OXB) 2种 ,它们来源于同一前体。orexins主要由下丘脑神经元产生 ,通过其神经纤维的直接投射或释放入脑脊髓液作用于靶位点 ,激活 2种与G蛋白耦联的细胞表面受体OX1R、OX2 R ,参与机体对摄食、能量代谢、睡眠—觉醒循环等生理活动的调节。

一种新的神经肽——Orexins

Orexins hypocretins是新发现的源于同一前体的一类神经肽 ,有orexinA和orexinB两种。orexins主要由下丘脑神经元产生 ,通过神经纤维的直接投射或释放进入脑室循环间接作用于远处的靶细胞 ,激活两种与G蛋白偶联的细胞表面受体OX1R和OX2R。orexins参与了下丘脑对摄食、能量代谢、心血管功能。

神经肽Orexins的研究进展

orexins是一组神经肽,分为orexinA、orexinB(OXA、OXB)2种,它们来源于同一前体。orexins主要由下丘脑神经元产生,通过其神经纤维的直接投射或释放入脑脊髓液作用于靶位点,激活2种与G蛋白耦联的细胞表面受体OX1R、OX2R,参与机体对摄食、能量代谢、睡眠—觉醒循环等生理活动的调节。

FGF23、orexin A、BMP-7在肾衰竭患者中的表达水平及与临床预后的关系

目的探讨成纤维细胞生长因子23(fibroblast growth factor 23,FGF23)、食欲素A(orexin A)、骨形态发生蛋白7(bone morphogenetic protein-7,BMP-7)在肾衰竭患者中的表达水平及与临床预后的关系。方法选取收治的肾衰竭患者65例为研究组,另选同期健康体检人群65例为对照组。研究对象均检测血液中FGF23、orexin A、BMP-7水平并进行比较分析;进行1年随访后,比较不同临床预后患者的临床资料,并分析FGF23、orexin A、BMP-7与肾衰竭患者临床不良预后的相关性;COX回归分析影响肾衰竭患者预后因素,分析FGF23、orexin A、BMP-7预测肾衰竭患者预后不良的接受者操作特性曲线(receiver operating characteristic curve,ROC)图。结果与对照组比较,研究组FGF23、orexin A表达水平及血肌酐、尿酸、血尿素氮、C反应蛋白(C-reactive protein,CRP)水平较高,BMP-7表达水平较低(P<0.05);预后良好组48例,预后不良组17例,与预后良好组比较,预后不良组血肌酐、尿酸、血尿素氮、CRP、FGF23、orexin A表达水平较高,BMP-7表达水平较低(P<0.05);FGF23、orexin A与肾衰竭患者临床不良预后呈正相关,BMP-7与肾衰竭患者临床不良预后呈负相关(P<0.05);FGF23、orexin A是肾衰竭患者预后不良的独立危险因素,BMP-7是保护因素(P<0.05);FGF23、orexin A、BMP-7 AUC分别为0.920、0.697、0.849。结论肾衰竭患者FGF23、orexin A表达水平较高,BMP-7表达水平较低,对肾衰竭患者的预后具有预测价值。

丘脑深部电刺激对脑外伤昏迷大鼠意识状态及前额叶皮质Orexins受体OX1R表达的影响

目的探讨丘脑深部电刺激(DBS)对脑外伤后昏迷大鼠的促醒作用及对Orexins受体1(OX1R)表达的影响。方法将54只SD大鼠随机分为3组:空白对照组(n=18,不做任何处理);对照组(n=18)和DBS组(n=18)。通过自由落体撞击大鼠脑部建立脑外伤昏迷大鼠模型,造模成功后对照组大鼠丘脑植入电极,但不予DBS,DBS组大鼠丘脑植入电极,并予DBS。用意识状态六级评分法评估大鼠的意识状态和行为学变化,并用Western-blot(WB)、免疫荧光技术检测3组大鼠前额叶皮质(PFC)区OX1R的表达水平。结果DBS 1 h后,DBS组16只出现翻正反射(16/18),对照组7只出现翻正反射(7/18),DBS组意识状态水平好于对照组(U=96.00,P=0.026)。在DBS刺激完成后的12 h,WB、免疫荧光技术检测Orexins受体OX1R的表达水平,DBS组均明显高于对照组(P<0.05);对照组明显低于空白对照组(P<0.05)。结论脑外伤昏迷大鼠可以通过DBS提高它的意识状态水平,其机制可能与DBS能上调PFC区OX1R的表达水平有关。

orexin/hypocretin与发作性睡病

发现orexin／hypocretin已经10多年，作为体内重要的内源性物质之一，研究发现其与发作性睡病密切相关。国内关于0rexin／hypocretin与发作性睡病的研究较少，本文对orexin／hypocretin系统，hypocretin与发作性睡病的诊断和治疗进行了介绍，并对发作性睡病患者hypocretin神经元减少的神经元变性、免疫学、理化因素途径进行了综述，并提出了未来的研究方向。

Orexins and male reproduction

Orexins (or hypocretins) are hypothalamic neuropeptides with a multitude of physiological functions. They occur in two known forms, namely, orexin A and orexin B with a common precursor, preproorexin. The orexin receptors (orexin 1R and orexin 2R) belong to the Family of G-protein coupled receptors. The primary function of the orexin system,i.e. the orexins, their receptors and associated neuronal circuitries, perhaps is to increase spontaneous physical activity and food intake, thereby promoting an increase in energy expenditure. Reports suggest that orexins may be the key brain components to mediate the mechanism of obesity resistance. Recent research also has thrown lights upon a significant role of orexins, especially orexin A, in regulation of male reproductive functions owing to their receptor expressions in vital testicular cells, such as Leydig cells, Sertoli cells as well as spermatozoa at different developmental stages, even in the epididymis and penis. Moreover, orexins have been reported to greatly influence gonadotropin-releasing hormone neurons and their secretions to regulate reproductive functionsvia modulation of the hypothalamic-pituitary-gonadal axis. Evidence thus implicates participation of orexins in steroidogenesis, spermatogenesis, transportation and maturation of sperm as well as in the control of penile function. However, further research is required in this direction to elucidate the mechanisms by which orexins play a role in different testicular functions and effect of orexins on semen quality.

Orexins:A promising target to digestive cancers,inflammation,obesity and metabolism dysfunctions

Hypothalamic neuropeptides named hypocretin/orexins which were identified in 1998 regulate critical functions such as wakefulness in the central nervous system.These past 20 years had revealed that orexins/receptors system was also present in the peripheral nervous system where they participated to the regulation of multiple functions including blood pressure regulation,intestinal motility,hormone secretion,lipolyze and reproduction functions.Associated to these peripheral functions,it was found that orexins and their receptors were involved in various diseases such as acute/chronic inflammation,metabolic syndrome and cancers.The present review suggests that orexins or the orexin neural circuitry represent potential therapeutic targets for the treatment of multiple pathologies related to inflammation including intestinal bowel disease,multiple sclerosis and septic shock,obesity and digestive cancers.

Hypocretin(orexin) pathology in Alzheimer's disease

Alzheimer's disease(AD) is a growing health problem. It has enormous public health impact. Sleep problems show an early component of this disease. Hypocretin hasa major function in sleep-wake cycle. The total number of hypocretin neurons in the normal humans ranges from 51000-83000, located exclusively in the hypothalamus. Deficiency in hypocretins neurotransmission results in narcolepsy, Parkinson's disease, and other neurological and psychological disorders. Cerebrospinal fluid(CSF) hypocretin levels were directly related with t-tau protein amount in AD. Increased hypocretin CSF in AD suggest that hypocretin is involved in the mechanism of AD pathology.

Alzheimer's disease with sleep insufficiency:a cross-sectional study on correlations among clinical characteristics,orexin,its receptors,and the bloodbrain barrier

Previous studies have shown that reduced sleep duration,sleep fragmentation,and decreased sleep quality in patients with Alzheimer's disease are related to dysfunction in orexin signaling.At the same time,blood-brain barrier disruption is considered an early biomarker of Alzheimer's disease.However,currently no report has examined how changes in orexin signaling relate to changes in the blood-brain barrier of patients who have Alzheimer's disease with sleep insufficiency.This cross-sectional study included 50 patients with Alzheimer's disease who received treatment in 2019 at Beijing Tiantan Hospital.Patients were divided into two groups:those with insufficient sleep(sleep duration≤6 hours,n=19,age 61.58±8.54 years,10 men)and those with normal sleep durations(sleep duration>6 hours,n=31,age 63.19±10.09 years,18 men).Demographic variables were collected to evaluate cognitive function,neuropsychiatric symptoms,and activities of daily living.The levels of orexin,its receptor proteins,and several blood-brain barrier factors were measured in cerebrospinal fluid.Sleep insufficiency was associated with impaired overall cognitive function that spanned multiple cognitive domains.Furthermore,levels of orexin and its receptors were upregulated in the cerebrospinal fluid,and the blood–brain barrier was destroyed.Both these events precipitated each other and accelerated the progression of Alzheimer's disease.These findings describe the clinical characteristics and potential mechanism underlying Alzheimer's disease accompanied by sleep deprivation.Inhibiting the upregulation of elements within the orexin system or preventing the breakdown of the blood-brain barrier could thus be targets for treating Alzheimer's disease.

电针“内关”和“足三里”对脑梗死大鼠神经损伤修复及Orexin-A、炎性因子表达的影响

目的:观察电针“内关”和“足三里”对脑梗死大鼠神经损伤修复及食欲素A(Orexin-A)、血清炎性因子表达的影响。方法:54只成年雄性SPF级大鼠随机分为假手术组、模型组和电针组,电针组和模型组制备大脑中动脉闭塞(MCAO)模型,24 h后电针组大鼠取双侧“内关”和“足三里”电针治疗14 d。假手术组仅做颈部皮肤切开缝合处理。各组做神经功能缺损评分、称重,取材后行TTC、HE和尼氏染色,蛋白印记和荧光定量PCR检测Orexin-A表达。采用酶联免疫吸附试验(ELISA)法检测血清Orexin-A、血清炎性因子(TNF-α、IL-6、IL-1β)等。结果:与假手术组相比,模型组神经功能缺损评分和脑梗死体积升高,体重降低(P<0.05),模型组神经元数量、血清Orexin-A表达和脑组织Orexin-A蛋白及mRNA表达量明显降低,血清炎性因子水平明显升高(P<0.01);与模型组相比,电针组神经功能缺损评分和脑梗死体积降低,体重升高(P<0.05),电针组神经元数量、血清Orexin-A表达和脑组织Orexin-A蛋白及mRNA表达量明显升高,血清炎症因子水平明显降低(P<0.01)。模型组大鼠脑组织完整神经细胞数量减少,细胞胞核分离,电针组神经细胞形态相对完整,趋于正常。结论:电针疗法可以改善脑梗死大鼠的神经功能缺损情况,减小脑梗死体积,改善体重情况,其机制可能与调节Orexin-A水平,抑制血清炎性因子产生,促进神经损伤修复有关。

下丘脑泌素／进食素（Hypocretin／orexin）与睡眠：发作性睡病的病理生理和诊断

综述目的：发作性睡病是一种睡眠障碍，临床特征是白天过度嗜睡和猝倒。研究发现大多数病人存在下丘脑神经肽-hypocretin-1的缺乏。这项发现推动了该研究的进展。最近研究：对发作性睡病和其他一些睡眠障碍病人的脑脊液hypocretin-1水平的研究显示，hypocretin缺乏对发作性睡病／猝倒具有高度敏感性和特异性。约有15％的发作性睡病病人，尽管其多次小睡潜伏期实验是阴性的，但其hypocretin的水平是降低的。hypocretin系统除了调节睡眠，还参与了能量平衡、植物神经功能和一些神经内分泌功能的调节。因而多达1／3的病人有肥胖(体重指数>30)。此外，无论体重是否超重，血致瘦素水平均降低。而新的发作性睡病的啮齿类动物模型的建立也许有助于对这些内分泌异常的了解。最后，对于hypocretin系统在睡眠和觉醒调节方面的生理作用的研究也在不断增加。摘要：hypocretin的测定有可能作为一种新的诊断方法，结合临床对发作性睡病进行诊断。发作性睡病病人的临床处理中，应注意其常见的伴发病肥胖。将来，拟hypocretin药物的可能出现为该病的治疗提供新的途径。而具有发作性睡病特征的的动物模型的建立毫无疑问会增加我们对这种疾病病理生理方面的认识。

血清FGF1、Orexin A水平与妊娠期糖尿病的相关性研究

目的研究妊娠期糖尿病(gestational diabetes mellitus,GDM)患者血清成纤维细胞生长因子1(fibroblast growth factor 1,FGF1)、食欲素A(Orexin A)水平与糖脂代谢、炎性细胞因子及胰岛素抵抗的相关性。方法随机选取2021年12月~2022年6月在徐州医科大学附属医院产科进行规范产检并分娩的50例足月妊娠(37~40周)GDM孕妇为研究组;选取同期正常妊娠的50例孕妇为对照组。检测两组血清FGF1、Orexin A水平,测定糖脂代谢、炎性细胞因子及胰岛素抵抗相关指标水平。分析GDM孕妇血清FGF1及Orexin A水平与糖脂代谢、炎性细胞因子及胰岛素抵抗相关指标的相关性。结果研究组产前体重指数(body mass index,BMI)、空腹血糖(fasting plasma glucose,FPG)、糖化血红蛋白(glycated hemoglobin,HbA1c)、总胆固醇(total cholesterol,TC)、甘油三酯(triglyceride,TG)、低密度脂蛋白胆固醇(low-density lipoprotein cholesterol,LDL-C)、肿瘤坏死因子-α(tumor necrosis factor-α,TNF-α)、白细胞介素-6(interleukin-6,IL-6)、空腹胰岛素(fasting insulin,FINS)、胰岛素抵抗指数(homeostasis model assessment of insulin resistance,HOMA-IR)、FGF1水平均高于对照组(均P<0.05)。而高密度脂蛋白胆固醇(high-density lipoprotein cholesterol,HDL-C)、胰岛β细胞功能指数(homeostasis model assessment beta-cell function index,HOMA-β)、Orexin A水平低于对照组(P均<0.05)。Pearson相关性分析结果显示,研究组血清FGF1水平与产前BMI、HbA1c、FPG、TC、TG、LDL-C、TNF-α、IL-6、FINS、HOMA-IR均呈正相关,而与HDL-C、HOMA-β呈负相关(P均<0.05)。研究组患者血清Orexin A水平与HbA1c、FPG、TC、TG、LDL-C、TNF-α、IL-6、FINS、HOMA-IR均呈负相关,而与HOMA-β呈正相关(P均<0.05)。多元线性回归分析提示,产前BMI、HbA1c、TC、TNF-α是GDM患者血清FGF1的独立影响因素(P均<0.05);HbA1c、TNF-α、HOMA-β是GDM患者血清Orexin A的独立影响因素(P均<0.05)。结论GDM患者血清中高水平的FGF1表达及低水平的Orexin A表达与GDM所致的糖脂代谢紊乱、炎性反应及胰岛素抵抗有一定关联,未来可能成为GDM潜在治疗靶点。

食欲素受体拮抗剂类抗失眠药物的研究进展

随着现代社会生活节奏的加快,失眠的患病率逐渐增加,长期失眠会严重影响个人的工作和生活。目前临床常用的改善失眠症状的药物主要为镇静催眠药。作为新一代抗失眠药物,食欲素受体拮抗剂可以增加睡眠各阶段的持续时间、减弱觉醒信号从而抑制清醒状态而非诱导镇静,从而可以有效避免传统镇静催眠药物的一些缺点。本研究对食欲素受体拮抗剂中3个明星药物suvorexant、lemborexant、daridorexant的有效性和安全性进展进行综述,以期为治疗失眠提供参考。

Orexin-A对急性乙醇中毒昏迷大鼠的实验性促醒疗效研究

目的建立大鼠急性乙醇中毒昏迷模型,观察orexinA对昏迷动物的促醒作用。方法取成年雌性SD大鼠74只,分别通过腹腔注射乙醇的方法建立大鼠急性乙醇中毒昏迷实验模型。通过翻正反射判断大鼠意识状态的改变;通过脑电图判断脑电活动变化。结果给予腹腔注射32%乙醇(14ml/kg)后,大鼠行为状态和脑电图变化符合昏迷诊断标准。同对照组比较,高剂量orexinA治疗组(7.70nmol/kg)大鼠翻正反射消失持续时间明显缩短,行为觉醒改变较为显著,而低剂量治疗组(3.85nmol/kg)行为变化不明显。此外,给予高剂量orexinA可引起大鼠脑电活动改变,同给药前比较,δ波显著减少。结论侧脑室使用orexinA对昏迷大鼠具有促醒治疗作用。

Orexin A对麻醉大鼠前额叶皮层神经元单位放电的影响及其机制研究

目的研究orexinA对麻醉大鼠前额叶皮层神经元自发放电的影响,并初步探讨其作用机制。方法用玻璃微电极记录大鼠前额叶皮层神经元的单位放电,分别观察侧脑室给予orexinA、组胺H1受体拮抗剂pyrilamine、以及pyrilamine+orexinA后放电活动的变化。结果侧脑室给orexinA溶液可明显增加前额叶皮层神经元的自发放电频率;而给pyrilamine对前额叶皮层神经元自发放电频率无显著影响;给予pyrilamine预处理后,orexinA未能引起前额叶皮层神经元放电频率发生改变。结论OrexinA对麻醉大鼠前额叶皮层神经元放电活动有明显的兴奋性,这一作用可能与活跃的组胺能系统有关。

Orexin-A对氯胺酮-咪达唑仑麻醉大鼠的促醒作用研究

目的研究侧脑室注射orexin-A对氯胺酮-咪达唑仑麻醉大鼠的促醒作用。方法腹腔注射氯胺酮(75mg/kg)和咪达唑仑(5mg/kg)麻醉大鼠后,侧脑室注射不同剂量orexin-A,以脑电δ波比例评价麻醉深度,以大鼠翻正反射消失(LRR)持续时间评价麻醉时间,以共济失调期评价运动功能恢复。结果同对照组相比,高剂量orexin-A治疗组(4nmol)麻醉大鼠脑电δ波比例明显降低(P<0.01),LRR持续时间和共济失调期明显缩短(P<0.01);而低剂量orexin-A治疗组(1nmol)无明显变化(P>0.05)。结论侧脑室注射orexin-A可使麻醉深度变浅,麻醉时间缩短,并可促进麻醉后运动功能恢复,从而发挥了对麻醉的促醒作用。