Low utility of plasma Nociceptin/orphanin FQ in the diagnosis of hepatocellular carcinoma

AIM： The utility of serum alpha-fetoprotein （α-FP） in the detection of hepatocellular carcinoma （HCC） is questionable. Very high circulating levels of nociceptin/ orphanin FQ （N/OFQ）, a ligand for a novel opioid receptor, have recently been reported in HCC. The aim of this study was to assess the role of plasma N/OFQ in the diagnosis of HCC arising in patients with liver cirrhosis. METHODS： Plasma N/OFQ levels were measured by ELISA in 58 patients （28 HCC and 30 liver cirrhosis） and in 25 healthy controls. The values were correlated with clinical and laboratory features including α-FP. Spearman index, biserial correlation coefficient, non parametric combination （NPC） test and discriminant stepwise analysis were used for statistical evaluation of data.RESULTS： The upper normal limit of nociceptin was 122 pg/mL. Plasma levels above this cut-off were found in 21.4% of patients with HCC, in 23.3% of those with cirrhosis and in 8% of healthy subjects. α-FP serum levels〉200 ng/mL were found in 46.4% of the patients with HCC and in none of those with cirrhosis. No correlation was found between N/OFQ levels and any of the clinical and laboratory features, including α-FP. By NPC test, HCC and cirrhotic patients were different with regard to α-FP （P = 0.000） but not in terms of nociceptin （P = 0.595）. By point biserial correlation, HCC presence was positively correlated with α-FP （rpb = 0.52, P = 0.000） but not with N/OFQ （rpb = 0.16, P = 0.157）. In a discriminant analysis, α-FP was significant in the Wilks test （Y = -0.709 ＋ 0.03 α-FP） and properly classified 81% of all patients and 61% of HCC. N/OFQ had lower sensitivity, specificity and predictive values than α-FP. CONCLUSION： Nociceptin is increased in patients with chronic liver disease, independently of the presence of HCC, although the underlying mechanism has yet to be clarified. We conclude it is not a useful marker for HCC.

Functional expression of opioid receptor-like receptorand its endogenous specific agonist nociceptin/orphanin FQ during mouse embryogenesis

Expression of opioid receptor-like receptor (ORL1)and its endogenous peptide agonist nociceptin/orphaninFo (N/OFQ) during mouse embryogenesis have been investigated. Transcripts of ORL1 and N/OFQ were detected by RT-PCR in mouse brain of day 8 embryo (E8)and the expression continued afterwards. Northern blotanalysis revealed abundant expression of ORL1 at postnatal day 1 (P1) and N/OFQ at E17 and P1 in the brain butnone was detected in other embryonic tissues. The presence of functional ORL1 in mouse embryonic brain wasalso confirmed by specific binding of [3H] N/OFQ (kd=1.3±0.5 nM and Bmax = 72±9 fmol/mg protein) as wellas by N/OFQ-stimulated G protein activation.

POTENT HYPOTENSIVE EFFECTS OF ORPHANIN FQ IN CONSCIOUS STROKE-PRONE SPONTANEOUSLY HYPERTENSIVE RATS

Orphanin FQ（OFQ） or nociceptin is a novel neuropeptide consisting of 17 amino acids. This peptide has a primary structure reminiscent of that of opioid peptide but exhibits an opposite effect to make animals hyperreactive. The effect of this new peptide on cardiovascular function are not completely known. The present study was conducted to investigate the effect of intravenous bolus injection of orphanin FQ on mean arterial blood presure （MABP） in conscious stroke-prone spontaneously hypertensive rats (SHRsp). Adult male SHRsp and Wistar normotensive rats （250～300 g body weight, 2. 5～3 months old） were used in this study. The MABP was measured in the conscious state by a tail-cuff method. In SHRsp model, intravenous bolus injection of orphanin FQ or Tyr1-orphanin FQ （0. 5 mg/kg） induced a prolonged and marked reduc- tion in MABP. The maximum changes in MABP were -30. 2±4. 2 mmHg by orphanin FQ and -28. 2± 4. 7 mmHg by Tyr1-orphanin FQ at 10 min after administration,and this effect lasted over 30 min. The Phe1→Tyr substitution in orphanin FQ was found to retain almost fully hypotensive activity. Pretreatment of SHRsp with naloxone-HCI（60 μg/kg）, 5 min before the injection of orphanin FQ, did not block the hy- potensive effect of orphanin FQ. Therefore, opioid receptors could not account for the hypotensive effect of orphanin FQ in SHRsp. In Wistar rats, intravenous bolus injection of the same dose of orphanin FQ did not cause a change in MABP. These observations suggest that orphanin FQ is a novel hypotensive peptide and may have some role in the regulation of blood pressure in SHRsp, rather than in normotensive rats. The ex-act underlying mechanisms are waiting to be clarified.

PERIPHERAL TISSUE DISTRIBUTION OF ORPHANIN FQ PRECUSOR mRNA IN STROKE-PRONE SPONTANEOUSLY HYPERTENSIVE RATS

The heptadecapeptide orphanin FQ (OFQ) is a recently discovered neuropeptide that exhibits structural features reminiscent of the opioid peptides and that is an endogenous ligant to a G protein-coupled receptor sequentially related to the opioid receptors. OFQ was originally isolated from brain, but the presence of OFQ in peripheral tissues, especially in cardiovascular system, has not been clarified. The present study was designed to investigate the peripheral tissue distribution of OFQ precusor mRNA in stroke-prone spontaneously hypertensive rats (SHRSP) and compare the difference of OFQ precusor mRNA expression in aorta or cultured vascular smooth muscle cells (VSMCs) between SHRSP and wistar-Kyoto normotensive (WKY) rats. By using quantitative reverse transcription-polymerase chain reaction (RT-PCR), OFQ precusor mRNA was detected in aorta and ovary at high levels comparable with the amounts found in brain. Moderate expression was found in testis, while a little OFQ precusor mRNA could be detected in atrium. All other peripheral tissues examined from SHRSP, including ventricle, liver, lung and kidney, showed no expression of OFQ precusor mRNA. In the vascular system, OFQ precusor mRNA was expressed in aorta, pulmonary artery, renal artery and vein at high levels comparable with the amounts found in brain. We also found that OFQ precusor mRNA levels were much higher in aorta or cultured VSMCs from SHRSP than those from WKY rats. In conclusion, the present study has shown that OFQ precusor mRNA is present in some peripheral tissues, especially in cardiovascular and reproductive system, suggesting that OFQ possibly involves in the regulation of cardiovascular and reproductive functions.

孤啡肽改善尼古丁戒断大鼠的焦虑样行为及其对HPA轴与炎症因子的调控机制

目的:探讨孤啡肽(nociceptin/orphanin FQ,N/OFQ)对尼古丁(nicotine,NIC)戒断大鼠焦虑样行为的改善作用及其对下丘脑-垂体-肾上腺(hypothalamic-pituitary-adrenal,HPA)轴神经递质与炎症因子表达的调控机制。方法:成年雄性Sprague-Dawley大鼠32只,随机分为正常对照组、NIC戒断模型组、N/OFQ低剂量治疗组和N/OFQ高剂量治疗组,每组各8只。模型组和N/OFQ治疗组大鼠每次皮下注射NIC(0.4 mg/kg),每天2次,连续7 d,然后戒断3 d制备大鼠尼古丁戒断焦虑模型。戒断期间N/OFQ低、高剂量治疗组大鼠每天一次侧脑室注射N/OFQ 1nmol和N/OFQ 10 nmol,连续3 d。第3次给药10 min后,利用旷场实验(open filed,OF)和高架十字迷宫实验(elevated plus maze,EPM)检测大鼠行为学变化;ELISA检测血清中促肾上腺皮质激素释放激素(corticotrophin-releasing hormone,CRH)、促肾上腺皮质激素(adrenocor ticotropic hormore,ACTH)和皮质酮(coritosterone,CORT)浓度以及血清中炎症因子肿瘤坏死因子α(tumor necrosis factor-α,TNF-α)、白细胞介素1β(interleukin-1β,IL-1β)和IL-6的浓度;用RT-qPCR检测大脑杏仁核中央核(centraln nucleus of amygdala,CeA)中TNF-α、IL-1β和IL-6的mRNA表达水平;HE染色光镜下观察海马组织CA1区神经元形态学变化;利用高效液相色谱检测大脑CeA的去甲肾上腺素(norepinephrine,NE)水平;利用Western blot检测大脑CeA的酪氨酸羟化酶(tyrosine hydroxylase,TH)蛋白表达。结果:与模型组比较,N/OFQ低、高剂量治疗组大鼠在OF中央区活动距离和活动时间显著升高(P<0.05或P<0.01),EPM的开放臂进入次数和停留时间百分率显著升高(P<0.05或P<0.01);同时,N/OFQ低、高剂量治疗组显著抑制NIC戒断大鼠血清中CRH、ACTH和CORT浓度(P<0.01);显著抑制血清中TNF-α、IL-1β和IL-6等炎症因子水平以及大脑CeA中TNF-α、IL-1β和IL-6 mRNA表达水平(P<0.05或P<0.01);N/OFQ低、高剂量治疗组显著减轻大鼠海马CA1区神经元损伤;并且显著降低NIC戒断大鼠大脑CeA中NE的水平和TH蛋白的表达(P<0.01)。结论:N/OFQ改善NIC戒断大鼠焦虑样行为,其机制通过HPA轴神经递质与炎症因子的调控所介导。

孤啡肽(OFQ)的分布、特性及其可能作用

孤啡肽是１９９５年底新发现的一种结构与内阿片肽类似的物质，它的发现引发了国际上相关研究的热潮。近年来的研究已经基本阐明了孤啡肽在中枢及外周的分布及其生化与药理特性，并初步发现该物质参与痛觉调制、影响运动与行为、调控递质释放，还可能参与情绪反应与学习记忆、神经内分泌与免疫过程以及胃的活动等，但其确切作用仍有待于进一步阐明。

孤啡肽与老年冠心病患者围术期心肌损伤的相关性研究

目的评价老年冠状动脉粥样硬化性心脏病(以下简称冠心病)患者围术期心肌损伤(perioperative myocardial injury,PMI)与血清孤啡肽(nociceptin/orphanin FQ,N/OFQ)含量的关系。方法纳入2022年1月至2023年5月在全身麻醉下行髋部骨折手术的老年患者120例,其中冠心病(冠心病组)与非冠心病(对照组)患者各60例。分别于麻醉诱导前10min(T_(0))、术后12h(T_(1))以及术后24h(T_(2))采集患者静脉血检测血清中N/OFQ以及高敏心肌肌钙蛋白I(high-sensitivity myocardial troponin I,hs-cTnI)含量,记录围术期不良心血管事件(perioperative adverse cardiovascular events,PACE)及术中血管活性药物的使用情况。结果与对照组比较,冠心病组患者T_(0)及T_(1)时刻N/OFQ及hs-cTnI含量显著升高(P<0.05),冠心病组和对照组患者T_(1)及T_(2)时刻N/OFQ与hs-cTnI含量呈正相关(P<0.05),冠心病组患者PACE及术中血管活性药物使用均多于对照组差异有统计学意义(P<0.05)。结论老年冠心病患者术后N/OFQ含量升高与PMI存在正相关性,可能成为PMI的早期预测指标。

ERK-1/2对N/OFQ调节大鼠皮层神经元延迟整流钾电流激活动力学的影响

目的研究ERK-1/2对N/OFQ调节大鼠皮层神经元延迟整流钾电流(IK)激活动力学的影响,初步探讨N/OFQ调节大鼠皮层神经元IK的ERK-1/2途径。方法研究采用全细胞膜片钳技术,观察ERK-1/2特异性抑制剂U0126对N/OFQ调节大鼠皮层神经元IK激活动力学的影响。结果在ERK-1/2抑制剂U0126存在情况下,IK激活曲线的V1/2由给药前的(-42±3.7)mV向超极化方向移动为(-39.9±5.9)mV(P<0.01)。IK激活曲线的κ由给药前的(21.6±8.1)mV变为给药后的(22.9±3.8)mV(P<0.05)。结论 U0126可以显著抑制N/OFQ对IK激活曲线的影响。

孤啡肽OFQ的溶液构象研究

应用近代NMR波谱技术对孤啡肽OFQ及其片段OFQ_(8-17)的溶液结构进行了比较研究,测定了孤啡肽OFQ和片段OFQ_(8-17)在H_2O和TFE/H_2O两种溶剂条件下的2D-DQF-COSY,2D-TOCSY,2D-NOESY(ROESY)谱,完成了它们氨基酸残基的自旋系统识别和序列特异性归属,获得分子中质子化学位移的完全归属,根据NOE特征和主链偶合常数等结构参数确定了它们的特征二级结构,以NOE提供的距离约束,进行了距离几何,分子力学和分子动力学模拟,得到了孤啡肽OFQ在不同溶剂条件下的溶液结构.在H_2O溶剂中,孤啡肽OFQ在G3-F4-T5-G6处形成一复合型转角结构.在TFE/H_2O溶剂中,OFQ整个分子形成两亲性α-螺旋结构.而孤啡肽片段OFQ_(8-17)在这两种环境中均为伸展的无规结构.孤啡肽OFQ在类似膜环境(TFE/H_2O)下的α-螺旋结构可能为其活性构象.

急性脑梗塞并发脑心综合征患者血清内源性孤啡肽与血清S-100钙结合蛋白β水平变化的研究

目的观察急性脑梗塞并发脑心综合征患者血清内源性孤啡肽(N/OFQ)与血清S-100钙结合蛋白β(S100β)水平变化并探讨其意义。方法选取2022年3月至12月于山西医科大学第二医院确诊的急性脑梗塞患者120例为研究对象,根据其是否并发脑心综合征分为脑梗塞组60例和脑心综合征组60例。收集2组临床资料,检测各组的血清N/OFQ、S100β水平,左心室射血分数(LVEF)、N端脑钠肽前体(NT-proBNP)、肌酸磷酸激酶同工酶(CK-MB)、心肌肌钙蛋白I(cTnI)水平。比较两组血清N/OFQ、S100β水平的差异并分析与各临床指标之间的相关性,分析脑心综合征的危险因素,通过受试者工作特征(ROC)曲线分析N/OFQ、S100β联合预测因子对脑心综合征的预测价值。结果脑心综合征组血清N/OFQ、S100β水平明显高于脑梗塞组,差异均具有统计学意义(P<0.05)。脑心综合征患者大面积组血清N/OFQ、S100β水平高于小面积组、中面积组,中面积组血清N/OFQ、S100β水平高于小面积组,差异均具有统计学意义(P<0.05)。相关性分析显示,血清N/OFQ水平与S100β水平呈正相关(P<0.05);血清N/OFQ、S100β与CK-MB、NT-proBNP、cTnI均呈正相关(P<0.05),与LVEF呈负相关(P<0.05)。Logistic回归分析显示,N/OFQ、S100β、CK-MB、NT-proBNP、cTnI水平高是脑心综合征的危险因素;高LVEF是脑心综合征的保护因素。ROC曲线分析显示,N/OFQ、S100β、二者联合预测脑心综合征的曲线下面积分别为0.816、0.818、0.877(P<0.001)。结论血清N/OFQ、S100β与急性脑梗塞并发脑心综合征密切相关,联合检测对脑心综合征的预防和治疗具有很好的临床价值。

醒脑开窍针刺法治疗产后抑郁的临床疗效

目的:探讨醒脑开窍针刺法治疗产后抑郁(postpartum depression,PPD)的效果。方法:选取2022年1—9月石家庄市妇幼保健院收治的PPD患者80例,采用随机数字表法分为2组,每组各40例。对照组给予常规西药治疗,观察组给予醒脑开窍针刺法结合西药治疗,疗程为8周。统计2组患者的疗效、安全性,并比较2组患者治疗前、后的抑郁程度[汉密尔顿抑郁量表(Hamilton Depression Scale,HAMD)、爱丁堡产后抑郁量表(Edinburgh Postnatal Depression Scale,EPDS)]、性激素水平[孕酮(progesterone,P)、雌二醇(estradiol,E2)]和神经递质水平[5-羟色胺(5-hydroxytryptamin,5-HT)、孤啡肽(OFQ)]。结果:观察组的疗效和总有效率均高于对照组,差异有统计学意义(P<0.05);治疗8周后,2组患者的HAMD、EPDS评分及OFQ水平均较治疗前下降,观察组低于对照组,2组P、E2、5-HT水平均较治疗前升高,观察组高于对照组,差异有统计学意义(P<0.05)。结论:醒脑开窍针刺法治疗PPD疗效显著,能改善抑郁相关因子表达,降低抑郁程度,且安全性高。

产后抑郁症与孤啡肽及单胺类递质的相关性研究

目的 探讨孤啡肽 (OFQ)及单胺类递质与产后抑郁症的关系。方法 采用放射免疫法测定 2 5名健康产妇 (对照组 )及 17例产后抑郁症妇女 (抑郁组 )静脉血中孤啡肽及单胺类递质含量。结果 ①抑郁组及对照组血孤啡肽含量分别为 (2 7 39± 6 0 4 )ng/L及 (10 37± 3 6 5 )ng/L ,与对照组相比 ,抑郁组孤啡肽含量显著升高 (P <0 0 1) ;抑郁组及对照组血 5 羟色胺 (5 HT)含量分别为 (0 93± 0 2 1) μmol/L及 (1 4 3± 0 36 ) μmol/L ,二者间有显著差异 (P <0 0 5 ) ;抑郁组血多巴胺 (DA)含量为 (2 15± 0 4 1) μmol/L ,显著低于对照组 (P <0 0 5 )。②抑郁组孤啡肽与5 HT及DA含量呈显著负相关 (r为 0 6 0 1及 0 5 93,P <0 0 5 )。③抑郁组爱丁保产后抑郁量表总分 (EPDS)与OFQ含量呈显著正相关 (r为 0 5 12 ,P <0 0 5 ) ,与 5 HT、DA含量呈显著负相关 (r分别为 - 0 5 71及 - 0 5 2 6 ,P <0 0 5 )。结论 孤啡肽与产后抑郁症的发生发展密切相关。

孤啡肽对大鼠顶叶皮层神经元延迟整流钾电流的抑制作用

目的研究孤啡肽(orphanin FQ/nociceptin,OFQ/N)对大鼠顶叶皮层神经元延迟整流钾电流(IK)的影响,初步探讨其干扰学习记忆过程的离子机制。方法采用全细胞膜片钳技术,观察OFQ/N对急性分离的大鼠顶叶皮层神经元IK的作用。结果①OFQ/N明显抑制IK,并呈剂量依赖性(P<0.05)。②0.1μmol.L-1OFQ/N使IK的电流-电压(I-V)曲线降低(n=8,P<0.01)。③0.1μmol.L-1OFQ/N使IK激活曲线的半数激活电压(V1/2)和斜率因子(k)分别由给药前的(-43.4±6.1)mV和(11.5±1.1)mV变为给药后的(-19.1±4.6)mV和(17.3±3.2)mV(n=8,P<0.01)。④0.1μmol.L-1OFQ/N使IK失活曲线的半数失活电压(V1/2)和斜率因子(k)分别由给药前的(-68.8±2.6)mV和(16.5±1.7)mV变为给药后的(-76.8±2.8)mV(n=5,P<0.01)和(15.7±3.1)mV(n=5,P>0.05)。结论OFQ/N可抑制大鼠顶叶皮层神经元IK,使IK激活曲线右移,失活曲线左移。

PKC在孤啡肽抑制大鼠皮层神经元瞬时外向钾离子电流中的作用

目的研究蛋白激酶C(PKC)对孤啡肽(N/OFQ)抑制大鼠皮层神经元瞬时外向钾电流(IA)的影响,初步探讨N/OFQ抑制IA的PKC信号途径。方法采用全细胞膜片钳技术,观察PKC特异性抑制剂chelerythrine对N/OFQ抑制大鼠皮层神经IA的影响。结果①与0.1μmol/L N/OFQ单独作用时,对IA的抑制作用相比,在cherythrine预处理的大鼠皮层神经元,在-40～-15 mV电压范围内,N/OFQ使IA的I-V曲线升高,而在-15～+60 mV电压范围内使IA的I-V曲线明显降低(n=10,P<0.05);②在指令电压+60 mV时,给予N/OFQ使IA的电流值由(1778.51±239.50)pA降至(1175.1±257.03)pA(n=10,P<0.05),抑制百分率为(33.93±6.62)%,与N/OFQ单独作用引起的(23.20±2.17)%的抑制率相比,具有显著性差异(n=10,P<0.05)。结论在不同电压下,chelerythrine对N/OFQ抑制大鼠皮层神经IA的影响不同,说明PKC在N/OFQ抑制IA中的作用因不同电压而具有双向性。

孤啡肽诱导白血病细胞K562凋亡

本研究探讨孤啡肽对白血病细胞K562增殖的影响及诱导凋亡的作用,采用MTT(四唑氮蓝)法检测不同浓度的孤啡肽对K562细胞生长的影响,应用瑞氏染色、电子显微镜观察药物作用后K562细胞形态的改变,流式细胞术检测孤啡肽对K562细胞细胞凋亡作用,DNA琼脂糖凝胶电泳观察孤啡肽作用后K562细胞内DNA的损伤程度。结果表明10-6-10-13mol/L孤啡肽明显抑制K562细胞的生长,且存在时间依赖性,而剂量依赖性不明显;10-6-10-7、10-9、10-12mol/L孤啡肽作用72小时后显示明显的细胞毒作用。与对照组相比,10-9mol/L孤啡肽作用72小时后K562细胞出现典型凋亡特征;流式细胞术检测发现0、10-7、10-8、10-9mol/L孤啡肽作用72小时后出现凋亡峰,凋亡率分别为0%、22.8%、23.8%、26.5%;DNA琼脂糖凝胶电泳显示典型的梯状条带。结论孤啡肽能够抑制K562细胞增殖,诱导其凋亡。

脑内发现全新的阿片受体样受体及其内源性配体

１９９４年克隆了一种孤儿受体──阿片受体样（ＯＲＬ）受体。１９９５年又发现其内源性配体ＯＦＱ（试译：孤啡肽）或Ｎｏｃｉｃｅｐｔｉｎ（以试译：痛敏肽）。ＯＲＬ受体与已知的阿片受体有５０％同源性，ＯＦＱ则与强啡肽Ａ化学结构高度相似，这两系统在功能上可能既有相反的作用，又有相似的作用，其详情正在研究中。

孤啡肽基因敲除小鼠电针镇痛作用增强

目的 :孤啡肽是阿片受体样受体 (ORL1)的内源性配基 ,它能调节疼痛与镇痛反应以及针刺镇痛反应 ,但各个实验室所得结果各不相同。本文利用OFQ基因敲除的小鼠为工具 ,观察内源性OFQ在针刺镇痛中的作用。方法 :采用本实验室建立的小鼠电针方法 ,选用穴位足三里 (SP 36)与三阴交 (SP 6) ,电针参数采用韩氏仪恒流方波输出 ,强度 1.0 1.2 1.4mA ,每 10min递增一级。痛阈的改变以热辐射甩尾来评价。结果 :与野生型小鼠相比 ,OFQ基因敲除小鼠基础痛阈明显延长 ,对 10 0Hz电针镇痛反应显著增强 ,但不影响 2Hz电针镇痛。结论 :在整体情况下 ,内源性OFQ有紧张性的致痛敏作用 ,并对 10 0Hz针刺镇痛有拮抗作用。

孤啡肽和内吗啡肽在神经源性痛模型大鼠疼痛相关脑区的改变

目的 :检测孤啡肽 (nociceptin/orphaninFQ ,OFQ)和内吗啡肽 (endomorphins,EM )在神经源性痛模型大鼠疼痛相关脑区杏仁核、下丘脑、导水管中央灰质 (PAG)和纹状体的含量变化 ,以假手术大鼠为对照。方法 :利用大鼠L5/L6 脊神经结扎神经源性痛模型 ,采用放射免疫的方法 ,检测OFQ和内吗啡肽在疼痛相关脑区的变化。结果 :发现在下列脑区发生了显著变化 :(1 )内吗啡肽 1 (EM1 )含量在神经源性痛大鼠下丘脑较对照鼠增加了 38% ,纹状体降低了 41 % ,而在杏仁核和PAG与对照大鼠差异无显著性。(2 )内吗啡肽 2 (EM 2 )含量在神经源性痛大鼠PAG较对照大鼠增加了 778% ,在纹状体降低了 43 % ,而在杏仁核和下丘脑与对照大鼠差异无显著性。 (3)OFQ含量在在神经源性痛大鼠的杏仁核比对照大鼠增加了 841 % ,在PAG比对照大鼠增加了 459% ;而在下丘脑和纹状体与对照大鼠差异无显著性。结论 :神经源性痛引起中枢神经系统疼痛相关脑区EM 1、EM2和OFQ的含量发生改变。

孤啡肽对大鼠顶叶皮层神经元瞬时外向钾电流的抑制作用

目的:研究孤啡肽(N/OFQ)对大鼠顶叶皮层神经元瞬时外向钾电流(IA)的影响,初步探讨其作用的通道动力学机制。方法:采用全细胞膜片钳技术,观察N/OFQ对急性分离的大鼠顶叶皮层神经元IA的作用。结果:①0.1μmol/L N/OFQ使IA幅值由给药前的(5356.1±361.6)pA下降为(4113.3±312.7)pA,抑制率为23.20%±2.17%(P<0.01,n=10)。②0.1μmol/L N/OFQ使IA的电流-电压(I-V)曲线降低(P<0.01,n=10)。③0.1μmol/L N/OFQ使IA激活曲线的半数激活电压(V1/2)和斜率因子(κ)分别由给药前的(-9.2±2.5)mV和(20.4±2.3)mV变为给药后的(30.6±3.7)mV(P<0.01,n=8)和(22.6±2.1)mV(P>0.05,n=8)。④0.1μmol/L N/OFQ使IA失活曲线的半数失活电压(V1/2)和斜率因子(κ)分别由给药前的(-64.1±3.2)mV和(21.5±2.1)mV变为给药后的(-55.9±1.9)mV(P<0.05,n=5)和(19.6±2.2)mV(P>0.05,n=5)。结论:N/OFQ可抑制大鼠顶叶皮层神经元IA,使其激活曲线、失活曲线均右移。

孤啡肽对大鼠体内外结肠动力的影响

目的:探讨孤啡肽受体在结肠运动中的作用. 方法:采用大鼠离体结肠肌条张力测定法、在体结肠肌电测定、炭末推进试验等研究了孤啡肽受体的内源性配基——孤啡肽对大鼠结肠动力的影响．结果:孤啡肽(1-1000 nmol／L)剂量依赖性地引起离体结肠肌条的强直性收缩;孤啡肽(1 μg／ kg)iv诱导在体近端结肠的相位性收缩和基础张力的增加(t=2．41,P=0．02);孤啡肽(3 nmol／ kg)sc加速活性炭悬液通过结肠的转运(48．0± 1．24 vs 43．5±2．63,t=-4．5,P=0．008)．结论:孤啡肽通过一个神经性的非阿片受体介导的机制加速大鼠结肠的收缩和转运,孤啡肽在结肠生理功能中起了一定的作用．