Beta-endorphin in serum and seminal plasma in infertile men

Aim： To access beta-endorphin levels in serum as well as seminal plasma in different infertile male groups. Methods： Beta-endorphin was estimated in the serum and seminal plasma by enzyme-linked immunosorbent assay （ELISA） method in 80 infertile men equally divided into four groups： non-obstructive azoospermia （NOA）, obstructive azoospermia （OA）, congenital bilateral absent vas deferens （CBVAD） and asthenozoospermia. The results were compared to those of 20 normozoospermic proven fertile men. Results： There was a decrease in the mean levels of betaendorphin in the seminal plasma of all successive infertile groups （mean ± SD： NOA 51.30 ± 27.37, OA 51.88 ± 9.47, CBAVD 20.36 ± 13.39, asthenozoospermia 49.26 ± 12.49 pg/mL, respectively） compared to the normozoospermic fertile control （87.23 ± 29.55 pg/mL）. This relation was not present in mean serum level of beta-endorphin between four infertile groups （51.09 ± 14.71, 49.76 ± 12.4, 33.96 ± 7.2, 69.1 ± 16.57 pg/mL, respectively） and the fertile control group （49.26 ± 31.32 pg/mL）. The CBVAD group showed the lowest seminal plasma mean level of beta-endorphin. Testicular contribution of seminal beta-endorphin was estimated to be approximately 40%. Seminal beta-endorphin showed significant correlation with the sperm concentration （r = 0.699, P = 0.0188） and nonsignificant correlation with its serum level （r = 0.375, P = 0.185） or with the sperm motility percentage （r = 0.470, P = 0.899）. Conclusion： The estimation of beta-endorphin alone is not conclusive to evaluate male reproduction as there are many other opiates acting at the hypothalamic pituitary gonadal axis.

Effect of naloxone on level of plasma beta-endorphin in neonates with severe asphyxia

β-endorphin is the most actively endogenous substance of cerebral endorphin. When combined with opiate receptor specially, it manifests a strong morphine-like activity and can decrease sensitivity of central nervous system to carbon dioxide so as to inhibit breath. OBJECTIVE： To observe the changes of content of plasma β-endorphin in neonates with severe asphyxia after naloxone treatment in a large dosage. DESIGN： Randomized controlled observation. SETTINGS： Department of Pediatrics, Shenzhen Shajing People＇s Hospital; Center of Pediatrics, Guangzhou Zhujiang Hospital. PARTICIPANTS： A total of 97 neonates with severe asphyxia including 57 boys and 40 girls were selected from Neonatal Intensive Care Unit, Department of Pediatrics, Shenzhen Shajing People＇s Hospital from January 2004 to November 2005. Their gestational age was （38±3） weeks, body mass was （3.2±1.7） kg, and hospitalization duration was （2.8±2.3） hours. All neonates met the diagnostic criteria of with severe asphyxia and all their parents provided the confirmed consent. METHODS： All neonates were treated with inspired oxygen, sedation, stopping terror, decreasing cranial pressure, maintaining a well blood perfusion and normal level of blood glucose （about 5.0 retool/L）. After hospitalization, 0.1 mg/（kg·d） naloxone hydrochloride （Beijing Sihuan Pharmaceutical Technology Co., Ltd.; certification： HI0900021; bullet preparation; 0.4 mg/ampoule） was intravenously dribbled into neonates for 4 - 6 hours, 14 days in total. 2 mL blood was collected from radial artery in neonates at the beginning of hospitalization and at 3 days after naloxone treatment, put in aprotinin-pre-cool tube, mixed evenly, and centrifuged at hypothermia. Plasma was maintained in refrigerator at - 70 ℃. The kit was provided by Neurobiology Department of Shanghai Second Military Medical University of Chinese PLA. Concentration of plasma β-endorphin was measured by using radio-immunity assay.All data were expressed as Mean ± SD and results were compared with paired t test. MAIN OUTCOME MEASURE： Concentration of plasma β-endorphin. RESULTS： All 97 neonates were involved in the final analysis. Concentration of plasma β-endorphin in neonates with severe asphyxia was lower after treatment as compared with that before treatment, and there was significant difference （t = 10.31, P 〈 0.01 ）. CONCLUSION： Naloxone can decrease level of plasma β-endorphin in neonates with severe asphyxia.

Correlating plasma endothelin-1 and beta-endorphin levels to nine risk factors of acute cerebral infarction

BACKGROUND： Several studies have confirmed that endothelin and endorphin are involved in the occurrence of cerebral vasospasm. However, the correlation of these factors to acute cerebral infarction-related risk factors needs to be confirmed. OBJECTIVE： To detect endothelin-1 （ET-1） and beta-endorphin （β -EP） levels in plasma of patients with acute cerebral infarction, and to analyze the correlations of these factors to smoking, alcohol abuse, hypertension, diabetes mellitus, diseased region, diseased degree, gender, and other factors related to acute cerebral infarction. DESIGN： A case-control observation. SETTING： First Department of Neurology, Guangdong Hospital of Traditional Chinese Medicine; Department of Neurology, Second Affiliated Hospital of Sun Yat-sen University. PARTICIPANTS： Sixty-nine inpatients with acute cerebral infarction were admitted to the Department of Neurology, Second Affiliated Hospital of Sun Yat-sen University （March 2003-January 2004） and First Department of Neurology, Guangdong Hospital of Traditional Chinese Medicine （March July 2004） and recruited for this study. All 69 inpatients corresponded to the diagnosis criteria of acute cerebral infarction, formulated in the National Working Conference of Cerebrovascular Disease in 1998, and were confirmed as acute cerebral infarction by CT/MRI. The patient group consisted of 35 males [（644- 12） years old] and 34 females[ （674- 13 ） years old]. Among them, 9 patients were smokers, 7 were alcohol users, 48 had a history of hypertension, and 16 had a history of diabetes mellitus. CT/MRI examinations revealed that 35 patients presented with left focus sites, 11 with right ones and 23 with bilateral ones. Following attack, 24 patients had Barthel Index Scale grading 〈 40 points, 21 patients 40-50 points, and 24 patients 〉 60 points. An additional 59 healthy individuals, who received health examinations simultaneously, were included as controls. Among the control subjects, there were 37 males [（62±10） years old] and 22 females [（65±11） years old]. Among them, 7 patients were smokers, and 6 were alcohol users. All controls had no history of stroke, hypertension, or diabetes mellitus. Informed consents of laboratory measurements were obtained from all subjects, and this study was approved by the Hospital Ethics Committee. METHODS： ① Following admission, all subjects were scored by Barthel Index Scale （BIS） and Hamilton Depression Scale. Meanwhile, hypertension, diabetes mellitus, gender, smoking, drinking, and other conditions were recorded. CT/MRI examination was conducted to identify the focus site.②On the 2^nd day after admission, ET-1 and β -EP plasma levels were measured with an automatic ET-1 and β -EP analysis kit. MAIN OUTCOME MEASURES： ET-1 and β -EP plasma levels and their correlation to acute cerebral infarction-related factors. RESULTS： Sixty-nine patients with acute cerebral infarction, and an additional 59 healthy individuals participated in the final analysis. β ET-1 [（63.80±27.65） ng/L vs. （46.50±9.36） ng/L, P 〈 0.05] and β - EP [（94.18±33.94） mg/L vs. （51.87±23.43） mg/L, P 〈 0.05] levels of the patient group were obviously higher than respective values of the control group. ② The ET-1 and β -EP levels of patients with cerebral infarction did not correlate to hypertension, diabetes mellitus, BIS, depression, cerebral infarct focus, disease course, gender, smoking or drinking （P 〉 0.05）. CONCLUSION： The ET-I and β-EP levels of patients with acute cerebral infarction increased, but they were not obviously associated with disease course, blood pressure, blood glucose, BIS, or other common cerebral infarction-related factors.

Thyrotropin－releasing hormone antagonizes the inhibitory effects of beta－endorphin on cardiovascular system

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Beta-内啡肽足爪注射对慢性炎性痛大鼠局部炎性因子的抑制作用

[目的]观察足爪注射beta-endorphin(Beta-END)对慢性炎性痛大鼠的治疗作用,探讨其对外周局部致炎性细胞因子Prostaglandin E2(PGE2)、Interleukin-1 beta(IL-1 beta)、Tumor Necrosis Factor-alpha(TNF-alpha)的基因和蛋白表达的干预作用。[方法]建立大鼠Complete Freund's Adju-vant(CFA)诱导的炎性痛模型,随机分为模型对照组和beta-END足爪局部注射组。Beta-END注射从模后1d至13d,隔日1次。观察痛阈(PWLs)变化,检测足爪炎症组织PGE2、IL-1 beta、TNF-alpha的mRNA和蛋白水平。[结果]与模型对照组比较,足爪局部注射beta-END能显著提高慢性炎性痛大鼠的痛阈,能显著降低IL-1 beta和TNF-alpha的蛋白水平,并对PGE2蛋白水平和PGE2、IL-1 beta、TNF-alpha mRNA表达呈现下调趋势。[结论]Beta-END足爪局部注射对慢性炎性痛大鼠具有良好的治疗作用,除传统的外周阿片受体机制外,其外周治疗慢性炎性痛的作用可能还与其有效抑制局部炎性因子的表达有关。

非自杀性自伤行为成瘾的研究进展

非自杀性自伤是一个严重的临床问题,由心理、社会和生物学因素交互作用所致,最常发生于青少年及成年早期。心理和社会因素一定程度上指导了自我伤害心理社会干预方法。非自杀性自伤的生物学机制尚不明确,部分患者自伤行为具有成瘾特点,导致纠正和治愈困难。本文就非自杀性自伤行为成瘾的生物学机制、风险因素、共病疾病及治疗措施等研究进展作一综述。

脊髓电刺激治疗带状疱疹后神经痛患者血清β-EP、NT水平变化及对治疗反应性的评估价值

目的探讨脊髓电刺激(Spinal cord stimulation,SCS)治疗带状疱疹后神经痛(Postherpetic neuralgia,PHN)患者血清β-内啡肽(β-endorplhin,β-EP)、神经降压素(Neurotensin,NT)水平变化及对治疗反应性的评估价值。方法选取2021年7月-2023年3月武汉市新洲区人民医院接受SCS治疗的PHN患者108例作为研究组,根据治疗6个月效果分为反应良好患者、反应差患者。根据随机病例对照研究原则1∶1选取同期常规药物治疗的PHN患者108例作为对照组。检测并比较两组血清β-EP、NT水平及对治疗反应性的评估价值。结果治疗前,两组血清β-EP、NT水平比较,差异无统计学意义(P>0.05);治疗后,两组血清β-EP、NT水平较治疗前均升高,且研究组高于对照组(P<0.05)。皮疹面积≥10 cm^(2)、初治时间>3 d是PHN治疗反应差的独立危险因素,血清β-EP、NT水平升高是PHN治疗反应差的独立保护因素(P<0.05)。受试者工作特征(Receiver operating characteristic curve,ROC)分析显示,血清β-EP、NT水平单独预测PHN治疗反应差的曲线下面积(Area under curve,AUC)值分别为0.776、0.793,加入多因素Logistic回归模型后可将AUC值提升至0.936,高于血清β-EP(Z=3.490,P=0.001)、NT(Z=3.430,P=0.001)单独预测。结论SCS治疗可提升PHN患者血清β-EP、NT水平,二者联合检测可为临床评估SCS疗效提供参考。

脐针“山泽通气”疗法对急性肾绞痛内源性致痛因子影响的研究

目的从脐针治疗前后的内源性致痛因子含量变化,探索脐针治疗肾绞痛的效果和机制。方法收集2021年1月至2022年12月在福建中医药大学附属第三人民医院急诊科及门诊就诊的150例急性肾绞痛患者,根据随机数字表法分为观察组(采用脐针“山泽通气”法治疗)和对照组(采用地佐辛肌内注射),每组各75例。比较两组患者疼痛量表、血清致痛因子和镇痛因子水平及临床疗效。结果两组患者治疗前视觉模拟评分法(Visual Analogue Scale,VAS)评分和现时疼痛强度(Present Pain Intensity,PPI)评分均无显著差异(P>0.05)。治疗后,VAS评分和PPI评分均显著降低(P<0.001),且和对照组相比,观察组评分下降更显著(P<0.001)。治疗前,两组患者血清致痛因子P物质、5-羟色胺、镇痛因子β-内啡肽水平无显著差异(P>0.05);治疗后,观察组患者血清致痛因子P物质和5-羟色胺水平均显著升高(P<0.001),镇痛因子β-内啡肽水平显著降低(P<0.001);且和对照组相比,观察组血清P物质和5-羟色胺升高更显著,β-内啡肽下降更明显(P<0.001)。观察组临床有效率为94.67%,显著高于对照组的80.00%(P=0.007)。结论脐针“山泽通气”法治疗急性肾绞痛可明显降低患者疼痛感、降低内源性致痛因子水平,临床疗效显著。

β－内啡肽在新生鼠缺氧缺血性脑损伤中的作用

本实验观察到新生鼠缺氧缺血后，皮层β－内啡肽（β─Ｅｐ）含量显著增多，与此同时，皮层比重显著降低，两者呈显著相关；注射适量的纳洛酮或β─Ｅｐ抗血清，可显著减轻皮层水肿；注射β─Ｅｐ，则可加重皮层水肿。提示β─Ｅｐ可能参与新生鼠缺氧缺血性脑损伤的病理过程。

隔物灸对寒湿凝滞型原发性痛经患者经期血浆β-EP含量的影响

目的:探讨隔物灸治疗寒湿凝滞型原发性痛经的作用机制。方法:以隔物灸治疗寒湿凝滞型原发性痛经患者105例(隔物灸组),并设中药月月舒作对照104例(药物组),观察临床疗效,同时对两组各40例进行了治疗前后经期β-内啡肽(β-EP)含量的变化检测。结果:隔物灸组总有效率为95.2%,优于药物组的85.6%(P<0.05);隔物灸组β-EP水平较治疗前明显升高(P<0.01)。结论:隔物灸对寒湿凝滞型原发性痛经患者有明显的治疗作用,其作用机制之一可能是通过调节血浆中β-EP的水平而发挥止痛效应。

头穴透刺治疗急性脑梗塞及对血浆中β-内啡肽含量的影响

选 1 0 0例急性脑梗塞患者 ,随机分为头穴透刺组 (治疗组 )和药物组 (对照组 )各 5 0例。治疗组用百会透前顶 ,率谷透悬厘 ;对照组先后用川芎嗪和脑复康注射液静滴。结果 :在显效率上 ,治疗组较对照组疗效显著 (P <0 0 1 ) ;在改善偏瘫和失语积分中 ,治疗组优于对照组 ;在调节其血浆中 β EP含量上 ,两组均呈下降趋势 ,治疗组下降更明显 ,已接近正常值水平。表明头穴透刺治疗急性脑梗塞疗效显著 ,其作用机理可能是通过调节 β EP含量 。

纳络酮对缺氧缺血性脑病新生儿血浆神经肽Y和β-内啡肽的影响

目的探讨新生儿缺氧缺血性脑病(HIE)血浆神经肽Y(NPY)、β-内啡肽(β-EP)的变化及纳络酮治疗后对其的影响。方法将34例中、重度HIE患儿随机分成常规治疗组(18例),纳络酮治疗组(16例),以14例正常新生儿为对照组,纳络酮治疗组入院后在常规治疗的基础上给予纳络酮治疗,连用3天。HIE患儿组治疗前、治疗3d后各采血收集标本一次,采用放射免疫法测定NPY、β-EP。结果①HIE患儿血浆NPY、β-EP水平为(174.23±18.31)ng／L、(123.36±16.42)ng／L均显著高于正常对照组(87.19±12.95)ng／L、(63.27±12.65)ng／L(P<0.01)。HIE急性期NPY与β-EP呈正相关(r=0.347,P<0.05)。②HIE常规组、纳络酮组治疗3d后血浆NPY、β-EP水平均较治疗前显著降低(P<0.01)。治疗后HIE纳络酮组NPY、β-EP水平均显著低于常规组(P<0.01)。结论NPY、β-EP共同参与了HIE的病理生理过程,在HIE发病机制中可能起重要作用;纳络酮能显著降低NPY、β-EP水平,减轻脑损伤。

急性脑梗死患者不同时期Apelin-13及应激相关蛋白水平的变化及其与预后的关系研究

目的探讨急性脑梗死(ACI)患者不同时期Apelin-13和应激相关蛋白热休克蛋白70(HSP-70)、β内啡肽(β-EP)水平的变化及其与预后的相关性。方法选取2013年1月—2014年12月在复旦大学附属上海市第五人民医院确诊为ACI的患者50例作为ACI组,另选取同期在本院体检正常者40例作为对照组。采集两组受试者血液,并检测对照组和ACI组发病第1、3、7、14、21、30天Apelin-13、HSP-70、β-EP水平。ACI患者根据改良Rankin分级法评估预后,分为预后好(n=28)、一般(n=15)、差(n=7),并比较不同预后患者发病第1天的Apelin-13、HSP-70、β-EP水平、格拉斯哥昏迷量表(GCS)评分、急性生理学与慢性健康状况评分系统Ⅱ(APACHEⅡ)评分、美国国立卫生研究所卒中量表(NHISS)评分、洼田饮水试验分级。结果对照组、ACI组不同时期Apelin-13、HSP-70水平比较,差异有统计学意义(P<0.05),β-EP水平比较差异无统计学意义(P>0.05);其中ACI组第1天Apelin-13水平低于对照组,ACI组第14、21、30天Apelin-13水平高于ACI组第1天(P<0.05);ACI组第1、3天HSP-70水平高于对照组,ACI组第3、7、14、21、30天HSP-70水平低于ACI组第1天(P<0.05)。ACI患者Apelin-13与HSP-70呈直线负相关(r=-0.909,P=0.012),Apelin-13与β-EP无直线相关性(r=-0.172,P=0.744),HSP-70与β-EP无直线相关性(r=0.121,P=0.820)。不同预后ACI患者β-EP水平比较,差异无统计学意义(P>0.05);不同预后ACI患者Apelin-13、HSP-70水平、GCS评分、APACHEⅡ评分、NHISS评分、洼田饮水试验分级比较,差异均有统计学意义(P<0.05);其中预后差者Apelin-13水平、GCS评分均低于预后好和预后一般者,HSP-70水平、APACHEⅡ评分、NHISS评分、洼田饮水试验分级高于预后好和预后一般者(P<0.05);预后一般者GCS评分低于预后好者,APACHEⅡ评分、NHISS评分、洼田饮水试验分级高于预后好者(P<0.05)。结论Apelin-13水平在ACI发病第1天降低,随ACI病程逐渐升高;HSP-70水平在ACI发病第1天升高,随ACI病程逐渐下降。预后差的ACI患者发病第1天的Apelin-13水平、GCS评分低于预后一般和预后好者,而HSP-70水平、APACHEⅡ评分、NHISS评分、洼田饮水试验分级高于预后一般和预后好者,可以根据这些指标的变化判断ACI患者预后。

电针对佐剂性关节炎大鼠下丘脑CRH、IL-2、β-EP含量的影响

目的:探讨电针抗炎免疫调节作用机理,比较“大椎”“命门”穴与非穴间的作用差异。方法:以佐剂性关节炎大鼠(AA)为研究对象,随机分为5组:正常组、模型组、电针“大椎”组、电针“命门”组、电针非穴组。观察电针对关节炎症局部及下丘脑促肾上腺皮质激素释放激素(CRH)、β-内啡肽(βEP)、白细胞介素-2(IL-2)含量的影响,并比较不同穴位间的作用差异。结果:电针“大椎”组下丘脑CRH的含量较模型组降低(P<0.05),电针各组下丘脑β-EP、IL-2的含量与模型组比较差异无显著意义(P>0.05);而下丘脑CRH含量与IL2含量,下丘脑IL-2含量与βEP含量具有显著正相关关系(γ=0.886,γ=0.946)。“大椎”组、“命门”组足爪肿胀率较非穴组低(P<0.05)。结论:电针可能是通过下丘脑CRH、IL-2、βEP等因素的相互调节,起到抗炎免疫调节作用的。“大椎”“命门”抗炎作用优于非穴处。

脑出血与蛛网膜下腔出血后β-内啡肽和促性腺激素释放激素水平变化研究

目的动态观察脑出血(ICH)及蛛网膜下腔出血(SAH)后β-内啡肽、促性腺激素释放激素(GnRH)水平,探讨ICH、SAH丘脑应激反应的差异。方法分别选取2014年5月—2016年5月于重庆市中医院神经外科住院的符合纳入标准的自发性ICH患者38例为ICH组,自发性SAH患者26例为SAH组。同期选取于本院行腰穿麻醉术的无神经系统疾病患者20例为对照组。分别检测并记录对照组患者入院时血浆、脑脊液中β-内啡肽、GnRH水平,ICH组、SAH组患者入院时及入院1、3、7、14、30 d血浆、脑脊液中β-内啡肽、GnRH水平。结果 ICH组根据剔除标准剔除18例,最终纳入20例;SAH组根据剔除标准剔除6例,最终纳入20例。ICH组、SAH组入院时及入院1、3、7、14、30 d血浆、脑脊液β-内啡肽水平高于对照组(P<0.05);SAH组入院时及入院1、3、7、14、30d血浆、脑脊液β-内啡肽水平高于ICH组(P<0.05)。ICH组、SAH组入院时及入院1、3、7、14、30 d血浆、脑脊液GnRH水平高于对照组(P<0.05);SAH组入院时及入院1、3、7、14、30 d血浆、脑脊液GnRH水平高于ICH组(P<0.05)。结论β-内啡肽和GnRH参与ICH、SAH下丘脑应激反应,ICH下丘脑应激反应比SAH轻,监测血液、脑脊液β-内啡肽、GnRH水平对脑损伤程度判定及预后评估有重要临床意义。

纳洛酮对重型颅脑损伤大鼠的脑保护机制

目的颅脑损伤后血浆内啡肽(β-EP)、内皮素(ET)增高可加重继发性颅脑损伤,监视纳洛酮对实验性颅脑损伤大鼠β-EP、ET及脑水肿变化的影响,对探讨其治疗机制及临床应用有一定意义。方法Wister大鼠63只,随机分为实验组、对照组、空白组,自由落体法制作重型颅脑损伤模型。伤后半小时实验组大鼠腹腔注射纳洛酮(苏诺)10mg/kg,对照组注射生理盐水,分别于伤后1,3,8,24h处死,以干湿重法检测脑水肿的变化,放免法监测血浆β-EP、ET改变。结果实验组脑水肿程度较对照组轻,血浆β-EP、ET轻度升高,与对照组比有统计学差异。结论纳洛酮可以降低实验型重型颅脑损伤大鼠血浆β-EP、ET的浓度,减轻脑水肿,起到脑保护的作用。

运动训练对应激大鼠中枢和外周β-内啡肽含量的影响

为了研究运动训练对大鼠应激后中枢和外周β－内啡肽（β－ＥＰ）含量的变化，对大鼠进行为期８周的运动训练，并在运动训练后期给予２１天的冷刺激，测定大鼠下丘脑和血清中β－ＥＰ的含量。结果发现：①经过２１天的冷应激后，大鼠产生显著的身心变化，下丘脑和血清β－ＥＰ的含量均显著升高，从而表明冷应激可使机体β－ＥＰ的合成和释放增多。参与调节机体的应激反应。②经过８周的运动训练后，大鼠下丘脑β－ＥＰ含量显著升高，血清β－ＥＰ含量显著下降；而对运动训练的大鼠施加冷刺激后，大鼠下丘脑和血清中β－ＥＰ含量显著低于应激组，以中等负荷运动训练组最为明显。从而表明运动训练可以减少内源性β－ＥＰ的释放，有效对抗大鼠机体对冷刺激产生的应激反应，维持机体在应激状态下内分泌功能的稳定。

中药芪参复康对焦虑模型大鼠β-EP及细胞因子的影响

目的:对中药芪参复康(QSFK)胶囊抗焦虑作用的神经-免疫调节机制进行初步探讨.方法:采用国际通用的高架十字迷宫模型(EPM)焦虑动物模型,用丁螺环酮(Bus)作对照,观察QSFK对EPM大鼠β-EP,血清NO,IL-1β,IL-6和TNFα的影响.结果:与模型组比较,QSFK和Bus均能降低EPM大鼠血浆β-EP含量(P<0.01),对下丘脑β-EP水平无明显影响;但两组均能升高EPM焦虑模型大鼠血清NO水平(P<0.05);QSFK还可升高EPM大鼠血清IL-1β和TNFα水平,对IL-6含量无明显影响;Bus并不能改变此焦虑模型大鼠的血清细胞因子水平.结论:QSFK降低血浆β-EP含量,提高血清NO浓度和EPM血清IL-1β和TNFα水平,以调节焦虑状态下机体免疫功能紊乱.

右美托咪啶在颅脑创伤应激控制中的作用及其对神经内分泌的影响

目的评估右美托咪啶在中重度颅脑创伤（TBI）患者应激控制中的作用及其对神经内分泌功能的影响。方法2009年5月-2012年1月成都军区昆明总医院收治的TBI患者90例[格拉斯哥评分（GCS）6～13分1，依入院顺序随机分为3组，采用不同镇痛镇静方案。A组（n=32）：右美托眯啶负荷量0．5～1．0μg／kg，30min内注完，0．2～0．6μg／（kg．h）维持24h，效果不佳者加用吗啡静脉注射；B组（n=31）：异丙酚负荷量0．5～2．0mg／kg，10min注完，1．0～3．0mg／（kg．h）维持72h，效果不佳者加用吗啡静脉注射；C组（n=27）：空白组，采用哌替啶等肌内注射作为临时用药。采用Riker镇静和躁动评分，结合生理与躯体反应阳性指标进行综合评估，监测血压、心率、呼吸、潮气量以及动脉血气、血浆皮质醇、血浆β内啡肽（β-EP）、外周血白细胞计数（WβC）、血糖变化等，并进行组间比较。结果A、B、C组单独用药（即不加用吗啡时）的镇静有效率分别为86．7％、80．6％、77．8％，组间比较差异无统计学意义。与给药前比较，给药后0．5hA组平均动脉压（MAP）下降（P〈0．05），余各时间点3组血压、心率及呼吸功能与给药前比较无明显差异（P〉0．05）。给药后24h时间点A组WβC、C组皮质醇水平低于给药前，余各时间点3组WBC、血糖、皮质醇及β-EP水平与给药前比较无明显差异（P〉0．05）。结论右美托咪啶可控制中重度颅脑伤后的过度应激反应，其抗应激及镇静效果与异丙酚类似，但需监测血压变化。β-EP可能在右美托咪啶的早期作用中发挥协同作用。

抗阿片肽血清对催产素增强电针镇痛的影响

本工作观察了大鼠侧脑室注射抗阿片肽血清对催产素增强电针镇痛作用的影响。脑室注射抗Beta-内啡肽血清(AEPS)使电针镇痛效应明显降低,但在注射催产素前预先注射AEPS对催产素增强电针镇痛作用无明显影响。注射抗强啡肽Al-13血清使电针镇痛明显降低,但却使催产素增强电针镇痛作用明显增强。无论抗甲-脑啡肽血清还是抗亮-脑啡肽血清对电针镇痛都无明显影响,对催产素增强电针镇痛的作用也不产生影响。上述结果说明,催产素增强电针镇痛的作用虽被脑内强啡肽Al-13部分对抗,但不受Beta-内啡肽和脑啡肽的影响,表明催产素增强针刺镇痛的作用不依赖于脑内内源性阿片肽系统。