Arginine vasopressin as a target in the treatment of acute heart failure

Congestive heart failure(CHF) is one of the most common reasons for hospitalization in the United States. Despite multiple different beneficial medications for the treatment of chronic CHF, there are no therapies with a demonstrated mortality benefit in the treatment of acute decompensated heart failure. In fact, studies of inotropes used in this setting have demonstrated more harm than good. Arginine vasopressin has been shown to be up regulated in CHF. When bound to the V1 a and/or V2 receptors, vasopressin causes vasoconstriction, left ventricular remodeling and free water reabsorption. Recently, two drugs have been approved for use that antagonize these receptors. Studies thus far have indicated that these medications, while effective at aquaresis(free water removal), are safe and not associated with increased morbidity such as renal failure and arrhythmias. Both conivaptan and tolvaptan have been approved for the treatment of euvolemic and hypervolemic hyponatremia. We review the results of these studies in patients with heart failure.

ARGININE VASOPRESSIN GENE EXPRESSION IN SUPRAOPTIC NUCLEUS AND PARAVENTRICULAR NUCLEUS OF HYPOTHALAMOUS FOLLOWING CEREBRAL ISCHEMIA AND REPERFUSION

Background. Our previous studies indicated that the increased arginine vasopressin(AVP) in ischemic brain regions of gerbils could exacerbate the ischemic brain edema. This experiments is further clarify the relation between AVP and cerebral ischemia at the molecular level. Methods. The contents of AVP, AVP mRNA, AVP immunoreactive(ir) neurons in supraoptic nucleus(SON) and paraventricular nucleus(PVN) after cerebral ischemia and reperfusion were respectively determined by radioimmunoassay(RIA), immunocytochemistry(ⅡC), situ hybridization and computed image pattern analysis. Results. The contents of AVP in SON, PVN were increased, and the AVP ir positive neurons in SON and PVN were also significantly increased as compared with the controls after ischemia and reperfusion. And there were very light staining of AVP ir positive neurons in the other brain areas such as suprachiasmatic nucleus (SC) and periventricular hypothalamic nucleus (PE), but these have no significant changes as compared with the controls. During different periods of cerebral ischemia (30～120 min) and reperfusion (30 min), AVP mRNA expression in SON and PVN were more markedly increased than the controls. Conclusions. The transcription of AVP gene elevated, then promoting synthesis and release of AVP in SON, PVN. Under the specific condition of cerebral ischemia and reperfusion, the activity and contents of central AVP increased abnormally is one of the important factors which causes ischemia brain damage.

Aquaporin-4 in the formation of cerebral edema following severe burns What role do arginine vasopressin levels play?

BACKGROUND： Aquaporin-4 （AQP-4）, which is able to rapidly transport water within the brain, is highly expressed in brain tissue. It also plays an important role in the formation of cerebral edema following brain injury. However, the role of AQP-4 in the formation of cerebral edema following severe bums remains unknown. OBJECTIVE： To study changes in AQP-4 protein and mRNA expression during formation of cerebral edema following severe burns, and to explore the correlation between AQP-4 protein and mRNA expression with plasma levels of arginine vasopressin （AVP）. DESIGN, TIME AND SETTING： A randomized, controlled, animal experiment was performed at the Research Center of Neuroscience, Chongqing Medical University from 2007 to 2008. MATERIALS： Biotin-labeled goat anti-rabbit antibody was provided by Beijing Zhongshan Biotechnology, China; in situ hybridization kit was provided by Wuhan Boster Biotechnology, China; rabbit anti-AQP-4 polyclonal antibody and horseradish peroxidase-labeled goat anti-rabbit IgG were provided by Chemicon, USA; AVP radioimmunoassay kit was provided by the Research Department of Neurobiology, the Second Military Medical University of Shanghai, China. METHODS： A total of 180 adult, healthy, Wistar rats were randomly assigned to control and burn groups with 30 rats in each group. The burn group was observed at five different time points： 2, 6, 12, 24, and 48 hours after burn. Hair on the mouse back was removed to expose skin on the back. After 1 day, skin with the hair removed was dipped into 100℃ water for 15 seconds to induce grade III bum injury that measures 30% of total bum surface area. MAIN OUTCOME MEASURES： Brain water content was measured using the dry-wet weight method. AQP-4 protein and mRNA expressions were detected using immunohistochemistry, in situ hybridization, Western blot, and reverse transcription-polymerase chain reaction; dynamic changes in plasma AVP were detected using radioimmunoassay. RESULTS： Brain water content gradually increased following severe burn injury. AQP-4 protein and mRNA expressions were upregulated in the supraoptic nucleus, suprachiasmatic nucleus, paraventricular nucleus, hippocampus, choroid plexus, and cerebral cortex. Plasma AVP levels increased following burn injury. AQP-4 protein and mRNA expressions positively correlated with brain water content and AVP levels during formation of cerebral edema （r= 0.870, 0.848, P 〈 0.01）. CONCLUSION： AQP-4 participated in the formation of cerebral edema following burn injury. Plasma AVP upregulated AQP-4 expression in brain tissue, thereby promoting formation of cerebral edema.

Congenital nephrogenic diabetes insipidus arginine vasopressin receptor 2 gene mutation at new site:A case report

BACKGROUND Congenital nephrogenic diabetes insipidus(CNDI)is a rare hereditary disorder.It is associated with mutations in the arginine vasopressin receptor 2(AVPR2)gene and aquaporin 2(AQP2)gene,and approximately 270 different mutation sites have been reported for AVPR2.Therefore,new mutations and new manifestations are crucial to complement the clinical deficiencies in the diagnosis of this disease.We report a case of a novel AVPR2 gene mutation locus and a new clinical manifestation.CASE SUMMARY We describe the case of a 48-d-old boy who presented with recurrent fever and diarrhea 5 d after birth.Laboratory tests showed electrolyte disturbances and low urine specific gravity,and imaging tests showed no abnormalities.Genetic testing revealed a novel X-linked recessive missense mutation,c.283(exon 2)C>T(p.P95S).This mutation results in the substitution of a proline residue with a serine residue in the AVPR2 protein sequence.The diagnosis of CNDI was confirmed based on the AVPR2 gene mutation.The treatment strategy for this patient was divided into two stages,including physical cooling supplemented with appropriate amounts of water in the early stage and oral hydrochlorothiazide(1-2 mg/kg)after a clear diagnosis.After follow-up of one and a half years,the patient gradually improved.CONCLUSION AVPR2 gene mutations in new loci and new clinical symptoms help clinicians understand this disease and shorten the diagnosis cycle.

Growth hormone promotes the reconstruction of injured axons in the hypothalamo-neurohypophyseal system

Previous studies have shown that growth hormone can regulate hypothalamic energy metabolism, stress, and hormone release. Therefore, growth hormone has great potential for treating hypothalamic injury. In this study, we established a specific hypothalamic axon injury model by inducing hypothalamic pituitary stalk electric lesions in male mice. We then treated mice by intraperitoneal administration of growth hormone. Our results showed that growth hormone increased the expression of insulin-like growth factor 1 and its receptors, and promoted the survival of hypothalamic neurons, axonal regeneration, and vascular reconstruction from the median eminence through the posterior pituitary. Altogether, this alleviated hypothalamic injury-caused central diabetes insipidus and anxiety. These results suggest that growth hormone can promote axonal reconstruction after hypothalamic injury by regulating the growth hormone-insulin-like growth factor 1 axis.

当归芍药散对肾病综合征大鼠水肿的改善作用及机制

目的探究当归芍药散对肾病综合征大鼠水肿的改善作用及作用机制。方法将大鼠随机分为正常组、模型组、当归芍药散组(17.2 g·kg^(-1)·d^(-1))、氯沙坦组(30 mg·kg^(-1)·d^(-1))、托伐普坦组(3 mg·kg^(-1)·d^(-1))。尾静脉注射阿霉素建立肾病综合征大鼠模型。给药4周后,检测各组大鼠肾功能指标及24 h尿蛋白含量变化;免疫组化法检测肾组织中水通道蛋白2(aquaporin 2,AQP2)和pS256-AQP2的分布;放射免疫法测定血浆精氨酸加压素(arginine vasopressin,AVP)和血管紧张素Ⅱ(angiotensinⅡ,AngⅡ)水平;Western blot和RT-PCR法分别检测肾脏AQP2、pS256-AQP2、血管紧张素1型受体(angiotensin type 1 receptor,AT1R)、精氨酸加压素受体2(arginine vasopressin receptor 2,V2R)蛋白及mRNA的表达。结果3种药物均可改善肾病综合征大鼠肾功能,减轻蛋白尿,降低血浆AVP及AngⅡ水平,下调AQP2、pS256-AQP2蛋白和mRNA表达。当归芍药散与托伐普坦对于降低血浆AVP水平的效果优于氯沙坦。结论当归芍药散可能通过降低AVP及AngⅡ水平,进而调节AQP2的表达,改善肾病综合征大鼠水肿。

Expression of hippocampal corticosteroid receptors,as well as corticotrophin-releasing hormone and vasopressin in the hypothalamic paraventricular nucleus,in fornix transected rats

BACKGROUND： The hippocampus regulates the hypothalamic-pituitary-adrenal axis through negative feedback. The hypothalamic paraventricular nucleus receives neuronal input from the hippocampus via the fomix, OBJECTIVE： To explore whether the negative feedback effect of the hippocampus on the hypothalamic-pituitary-adrenal axis is contributed to the inhibitory effect of mineralocorticoid receptor （MR） and glucocorticoid receptor （GR） in the hippocampus on the paraventricular nucleus via the fornix. DESIGN, TIME AND SETTING： Randomized, controlled, animal experiment. The study was performed at the Department of Histology and Embryology, China Medical University between September 2006 and September 2008. MATERIALS： Rabbit anti-rat anti-MR and rabbit anti-rat anti-GR antibodies were purchased from Santa Cruz Biotechnology, USA. Rabbit anti-rat anti-corticotrophin releasing hormone （CRH） and rabbit anti-rat anti-arginine vasopressin antibodies were purchased from Wuhan Boster. METHODS： A total of 90 male, Wistar rats were randomly divided into model and sham-surgery groups （n = 45）. Fornix transection was performed in the model group, while the sham-surgery group underwent surgery, but no fornix transection. MAIN OUTCOME MEASURES： Immunohistochemistry was used to examine MR and GR expression in the hippocampus, as well as CRH and anti-arginine vasopressin in the paraventricular nucleus. Western blot was used to measure alterations in MR, GR, and CRH protein expression following fomix transection. RESULTS： Compared with the sham-surgery group, there were no obvious changes in MR and GR expression in the hippocampus, or CRH and anti-arginine vasopressin expression in the paraventdcular nucleus within 4 days of fornix transection. However, after 7-10 days, significantly decreased MR and GR expression in the hippocampus, and increased CRH and anti-arginine vasopmssin expression in the paraventricular nucleus were observed （P 〈 0.05-0.01）. CONCLUSION： Negative feedback from the hippocampus on the hypothalamic-pituitary-adrenal axis might be mediated through the fornix, and the corticosterene actions mediated by hippocampal corticosteroid receptors indirectly modulated the hypothalamic-pituitary-adrenal axis.

精氨酸加压素兴奋视前区正中核谷氨酸能神经元及其机制

目的研究精氨酸加压素(AVP)对小鼠视前区正中核谷氨酸能(MnPO^(Vglut2))神经元放电活动的影响及其机制。方法采用Vglut2-tdTomato雄性小鼠制作脑片,通过荧光显微镜找到表达红色荧光蛋白的MnPO^(Vglut2)神经元,应用全细胞膜片钳技术观察AVP对MnPO^(Vglut2)神经元放电频率的影响;或观察突触传递阻断剂(STBs)对AVP引起的MnPO^(Vglut2)神经元放电频率改变的影响;或观察AVP的V1a受体拮抗剂对AVP引起的MnPO^(Vglut2)神经元放电频率改变的影响。结果与灌流人工脑脊液(ACSF)时比较,灌流ACSF+AVP时,MnPO^(Vglut2)神经元的平均放电频率明显升高(P<0.01),表明AVP可兴奋MnPO^(Vglut2)神经元。与灌流ACSF+STBs时比较,灌流ACSF+STBs+AVP时,MnPO^(Vglut2)神经元的平均放电频率仍明显升高(P<0.001);此外,与灌流ACSF+AVP时比较,灌流ACSF+STBs+AVP时,AVP引起的MnPO^(Vglut2)神经元的放电频率增加幅度无明显改变(P>0.05),提示AVP通过突触后的机制直接兴奋MnPO^(Vglut2)神经元。与灌流ACSF+STBs+AVP时比较,灌流ACSF+STBs+AVP+V1a受体拮抗剂时,AVP引起的MnPO^(Vglut2)神经元的放电频率增加幅度明显下降(P<0.01),提示AVP通过V1a受体直接兴奋MnPO^(Vglut2)神经元。结论AVP可通过突触后的机制经V1a受体直接兴奋MnPO^(Vglut2)神经元。该研究揭示了AVP作用的MnPO神经元的分子标记。

Vasopressin in vasoplegic shock:A systematic review

BACKGROUNDVasoplegic shock is a challenging complication of cardiac surgery and is oftenresistant to conventional therapies for shock. Norepinephrine and epinephrine arestandards of care for vasoplegic shock, but vasopressin has increasingly been usedas a primary pressor in vasoplegic shock because of its unique pharmacology andlack of inotropic activity. It remains unclear whether vasopressin has distinctbenefits over standard of care for patients with vasoplegic shock.AIMTo summarize the available literature evaluating vasopressin vs non-vasopressinalternatives on the clinical and patient-centered outcomes of vasoplegic shock inadult intensive care unit (ICU) patients.METHODSThis was a systematic review of vasopressin in adults (≥ 18 years) with vasoplegicshock after cardiac surgery. Randomized controlled trials, prospective cohorts,and retrospective cohorts comparing vasopressin to norepinephrine, epinephrine,methylene blue, hydroxocobalamin, or other pressors were included. The primaryoutcomes of interest were 30-d mortality, atrial/ventricular arrhythmias, stroke,ICU length of stay, duration of vasopressor therapy, incidence of acute kidneyinjury stage II-III, and mechanical ventilation for greater than 48 h.RESULTSA total of 1161 studies were screened for inclusion with 3 meeting inclusioncriteria with a total of 708 patients. Two studies were randomized controlled trials and one was a retrospective cohort study. Primary outcomes of 30-d mortality,stroke, ventricular arrhythmias, and duration of mechanical ventilation weresimilar between groups. Conflicting results were observed for acute kidney injurystage II-III, atrial arrhythmias, duration of vasopressors, and ICU length of staywith higher certainty of evidence in favor of vasopressin serving a protective rolefor these outcomes.CONCLUSIONVasopressin was not found to be superior to alternative pressor therapy for any ofthe included outcomes. Results are limited by mixed methodologies, small overallsample size, and heterogenous populations.

肝硬化腹水低钠血症与精氨酸加压素关系和V2受体拮抗剂应用的争议问题

肝硬化腹水患者限钠、利尿治疗中忽视补充丢失NaCl常导致低钠血症及精氨酸加压素(arginine vasopressin,AVP)合成与分泌增加和水潴留,有人强调给予AVP-V2受体拮抗剂(托伐普坦)治疗,但存在较多争议:(1)AVP升高及水潴留是否与低钠血症有关;(2)补充因应用利尿剂丢失NaCl是否能抑制AVP合成与释放;(3)高渗NaCl纠正低钠血症效果是否优于托伐普坦;(4)应用托伐普坦时如何规避等渗性血容量不足潜在风险因素;(5)从源头防止低钠血症是否能抑制AVP分泌等,本文就上述问题提出商榷。

Copeptin作为代谢性疾病生物标志物的研究进展

精氨酸加压素是一种由下丘脑合成以应对血浆渗透压增加和血容量减少的激素,它可以与精氨酸加压素受体结合影响糖脂代谢。最近有研究表明,Copeptin是一个稳定、敏感且暂未发现有生物活性的精氨酸加压素替代标志物,与精氨酸加压素以等摩尔量释放入血,其循环水平升高与糖尿病、糖尿病并发症、肥胖、胰岛素抵抗、高血压、高脂血症、非酒精性脂肪性肝病等代谢性疾病密切相关。积极探索Copeptin与代谢性疾病中的关系有助于疾病的早期诊断。

精氨酸加压素在睡眠-觉醒及焦虑、抑郁情绪调控中的作用

精氨酸加压素(argininevasopressin,AVP),又称抗利尿激素,是由下丘脑视上核或室旁核分泌的高度保守的神经肽,具有复杂的生理功能。本文对AVP的生理学特性进行了简单概述,阐述AVP可能通过下丘脑泌素能系统和去甲肾上腺素能系统参与睡眠-觉醒调控,并通过促进视交叉上核神经元细胞间耦合来维持昼夜节律稳态;并描述了AVP在焦虑和抑郁情绪调控的可能作用。

丁香酚对酵母菌发热大鼠血浆及脑脊液中精氨酸加压素含量的影响

目的探讨丁香酚抑制酵母菌所致发热的机制。方法建立大鼠酵母菌性发热模型,观察丁香酚对大鼠直肠温度的影响,放免法测定大鼠血浆及脑脊液中精氨酸加压素(AVP)含量的改变。结果皮下注射酵母混悬液后大鼠直肠温度明显升高(△T由-0.23℃升高至1.13℃,P<0.01),血浆及脑脊液中AVP含量也明显增加(分别由1.55,2.57ng/ml升高至2.03,4.29ng/ml,P<0.05),丁香酚能明显抑制酵母菌所致大鼠发热反应(△T由1.19℃降低至0.03℃,P<0.01),同时血浆及脑脊液中AVP含量也进一步增加(分别由2.03,4.29ng/ml升高至3.51,6.69ng/ml,P<0.05)。结论丁香酚通过增加体内AVP的含量而发挥其解热作用。

缺锌大鼠海马生长抑素和精氨酸加压素的变化

方法：采用液体缺锌饲料灌胃的方式使大鼠缺锌二周。采用Ｙ－迷宫实验和原子吸收及放射免疫分析技术，分别测定大鼠的学习记忆行为，血清锌含量和海马生长抑素（ＳＳ）、精氨酸加压素（ＡＶＰ）水平的变化。结果：与正常对照组相比，缺锌大鼠在Ｙ－迷宫中达到学会标准所用的时间明显增多（Ｐ＜０．０５）；血清锌含量明显降低（Ｐ＜０．０５）；海马ＳＳ和ＡＶＰ水平明显降低（Ｐ＜０．０１）。结论：在缺锌状态下，海马内的ＳＳ和ＡＶＰ水平是降低的，这种变化可能是缺锌影响脑的智力发育的重要因素之一。

艾灸头部穴位为主对血管性痴呆患者脑脊液中生长抑素和精氨酸血管加压素水平影响的随机对照试验

背景:血管性痴呆(vascular dementia,VaD)患者血浆和脑脊液中多种神经肽类物质发生明显变化;有效地干预神经肽水平,对VaD的预防和治疗十分重要。目的:以艾灸头部穴位为主治疗VaD,观察其改善临床症状和调控脑脊液中与学习记忆相关的神经肽物质生长抑素(somatostatin,SS)和精氨酸血管加压素(arginine vasopressin,AVP)水平的作用。设计、场所、对象和干预措施:65例VaD患者均为安徽中医学院针灸医院门诊或住院病例。按随机数字表法分为艾灸组(33例)和西药组(32例)。艾灸组患者给予隔附子饼压灸,反复灸20min;西药组口服吡拉西坦素片0.8g,3次/d。两组均治疗4个疗程,4周为1个疗程。主要结局指标:比较两组治疗前后长谷川痴呆智能检查量表(Hasegawas Dementia Scale,HDS)、简易智能精神状态检查量表(Mini-Mental State Examination,MMSE)和日常生活能力量表(Activity of Daily Living Scale,ADL)积分变化,以及脑脊液中SS和AVP水平。结果:艾灸组总有效率与西药组比较,差异有统计学意义(P<0.01)。两组治疗前后HDS、MMSE和ADL积分比较,差异均有统计学意义(P<0.05,P<0.01),艾灸组HDS、MMSE和ADL量表积分治疗前后差值较西药组有所改善(P<0.05,P<0.01)。两组治疗后脑脊液SS和AVP水平较治疗前明显升高(P<0.01),艾灸组治疗后SS和AVP升高水平较西药组明显(P<0.01)。结论:艾灸能改善临床相关症状积分,调控与学习记忆相关的神经肽物质,是治疗VaD的有效方法。

核因子κB在精氨酸血管升压素诱导大鼠心肌成纤维细胞一氧化氮合成中的作用

本文探讨了精氨酸血管升压素(AVP)刺激下体外培养的大鼠心肌成纤维细胞(CFs)内一氧化氮(NO)含量、一氧化氮合酶(NOS)活性、诱导型一氧化氮合酶基因表达的变化及其与核因子κB(NF-κB)的关系。用胰酶消化法分离培养Sprague Dawley仔鼠的CFs,分别采用硝酸还原酶法、分光光度法、逆转录一聚合酶链式反应(RTPCR)、免疫荧光-共聚焦显微镜和蛋白质印迹检测AVP干预下CFs的NO含量、NOS活性、iNOS mRNA表达和NFKB的活化。结果显示,AVP浓度依赖性(0.001—0.1μmol/L)地增加CFs的NO含量,提高NOS活性,增加iNOSmRNA表达;AVP能够活化NF-κB,使其由细胞浆转位于细胞核;NF-κB特异性抑制剂吡咯啉烷二甲基硫脲(PDTC)能够抑制AVP诱导的CFs NO含量增加、NOS活性提高和iNOS mRNA表达增加。上述结果提示,AVP干预下CFsiNOS mRNA表达增加、NOS活性增高、NO合成增多可能通过NF-κB激活途径,NF-κB激活参与心肌纤维化的发生和发展。

补肾活血中药治疗血管性痴呆的实验研究

在MID动物模型上,以西药脑复康为对照,采用水迷宫和放免法观察了醒脑胶囊主要成份补肾活血药物对痴呆大鼠学习记忆能力及脑组织(海马、皮质)中神经肽AVP、SS含量的影响。结果:中药组和脑复康组大鼠游迷宫所需时间和错误次数均明显少于模型组(P<0.05或P<0.01),其中中药组大鼠游全程时间显著少于脑复康组(P<0.05或P<0.01),错误次数与脑复康组无显著性差异(P>0.05)。同时中药组与脑复康组大鼠血浆、脑组织(海马、皮质)中AVP、SS含量均显著高于模型组(P<0.01),且中药组AVP、SS含量又明显高于脑复康组(P<0.05或P<0.01)。提示补肾活血中药能明显改善VD大鼠学习记忆能力,疗效与脑复康相近。同时补肾活血中药能显著提高VD大鼠血浆、脑组织(海马、皮质)中神经肽AVP、SS含量,且优于脑复康。推测血浆及脑组织中神经肽AVP、SS含量的提高可能是中医补肾活血法治疗VD的神经生化基础之一。

芪苈强心胶囊对慢性心力衰竭大鼠心脏功能及血浆血管加压素的影响

目的探讨芪苈强心胶囊对慢性心力衰竭(CHF)大鼠心脏功能及血浆血管加压素(AVP)的影响。方法 SD大鼠结扎冠脉前降支,建立CHF大鼠模型,将大鼠随机分为慢性心力衰竭组(C组),芪苈强心高、中、低剂量治疗组(Q1、Q2、Q3组)和呋塞米治疗组(F组),另设假手术组(S组)。药物灌胃6周后检测大鼠超声心动图和血流动力学指标,放射免疫法测定血浆AVP浓度。结果与S组比较,C组大鼠心脏功能显著减退,血浆AVP浓度显著升高(P<0.01)。经过芪苈强心胶囊治疗后,Q1、Q2、Q3组大鼠心脏功能、血流动力学指标均有显著改善,血浆AVP浓度显著降低(P<0.05);F组大鼠心脏功能及血流动力学指标均无显著改善,而血浆AVP浓度显著升高(P<0.05)。结论芪苈强心胶囊可以改善CHF大鼠的心脏功能,降低血浆AVP浓度。

刺激室旁核及加压素对大鼠胃缺血-再灌注损伤的保护作用

采用夹闭大鼠腹腔动脉 30min ,松开动脉夹血流复灌 1h的胃缺血 再灌注损伤 (gastricischemia reperfu sioninjury ,GI RI)模型 ,观察了电或化学刺激室旁核 (paraventricularnucleus,PVN)及外源性加压素 (arginine vasopres sion ,AVP)对GI RI的影响 ,并对PVN的调控通路进行了初步分析。结果表明 :电或化学刺激PVN后 ,GI RI显著减轻 ;损毁双侧孤束核 (nucleustractussolitarius,NTS)或一侧NTS内注射AVP V1受体阻断剂 ,均能取消电刺激PVN对GI RI的效应 ;去除脑垂体后不影响PVN的作用 ;切断膈下迷走神经或切除腹腔交感神经节 ,则能加强电刺激PVN对GI RI的影响 ;PVN内注射不同剂量的AVP同样能减轻大鼠GI RI损伤。结果提示 :PVN及AVP对大鼠GI RI具有保护作用 ;PVN的这种作用可能是因电或化学刺激后 ,激活了其中的加压素能神经元 ,经其下行投射纤维释放AVP作用于NTS神经元的AVP V1受体 ,并通过迷走和交感神经介导 ,从而影响GI RI;而似与PVN

血管性痴呆患者血浆、脑脊液Ang、AVP、NSE含量的变化及其临床意义

目的 了解血管性痴呆 (VD)患者血浆、脑脊液 (CSF)中血管紧张素 (Ang )、精氨酸加压素 (AVP)、神经元特异性烯醇化酶 (NSE)的质量浓度变化及临床意义。方法 运用简易精神状态量表 (MMSE)、P3 0 0潜伏期 (P3 0 0 PL)、Hachinski缺血量表 (HIS)和社会功能活动调查 (FAQ)评定患者认知功能 ,用放射免疫分析法(RIA)测定血浆、CSF中 Ang 、AVP质量浓度 ,用双抗体免疫夹心法 (ELASA)测定血浆、CSF中 NSE质量浓度。结果 VD组血浆、CSF中 Ang 质量浓度显著高于对照组 (P <0 .0 1 ) ,CSF中 Ang 质量浓度亦显著高于脑梗死 (CI)恢复期 (P <0 .0 1 ) ,血浆 AVP质量浓度无显著变化 (P >0 .0 5 ) ,CSF中 AVP质量浓度显著降低 (P <0 .0 1 ) ,血浆、CSF中 NSE质量浓度同对照组比较明显下降 (P <0 .0 5 ) ;直线相关分析 :VD组血浆与CSF中 Ang 、AVP质量浓度变化无显著相关 (P >0 .0 5 ) ,血浆与 CSF中 NSE质量浓度变化呈直线正相关(P <0 .0 1 )。结论 脑内 AVP、Ang 在 VD发病中可能起重要作用 ,CSF中 AVP、Ang 质量浓度变化与认知功能密切相关 ;脑内 NSE质量浓度变化与缺血性脑损害的严重程度密切相关 ,但不能作为反映认知功能的生化指标。