下丘脑减压区微量注射牛磺酸对血压的影响

实验采用微量注射和荧光分光光度测定的方法,探讨了下丘脑前部减压区牛磺酸对大鼠血压的影响及其可能的机制。结果显示：（１）下丘脑前部减压区微量注射牛磺酸可致大鼠血压降低;（２）侧脑室注射β受体阻断剂心得安可阻断牛磺酸的降压效应。而α受体阻断剂酚妥拉明对牛磺酸的降压效应无明显影响;（３）下丘脑前部减压区注射牛磺酸后,可使下丘脑去甲肾上腺素含量明显增高。     

伏核在躯体传入冲动抑制防御性心血管反应中的作用及机制

损毁伏核可明显削弱电刺激腓深神经（ＤＰＮ）对兴奋下丘脑背内侧核诱发的升压反应和心肌缺血的抑制作用（Ｐ＜０．０５,Ｐ＜０．０１）。电刺激伏核可引起明显的降压效应。中脑中央灰质腹侧部（ｖＰＡＧ）微量注射纳洛酮可明显衰减伏核的减压效应;损毁ｖＰＡＧ甚至可翻转伏核的减压效应,引起轻度升压（Ｐ＜０．０１）。损毁弓状核后伏核的减压效应基本消失,弓状核内微量注射纳洛酮明显衰减伏的的减压效应。故ＤＰＮ传入冲动可能     

下丘脑穹窿周围区不同部位兴奋对心肌Po_2及ECG－ST的影响

电刺激下丘脑穹窿周围区（ＰＦＡ）的下丘脑背内侧核（ＤＭＨ）,下丘脑腹内侧核（ＶＭＨ）与下丘脑外侧区（ＬＨＡ）均可引起心肌Ｐ０＿２下降与血压升高,而以ＤＭＨ所致的心肌Ｐ０,下降最明显（Ｐ＜０．０１）。心得安可取消电刺激ＬＨＡ所致的心肌ＰＯ＿２下降,部分取消电刺激ＶＭＨ引起的心肌ＰＯ＿２下降,而不改变电刺激ＤＭＨ所致的心肌ＰＯ＿２下降（Ｐ＞０．０５）。ＤＭＨ、ＶＭＨ微量注射谷氨酸钠（０．１ｍｏｌ／Ｌ０．５μｌ）均可诱发升压反应和ＥＣＧ－ＳＴ压低,而ＬＨＡ微量注射谷氨酸却导致降压反应,对ＥＣＧ－ＳＴ无明显影响。上述结果提示ＤＭＨ为ＰＦＡ各区诱发心肌缺血缺氧的主要核团。兴奋ＤＭＨ、ＶＭＨ所致的心血管效应主要由胞体兴奋诱发,而电刺激ＬＨＡ所致的升压反应主要为兴奋过路纤维引起,该区胞体兴奋主要导致降压反应。     

下丘脑穹窿周围区不同部位兴奋对心肌Po2及ECG—ST的影响

电刺激下丘脑穹窿周围区（ＰＦＡ）的下丘脑背内侧核（ＤＭＨ）,下丘脑腹内侧核（ＶＭＨ）与下丘脑外侧区（ＬＨＡ）均可引起心肌Ｐｏ２下降与血压升高,而以ＤＭＨ所致的心肌Ｐｏ２下降最明显。心得安可取消电刺激ＬＨＡ所致的心肌Ｐｏ２下降,部分取消电刺激ＶＭＨ引起的心肌Ｐｏ２下降,而不改变电刺激ＤＭＨ所致的心肌Ｐｏ２下降。ＤＭＨ、ＶＭＨ微量注射谷氨酸钠均可诱发升压反应和ＥＣＧ－ＳＴ压低,而ＬＨＡ微量注射谷氨酸却     

刺激家兔腹部迷走神经外周端降压效应中枢机制的研究

应用电解损毁和脑室内注射药物的方法研究了刺激家兔腹部迷走神经外周端所致降压效应的中枢机制。结果表明:1.电刺激延脑闩部尾侧1.5—2mm、中线旁开0.25mm、深1—2mm 处主要引起降压反应。2.电解损毁该部位可以使刺激腹部迷走神经外周端所引起的降压效应显著减弱(n=20,P<0.001),但对刺激减压神经所致降压反应无影响。3.在延脑闩部水平电解损毁减压神经纤维在孤束核的主要投射区可以使刺激减压神经所致降压反应显著减弱,而对刺激腹部迷走神经外周端所致降压反应无影响。4.第四脑室注射5,6-双羟色胺的动物较之注射人工脑脊液的动物颈、胸髓5-羟色胺含量明显降低、动物动脉压增高、心率明显增快、刺激减压神经所致降压反应未见减弱,而刺激腹部迷走神经外周端所致降压反应却明显减小。因此,我们认为家兔腹部迷走神经外周端所致降压效应依赖于延脑闩下部的中缝隐核及连合核等结构,而与减压神经的投射部位无关。延脑中缝核至脊髓的下行性5-HT能神经纤维抑制脊髓交感节前神经元的活动,是这个降压效应的中枢机制之一。     

大鼠蓝斑核区神经降压素对迷走—加压反应的影响

本文应用放射免疫、核团微量注射及组织荧光分光测定等实验方法,研究大鼠蓝斑核区神经降压素对迷走-加压反应的影响。结果表明:1.电刺激颈迷走神经向中端,孤束核、蓝斑核区和下丘脑中神经降压素免疫活性物的含量明显增高(p<0.05)。2.蓝斑核区注入神经降压素后,刺激颈迷走神经向中端,迷走-加压反应明显减弱(P<0.01),并呈明显的量效依赖关系。3.蓝斑核区注入抗神经降压素血清,迷走-加压反应明显加强(p<0.01)。4.蓝斑核区注入神经降压素后,刺激颈迷走神经向中端,该区去甲肾上腺素含量明显增高(p<0.05)。以上结果提示:内源与外源性神经降压素参与迷走-加压反应的调节过程,并可能与神经降压素引起蓝斑核区去甲肾上腺素含量增加有关。     

刺激蓝斑对心肌收缩力及肾交感神经放电的影响

在64只麻醉及人工呼吸的猫,观察到电刺激蓝斑(LC)能引起血压升高、心率加快,左心室收缩压升高,左心室内压最大变化率增加及肾交感神经放电(RNA)显著地增加。去缓冲神经对电刺激 LC 所引起的上述指标的增加幅度无明显影响,但可明显延长血压反应升高相以及血压恢复期的时间。LC 内微量注射谷氨酸钠可使血压下降,心率减慢,左室收缩压和左室内压最大变化率亦降低。LC 内注射海人酸,也能引起减压反应。而注射海人酸3h 后,使LC 神经元发生变性或去极化阻断时,再电刺激 LC 仍能引起明显的升压反应。以上结果表明,电刺激 LC 可使血压升高、心肌收缩力及肾交感神经放电增加,而 LC 内微量注射胞体兴奋剂则可降低血压、心率及心肌收缩力,说明电刺激 LC 引起的加压反应可能主要是兴奋了过路纤维所致,而 LC 本身神经元的兴奋引起的是减压反应。     

大鼠缰核与下丘脑外侧区在调节心血管活动方面的机能联系

电刺激大鼠下丘脑外侧区（LH）,动脉压明显升高,心率加快,在刺激电极同侧缰核（Hb)内微量注射盐酸利多卡因、电刺激LH引起的升压反应可被阻断38.9%,心率增快反应可被阻断44.4%,双侧Hb内微量注射盐酸利多卡因,电刺激LH引起的升压反应可被阻断40.7%,心率增快反应可被阻断41.2% ,单侧或双侧Hb内微量注射人工脑脊液均不能阻断电刺激LH引起的心血管反应。电刺激大鼠Hb,动脉压明显升高,心率无明显改变,在刺激电极同侧LH内微量注射盐酸利多卡因,电刺激Hb引起的升压反应可被阻断63.2%,双侧LH内微量注射盐酸利多卡因,电刺激Hb引起的升压反应可被阻断62.6%,单侧或双侧LH内微量注射人工脑脊液均不能阻断电刺激Hb引起的心血管反应。本实验提示Hb与LH在调节心血管活动方面有协同作用。     

大鼠孤束核神经降压素在迷走—加压反应中的作用

采放放射免疫、核团微量注射及组织荧光分光测定等实验方法,研究了大量孤束核神经降压素对迷走－加压反应的影响,结果表明,１．不走神经向中端,孤束核神经降压素免疫活性物的含量明显增高;２．孤束核内注入抗神经降压素血清后,刺激颈迷走神经向中端,迷走－加压反应明显;３．孤束核内注入神经降压素后,刺激颈迷走神经向中端,迷走－加压反应明显减弱,４．孤束核注入神经降压素后,刺激颈迷走神经向中端,孤束核去甲腺素含量     

室旁核在刺激中脑防御反应区诱发防御性升压反应中的作用

雄性ＳＤ大鼠,用乌拉坦（７００ｍｇ／ｋｇ）和氯醛糖（３０ｍｇ／ｋｇ）腹腔麻醉。实验结果：（１）每隔５ｍｉｎ电刺激中脑导水管周围灰质背侧部“防御反应区”（ｄＰＡＧ）,持续观察５０ｍｉｎ,可见恒定的升压反应。若电解毁单侧室旁核（ＰＶＮ）区。１ｈ后,电刺激中脑ｄＰＡＧ区诱发的升压反应幅度部分减小。而损毁穹隆部、下丘脑前部、下丘脑背内侧核、下丘脑腹内侧核则无上述效应。（２）电刺激或微量注射高半胱胺酸（ＤＬ     

安定降低家兔血压和减少刺激下丘脑诱发室性期前收缩的机制分析

家兔62只,用乌拉坦(700mg/kg)和氯醛醣(35mg/kg)静脉麻醉,三碘季铵酚制动,在人工呼吸下进行实验。用电刺激下丘脑近中线区的方法诱发室性期前收缩(HVE)。静脉注射安定(0.5mg/kg)可降低基础血压(BP),减弱刺激下丘脑引起升压反应(指收缩压峰值SBP_(max))和减少HVE。在双侧延髓腹外侧头端区(rVLM)微量注射氟安定(200μg溶于0.5μl中),γ-氨基丁酸(GABA)(6μg溶于0.5μl中)均能降低BP、SBP_(max)和减少HVE,若微量注射印防己毒素(7.5μg溶于0.5μl中)则可使BP上升并增多HVE。而于双侧延髓腹外侧尾端区(cVLM)微量注射同样剂量氟安定、GABA则无上述反应。安定降低BP、SBP_(max)和减少HVE的作用可被双侧rVLM区微量注射GABA受体拮抗剂荷包牡丹碱(3μg溶于0.5μl中)或印防己毒素所消除,但在双侧rVLM区微量注射甘氨酸受体拮抗剂士的宁(1μg溶于0.5μl中)、阿片受体拮抗剂纳洛酮(0.5μg溶于0.5μl中)、胆碱能阻断药阿托品(0.25μg溶于0.5μl中)、东莨菪碱(1.5μg溶于0.5μl中)后仍然存在。 上述结果提示,在双侧rVLM应用GABA受体拮抗剂可消除安定降低BP、SBP_(max)和减少HVE的作用,安定降低BP、SBP_(max)和减少HVE的作用可能通过GABA这一中间环节,而胆碱能受体、阿片受体、甘氨酸受体可能不起重要作用。     

Localization of alpha 2-adrenergic agonist sensitive area in the hypothalamus for growth hormone release in the rat

To determine the localization of the clonidine sensitive area responsible for GH release, a minute amount of the alpha 2-agonist (67 ng/0.2 microliter) was injected into the hypothalamus and vicinity of adult male conscious rats. The animals were chronically implanted with double metal cannulae fixed on the skull for clonidine microinjection and with silastic tubing into the right atria for collecting blood samples. Ten hr prior to the microinjection, alpha-methyl-p-tyrosine (250 mg/kg body weight) was intraperitoneally injected to prevent spontaneous pulsatile GH release. Localization of the microinjection was assessed by histological examination after the experiment. Clonidine microinjection into the amygdala nucleus had no effect on GH release, while the injection into the preoptic and anterior hypothalamic area (PO/AH) significantly stimulated GH release by causing it to begin 30 min earlier. However, the paraventricular nucleus, the dorsomedial nucleus, the lateral hypothalamus and the ventromedial hypothalamus areas did not respond to the injection, although the latter nucleus has been shown to be a specific locus sensitive to electrical stimulation of release. In the area from the posterior hypothalamus to the mammillary body, several injections stimulated GH release (6/15), but the stimulatory effect was statistically insignificant when comparison was made with the mean (+/- SE) for all 15 rats. These findings suggest that the alpha 2-agonist acts on the PO/AH to induce an increase in GH release in alpha-methyl-p-tyrosine-pretreated rats, probably mediating the inhibitory input to somatostatinergic neurons which reside in the periventricular nucleus of the PO/AH area.     

Role of the hypothalamus in regulating liver circulation

In acute experiments on nembutal anesthetized dogs stimulation of anterior hypothalamus elicited changes in the hepatic artery blood flow, which followed those of arterial pressure; the vascular resistance remaining unchanged. The stimulation of medial and posterior hypothalamus led to decrease in flow and increase in the resistance of the hepatic artery. In most cases of hypothalamic stimulation the portal blood flow diminished, portal pressure and vascular resistance increased. The opposite reactions were observed during stimulation of sympathoinhibitory area, paraventricular and lateral hypothalamic nuclei. The conclusion is made that the hypothalamus participates in integrative and differential control of the hepatic circulation.     

Hyperuricemia in the rat following hypothalamic stimulation

Ventromedial hypothalamic electrical stimulation elicited a marked elevation of plasma uric acid with a rise in plasma allantoin in the rat. The magnitude of this hyperuricemia was greater than that of the hyperglycemia which was also produced by the ventromedial stimulation. On the other hand, lateral hypothalamic stimulation did not significantly affect the plasma levels of either of the purine metabolites. These results strongly indicate that the ventromedial hypothalamus is specifically very active in producing hyperuricemia in the rat.     

Responses of neurons of different hypothalamic structures to stimulation of tooth pulp and Aß afferents in the cat sciatic nerve

The response of neurons of different hypothalamic structures to stimulation of painful tooth pulp afferents and painless sciatic nerve Aß afferents was investigated during acute experiments on cats. It was found that 80.7%, 81.5%, and 71.4% of neurons of the posterior, tuberal, and anterior hypothalamus respectively, responded to stimulation of the tooth pulp. Shortest latency of response was recorded in the posterolateral hypothalamus. Latency of response was shorter in the lateral than in the medial structures throughout the hypothalamus. A distinct prevalence of excitatory response was found in neurons of the posterior area and an almost equal proportion of excitatory and inhibitory response in neurons of the tuberal and anterior hypothalamus. A high degree of convergence between noxious and nonnoxious somatic afferents were discovered in hypothalamic neurons: 85.8% of those studied responded to stimulation of the sciatic nerve Aß afferents. The comparable unidirectional response pattern of hypothalamic neurons to stimulation of tooth pump painful afferents and painless sciatic nerve Aß fibers point to the nonspecific nature of the response observed in the mainstream population of multisensory hypothalamic neurons. A small population of unimodal nociceptive neurons (14.2%) was found in the hypothalamus. Nociceptive responses of anterior hypothalamic neurons were distinguished by their long refractory phase, lasting 200–500 msec, and their low rate of reproduction during rhythmic stimulation of tooth pulp (1.5–2 Hz). Neuronal organization of the nociceptive hypothalamic afferent system is discussed together with the role of convergent and specific "nociceptive" neurons in the shaping of thalamic regulatory functions.L. A. Orbeli Institute of Physiology, Academy of Sciences of the Armenian SSR, Erevan. Translated from Neirofiziologiya, Vol. 18, No. 2, pp. 171–180, March–April, 1986.