Pu S, Horvath T L, Diano S, Naftolin F, Kalra P S, Kalra S P
Department of Neuroscience, University of Florida College of Medicine, Gainesville 32610, USA.
Endocrinology. 1997 Apr;138(4):1537-43. doi: 10.1210/endo.138.4.5086.
Nitric oxide (NO) is now recognized as a diffusible messenger molecule that normally augments intercellular communication in the central nervous system, but is neurotoxic if released in excessive amounts. NO is synthesized from L-arginine by the Ca2+/calmodulin-dependent neuronal isoform NO synthase (NOS) localized in sub-populations of neurons throughout the brain, including the hypothalamus. In the hypothalamus, NO stimulates the release of GnRH, the primary neurohormone governing reproduction in mammals. Although the excitatory amino acid, glutamate, acting through the N-methyl-D-aspartate (NMDA) receptor is believed to be responsible for stimulation of NO release, the neuronal system(s) that inhibits NO efflux is unknown. As the endogenous opioids, primarily beta-endorphin (betaEND), exert a tonic restraint on GnRH secretion, we sought evidence for a possible functional link between betaEND and NOS pathways in the hypothalamus. We observed that restraining the opioid influence with the opiate receptor antagonist, naloxone, in intact, but not in castrated, rats rapidly augmented extracellular cGMP/NO efflux in the medial preoptic area, where GnRH, NOS, and betaEND immunoreactive pathways are coextensive. Pituitary LH secretion increased in conjunction with this augmented cGMP/NO response and pretreatment with the mu opiate receptor agonist, morphine, suppressed these naloxone-induced responses. Further, visualization of hypothalamic sections immunostained for both betaEND and NOS revealed betaEND-immunoreactive axon terminals in close proximity to NOS-positive cell bodies and dendrites in a number of hypothalamic subdivisions, including the medial preoptic area. These close appositions represented conventional synapses between betaEND nerve terminals and NOS-positive perikarya and dendrites under the electron microscope. Clearly, the experimental data, corroborated by morphological evidence, point to a direct inhibitory control of betaEND on NOS-immunoreactive neurons in monitoring cGMP/NO release. These findings together with the previous observations that the glutamate neurotransmitter acting through NMDA receptors located on NOS-immunopositive cells stimulates cGMP/NO efflux and plasma LH selectively in intact rats document the existence of a dual control comprised of the excitatory NMDA and the inhibitory mu opiate receptors in modulating cGMP/NO release, a response also directed by gonadal steroids. This new knowledge of an inhibitory opioid influence on cGMP/NO release is probably extremely important both in the generation of periodicities in GnRH secretion that underlie hypothalamic control of reproduction and in protecting against neurotoxic overstimulation of NO release by excitatory amino acids.
一氧化氮(NO)现在被认为是一种可扩散的信使分子,它通常增强中枢神经系统中的细胞间通讯,但如果过量释放则具有神经毒性。NO由L-精氨酸通过位于包括下丘脑在内的整个大脑中神经元亚群中的Ca2+/钙调蛋白依赖性神经元型一氧化氮合酶(NOS)合成。在下丘脑中,NO刺激促性腺激素释放激素(GnRH)的释放,GnRH是控制哺乳动物生殖的主要神经激素。尽管通过N-甲基-D-天冬氨酸(NMDA)受体起作用的兴奋性氨基酸谷氨酸被认为负责刺激NO释放,但抑制NO外流的神经元系统尚不清楚。由于内源性阿片类物质,主要是β-内啡肽(βEND),对GnRH分泌施加张力性抑制,我们寻找βEND与下丘脑NOS途径之间可能存在功能联系的证据。我们观察到,在完整但未阉割的大鼠中,用阿片受体拮抗剂纳洛酮抑制阿片类物质的影响,可迅速增加视前内侧区细胞外cGMP/NO外流,GnRH、NOS和βEND免疫反应途径在此区域共存。垂体促黄体生成素(LH)分泌随着这种增强 的cGMP/NO反应而增加,用μ阿片受体激动剂吗啡预处理可抑制这些纳洛酮诱导的反应。此外,对下丘脑切片进行βEND和NOS免疫染色的观察显示,在包括视前内侧区在内的一些下丘脑亚区中,βEND免疫反应性轴突终末紧邻NOS阳性细胞体和树突。在电子显微镜下,这些紧密的毗邻关系代表了βEND神经终末与NOS阳性核周体和树突之间的传统突触。显然,实验数据得到形态学证据的证实,表明βEND对监测cGMP/NO释放的NOS免疫反应性神经元具有直接抑制控制作用。这些发现与先前的观察结果一起,即在完整大鼠中,通过位于NOS免疫阳性细胞上的NMDA受体起作用的谷氨酸神经递质选择性刺激cGMP/NO外流和血浆LH,证明了在调节cGMP/NO释放方面存在由兴奋性NMDA和抑制性μ阿片受体组成的双重控制,这种反应也受性腺类固醇的指导。这种关于抑制性阿片类物质对cGMP/NO释放影响的新知识,可能在GnRH分泌周期性的产生中极为重要,GnRH分泌周期性是下丘脑对生殖控制的基础,并且在防止兴奋性氨基酸对NO释放的神经毒性过度刺激方面也极为重要。
