Myr+-Gi2 alpha and Go alpha subunits restore the efficacy of opioids, clonidine and neurotensin giving rise to antinociception in G-protein knock-down mice.

Garzon J; Rodriguez Diaz-M; DeAntonio I; DeFelipe J; Rodriguez JR; Sanchez Blazquez-P

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Myr+-Gi2 alpha and Go alpha subunits restore the efficacy of opioids, clonidine and neurotensin giving rise to antinociception in G-protein knock-down mice.

机译：Myr + -Gi2 alpha和Go alpha亚基可恢复阿片类药物，可乐定和神经降压素的功效，从而在G蛋白敲除小鼠中产生抗伤害感受作用。

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In mice whose Gi/o-protein function had been impaired by antisense 'knock-down' or pertussis toxin treatment, i.c.v. injection of myr+-Gi/o alpha subunits restored the effectiveness of beta-endorphin, morphine, DPDPE, clonidine and neurotensin to produce antinociception. Myr+-G alpha subunits of the class of G-proteins actually impaired were more effective than unlike but related myr+-G alpha subunits. Selectivity was noted in that only exogenous myr+-G alpha subunits affected (enhanced) the activity of agonists in G alpha-deficient signalling systems. This treatment had little effect on agonist potency when the impairment resided at the receptor level. The potential of the opioids, clonidine and R-PIA to increase G alpha-related in vitro hydrolysis of GTP was also re-established after injecting myr+-Gi2 alpha subunits into Gi2-knocked-down mice. Myr+-Gi2 alpha subunits pre-incubated with GTPgammaS or GDPbetaS before i.c.v. injection did not improve the activity of agonists in vivo (antinociception) or in vitro (regulation of low Km GTPase). After impairing the function of PKCbeta1 by antisense treatment or with the inhibitor H7, the effect of myr+-G alpha subunits on agonist potency was prevented. Electron microscope analysis showed the entry of gold-conjugated myr+-G alpha subunits into neural cells. These particles were found in the cytoplasm, associated with the plasma membranes of different neuronal processes and also in synaptic junctions. In cultured neurons and astrocytes myr+-Gi2 alpha-associated fluorescence was internalised in a dose-dependent manner and distributed in the plasma membrane and cytosol, as well as in nuclei of dividing astrocytes. Thus, G alpha subunits in CSF enter into neurons and functionally couple to the receptor-triggered signalling cascade. As G-proteins have been implicated in the pathophysiology of several neural disorders, this finding may be valuable in the therapy of such dysfunctions.

机译：在反义'敲除'或百日咳毒素治疗中其Gi / o蛋白功能受损的小鼠中注射myr + -Gi / oα亚基可恢复β-内啡肽，吗啡，DPDPE，可乐定和神经降压素产生抗伤害感受的功效。实际上受损的G蛋白类别的Myr + -G alpha亚基比起与之相关但与之相关的myr + -G alpha亚基更有效。注意到选择性，因为只有外源性的myr + -G alpha亚基会影响（增强）G alpha缺陷信号系统中激动剂的活性。当损伤位于受体水平时，该处理对激动剂效力几乎没有影响。将myr +-Gi2α亚基注入Gi2减低的小鼠体内后，阿片类药物，可乐定和R-PIA增加Gα相关的GTP体外水解的潜力也重新建立。在i.c.v.之前与GTPgammaS或GDPbetaS预温育的Myr + -Gi2 alpha亚基。注射不能改善激动剂的体内（抗伤害感受）或体外（低Km GTPase的调节）活性。通过反义处理或使用抑制剂H7破坏PKCbeta1的功能后，可防止myr + -Gα亚基对激动剂效力的影响。电子显微镜分析显示金共轭的myr + -G alpha亚基进入神经细胞。这些颗粒存在于细胞质中，与不同神经元过程的质膜有关，也存在于突触连接中。在培养的神经元和星形胶质细胞中，与myr + -Gi2α相关的荧光以剂量依赖的方式内在化，并分布在质膜和细胞溶胶以及星形胶质细胞的分裂核中。因此，CSF中的G alpha亚基进入神经元，并在功能上耦合至受体触发的信号级联。由于G蛋白已经牵涉到几种神经系统疾病的病理生理中，因此这一发现在治疗此类功能障碍中可能是有价值的。

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《Neuropharmacology》 |1999年第12期|共13页
作者
Garzon J; Rodriguez Diaz-M; DeAntonio I; DeFelipe J; Rodriguez JR; Sanchez Blazquez-P;
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正文语种 eng
中图分类药理学;
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Analgesics; Cerebral Cortex; GTP-Binding Proteins; GTP Phosphohydrolases; 镇痛药; 大脑皮质; GTP-结合蛋白质类;

机译：Analgesics;Cerebral Cortex;GTP-Binding Proteins;GTP Phosphohydrolases;镇痛药;大脑皮质;GTP-结合蛋白质类;

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1. Myr+-Gi2 alpha and Go alpha subunits restore the efficacy of opioids, clonidine and neurotensin giving rise to antinociception in G-protein knock-down mice. [J] . Garzon J, Rodriguez Diaz-M, DeAntonio I, Neuropharmacology . 1999,第12期

机译：Myr + -Gi2 alpha和Go alpha亚基可恢复阿片类药物，可乐定和神经降压素的功效，从而在G蛋白敲除小鼠中产生抗伤害感受作用。
2. Effect of deletion of the major brain G-protein alpha subunit (alpha(o)) on coordination of G-protein subunits and on adenylyl cyclase activity. [J] . Mende U, Zagrovic B, Cohen A, Journal of Neuroscience Research . 1998,第2期

机译：主要脑G蛋白α亚基（alpha（o））的删除对G蛋白亚基的协调和腺苷酸环化酶活性的影响。
3. Antinociception mediated by alpha(2)-adrenergic activation involves increasing tumor necrosis factor alpha (TNFalpha) expression and restoring TNFalpha and alpha(2)-adrenergic inhibition of norepinephrine release. [J] . Spengler RN, Sud R, Knight PR, Neuropharmacology . 2007,第2期

机译：由α（2）-肾上腺素激活介导的抗伤害感受涉及增加肿瘤坏死因子α（TNFalpha）的表达并恢复TNFα和α（2）-肾上腺素对去甲肾上腺素释放的抑制作用。
4. Vaccine efficacy of live-attenuated virus, whole-virus inactivated and alphavirus vectored subunit vaccines against antigenically distinct H3N2 swine influenza A viruses [C] . Eugenio J. Abente, Nicola S. Lewis, Mark A. Mogler, Annual^Meeting of the American^Association^of^Swine^Veterinarians. . 2016

机译：活病毒的疫苗疗效，全病毒灭活和alphavirus向量亚单位疫苗反对抗原性不同的H3N2猪流感病毒
5. alpha-Adrenoceptor and opioid receptor modulation of clonidine-induced antinociception. [O] . F. Sierralta, D. Naquira, G. Pinardi, 1996

机译：可乐定诱导的抗伤害感受的α-肾上腺素受体和阿片受体调节。
6. Membrane localization of the pertussis toxin-sensitive G-protein subunits alpha i-2 and alpha i-3 and expression of a metallothionein-alpha i-2 fusion gene in LLC-PK1 cells. [O] . Ercolani, L, Stow, J L, Boyle, J F, 1990

机译：百日咳毒素敏感的G蛋白亚基alpha i-2和alpha i-3的膜定位以及在LLC-PK1细胞中金属硫蛋白-alpha i-2融合基因的表达。

Myr+-Gi2 alpha and Go alpha subunits restore the efficacy of opioids, clonidine and neurotensin giving rise to antinociception in G-protein knock-down mice.

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