首页> 外文期刊>Neuropeptides: An International Journal >Chronic administration of nandrolone increases susceptibility to morphine dependence without correlation with LVV-hemorphin 7 in rats
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Chronic administration of nandrolone increases susceptibility to morphine dependence without correlation with LVV-hemorphin 7 in rats

机译:Nandrolone的慢性施用增加了对吗啡依赖的易感性,而不与大鼠的LVV-血红素7相关

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LVV-hemorphin 7 (LVVYPWTQRF; LVV-H7), an N-terminal fragment of the beta-chain of hemoglobin cleaved by cathepsin D/pepsin, is an atypical endogenous opioid peptide that is found in high concentration in blood. LVV-H7 acts as a-opioid agonist and an inhibitor of insulin-regulated aminopeptidase. Subchronic administration of anabolic androgenic steroids (AAS) has been clinically proven to induce the synthesis of erythrocytes and increase hemoglobin concentrations. Patients with a history of AAS abuse are more susceptible to opioid abuse. We hypothesized that this association could be at least partially attributed to the sensitization of the mesocorticolimbic dopaminergic pathway by LVV-H7. Using the conditioned place preference test and neurochemical analysis, we investigated the possible mechanism underlying the effect of chronic nandrolone administration on morphine induced reward and its correlation with LVV-H7 in rats. Either LVV-H7 may not sensitize the rewarding neural circuits or its inhibition on locomotor activity could mask reward-related behaviors. Chronic nandrolone pretreatment indeed caused a significant reward by low dose morphine, which did not cause any reward in control rats. However, coadministration of anti-LVV-H7 antiserum with nandrolone did not block this effect. This may rule out the possibility of the involvement of LVV-H7 in the action of nandrolone to intensify morphine-induced reward. Moreover, the serum level of LVV-H7 was mildly increased in response to chronic nandrolone administration in our animal model. According to the current clinical observations, we may conclude that the chronic administration of nandrolone can increase susceptibility to morphine dependence, but that this effect is not related to elevated LVV-H7. (C) 2016 Elsevier Ltd. All rights reserved.
机译:LVV-血红素7(LVVYPWTQRF; LVV-H7),由组织蛋白酶D /百辛粘合的血红蛋白β链的N-末端片段是一种非典型内源性阿片类肽,其在血液中高浓度。 LVV-H7充当阿片类激动剂和胰岛素调节氨基肽酶的抑制剂。在临床上证明了代谢雄激素类固醇(AAS)的次级施用以诱导红细胞的合成并增加血红蛋白浓度。 AAS滥用史的患者更容易受到阿片类药物的影响。我们假设该协会至少部分地归因于LVV-H7的含有Mesocorcolimbic多巴胺能途径的敏化。使用调节的地点偏好测试和神经化学分析,我们研究了慢性无龙龙酮施用对吗啡诱导奖励的影响的可能机制及其与大鼠LVV-H7的相关性。 LVV-H7可能不会敏感奖励神经电路或其对运动活动的抑制可能会掩盖奖励相关的行为。慢性Nandrolone预处理确实引起了低剂量吗啡的显着奖励,这并没有导致对照大鼠的任何奖励。然而,使用Nandrolone的抗LVV-H7抗血清的共同分析并没有阻断这种效果。这可能排除LVV-H7参与Nandrolone的作用,以加剧吗啡诱导的奖励。此外,响应于我们的动物模型中的慢性Nandrolone给药,温和地增加了LVV-H7的血清水平。根据目前的临床观察,我们可以得出结论,Nandrolone的慢性施用可以增加对吗啡依赖性的敏感性,但这种效果与升高的LVV-H7无关。 (c)2016 Elsevier Ltd.保留所有权利。

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