首页> 美国卫生研究院文献>The Journal of Neuroscience >Lateral Hypothalamic Orexin/Hypocretin Neurons That Project to Ventral Tegmental Area Are Differentially Activated with Morphine Preference
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Lateral Hypothalamic Orexin/Hypocretin Neurons That Project to Ventral Tegmental Area Are Differentially Activated with Morphine Preference

机译:投射到腹侧被盖区的下丘脑外食欲素/降血糖素神经元被吗啡偏爱激活。

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摘要

Orexin (or hypocretin) is synthesized exclusively in dorsomedial, perifornical, and lateral hypothalamus (LH). These neurons are implicated in several functions, including reward processing. We examined the ventral tegmental area (VTA) as a possible site of orexin action for drug preference during protracted morphine abstinence, and studied functional topography of orexin projections to VTA. Male Sprague Dawley rats were used to investigate whether orexin cells that project to VTA exhibit Fos activation with morphine conditioned place preference (CPP), and whether these cells exhibit increased Fos with morphine CPP during protracted abstinence. Unilateral injections of a retrograde tracer (WGA-Au, 350–400 nl) were made into the VTA or a nonreward area, locus ceruleus, and morphine or placebo pellets were implanted for 14 d. Approximately 2 weeks after pellet removal (post dependence), CPP conditioning and testing were conducted. Triple labeling for WGA-Au, Fos, and orexin revealed that the percentage of VTA-projecting orexin neurons Fos activated on the CPP test day significantly increased in post-dependent (vs nondependent) rats, and was exclusive to LH orexin neurons (not dorsomedial or perifornical). Post-dependent animals showed a positive correlation between CPP scores and percentages of Fos-activated, caudal VTA-projecting LH orexin cells. Unlike afferents to caudal VTA, percentages of rostral VTA-projecting, LH orexin cells that were Fos activated showed a positive correlation with CPP only in nondependent animals. Fos in LC-projecting orexin cells was not correlated with CPP in any group. These results indicate that VTA is a heterogeneous and functionally significant target of orexin neurons for morphine reward during protracted abstinence.
机译:食欲素(或降钙素)仅在背体,椎旁和下丘脑(LH)中合成。这些神经元涉及多种功能,包括奖励处理。我们研究了腹侧被盖区(VTA)作为吗啡禁欲症长期禁食期间orexin作用的药物可能的作用部位,并研究了orexin投射至VTA的功能性地形。使用雄性Sprague Dawley大鼠研究了投射到VTA的orexin细胞是否在吗啡条件位置偏爱(CPP)下表现出Fos活化,以及在禁欲期间这些细胞是否在吗啡CPP下表现出增加的Fos。将单侧逆行示踪剂(WGA-Au,350–400 nl)注射入VTA或非奖励区域,将蓝斑位置注入吗啡或安慰剂药丸14 d。去除颗粒后约2周(依赖后),进行CPP调理和测试。 WGA-Au,Fos和orexin的三重标记显示,在依赖后(相对于非依赖)大鼠中,在CPP测试日激活的VTA投射的orexin神经元Fos的百分比显着增加,并且是LH orexin神经元所独有的(不是背囊的)或perifronical)。依赖后的动物显示CPP评分与Fos激活的,尾部VTA投射LH食欲素细胞的百分比之间呈正相关。与传入VTA的尾巴不同,仅在非依赖性动物中,被Fos激活的经鼻VTA投射的LH orexin细胞的百分比与CPP呈正相关。在任何组中,投射LC的食欲素细胞中的Fos与CPP均不相关。这些结果表明,VTA是长期禁欲期间吗啡奖励的食欲素神经元的异质性和功能性重要靶标。

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