前额叶皮层在应激和可卡因诱导的大鼠可卡因觅求复燃中的作用。
A role for the prefrontal cortex in stress- and cocaine-induced reinstatement of cocaine seeking in rats.
作者信息
Capriles Nancy, Rodaros Demetra, Sorge Robert E, Stewart Jane
机构信息
Center for Studies in Behavioral Neurobiology, Department of Psychology, Concordia University, 1455 de Maisonneuve Blvd., Montreal, Quebec, Canada H3G 1M8, Canada.
Mental Health Research Institute, University of Michigan, 205 Zina, Pitcher Place, MI 48109-0720, USA, USA.
出版信息
Psychopharmacology (Berl). 2003 Jul;168(1-2):66-74. doi: 10.1007/s00213-002-1283-z. Epub 2002 Nov 20.
RATIONALE AND OBJECTIVE
It is well established that stress induces reinstatement of drug seeking in an animal model of relapse. Here we studied the role of the medial prefrontal cortex (mPFC) and orbitofrontal cortex (OFC) in foot-shock stress-induced reinstatement of cocaine seeking.
METHODS
Groups of rats were trained to self-administer cocaine (0.5 mg/kg per infusion, i.v., 3 h/day for 9 days) and after ten drug-free days were exposed to extinction and reinstatement test sessions. Each 60 min of extinction was separated by a 30-min time-out period after which the lever and stimulus lights were reintroduced. Rats were given four 1-h extinction sessions on day 1 and then on subsequent days were given two to three 1-h extinction sessions that were followed by a 3-h test for reinstatement. Tests were run every 48 h. In one set of experiments, the effects of inactivation of the prelimbic (PL), infralimbic (IL) or OFC by tetrodotoxin (TTX, 5 ng/0.5 micro l per side) on reinstatement induced by foot shock (5 min, intermittent, 1 mA) or priming injections of cocaine (20 mg/kg, i.p.) were determined. In a second set, the effects of infusions of the D1-like and D2-like dopamine receptor antagonists (SCH 23390 and raclopride) were studied using the same methods.
RESULTS
TTX infusions into the PL cortex blocked both foot shock and cocaine-induced reinstatement. TTX into OFC attenuated foot-shock-induced, but not cocaine-induced reinstatement. Infusions into IL were ineffective. Infusions of SCH 22390 (0.25 micro g/0.5 micro l per side) into either PL or OFC blocked foot-shock-induced reinstatement, but infusions into PL had no effect on cocaine-induced reinstatement. Raclopride (5 micro g/0.5 micro l per side) had no effect on foot-shock-induced reinstatement in either PL or OFC or on cocaine-induced reinstatement when infused into PL. Neither TTX nor SCH23390 infusions into PL or OFC had any effect on lever pressing for sucrose.
CONCLUSIONS
These results suggest that the PL and OFC regions form part of the circuitry mediating the effects of foot shock stress on reinstatement of drug seeking and that the PL region may be a common pathway for cue, drug and foot-shock stress-induced reinstatement of drug seeking.
原理与目的
在复发的动物模型中,应激诱导觅药行为的恢复这一点已得到充分证实。在此,我们研究了内侧前额叶皮质(mPFC)和眶额皮质(OFC)在足部电击应激诱导的可卡因觅药行为恢复中的作用。
方法
将大鼠分组训练以自我注射可卡因(每次注射0.5毫克/千克,静脉注射,每天3小时,共9天),在停药10天后进行消退和恢复测试。每次60分钟的消退过程中间隔30分钟的休息期,之后重新引入杠杆和刺激灯。第1天给予大鼠4次1小时的消退训练,随后几天给予2至3次1小时的消退训练,之后进行3小时的恢复测试。测试每48小时进行一次。在一组实验中,通过向内侧前额叶皮质(PL)、眶额皮质(OFC)或前边缘下皮质(IL)注射河豚毒素(TTX,每侧5纳克/0.5微升)来灭活这些区域,以确定其对足部电击(5分钟,间歇性,1毫安)或可卡因激发注射(20毫克/千克,腹腔注射)诱导的恢复的影响。在第二组实验中,使用相同方法研究注射D1样和D2样多巴胺受体拮抗剂(SCH 23390和雷氯必利)的影响。
结果
向PL皮质注射TTX可阻断足部电击和可卡因诱导的恢复。向OFC注射TTX可减弱足部电击诱导的恢复,但不能减弱可卡因诱导的恢复。向IL注射无效。向PL或OFC注射SCH 22390(每侧0.25微克/0.5微升)可阻断足部电击诱导的恢复,但向PL注射对可卡因诱导的恢复无影响。雷氯必利(每侧5微克/0.5微升)对PL或OFC中足部电击诱导的恢复无影响,向PL注射时对可卡因诱导的恢复也无影响。向PL或OFC注射TTX或SCH23390对蔗糖杠杆按压均无影响。
结论
这些结果表明,PL和OFC区域构成了介导足部电击应激对觅药行为恢复影响的神经回路的一部分,并且PL区域可能是线索、药物和足部电击应激诱导的觅药行为恢复的共同通路。
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