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本文引用的文献

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Measuring the incentive value of escalating doses of heroin in heroin-dependent Fischer rats during acute spontaneous withdrawal.在急性自发戒断期间测量递增剂量海洛因对依赖海洛因的 Fischer 大鼠的激励价值。
Psychopharmacology (Berl). 2012 Jan;219(1):59-72. doi: 10.1007/s00213-011-2380-7. Epub 2011 Jul 7.
2
Dose preference and dose escalation in extended-access cocaine self-administration in Fischer and Lewis rats.延长可卡因自我给药中 Fischer 和 Lewis 大鼠的剂量偏好和剂量递增。
Psychopharmacology (Berl). 2010 Aug;211(3):313-23. doi: 10.1007/s00213-010-1899-3. Epub 2010 Jun 19.
3
Strain differences in the dose-response relationship for morphine self-administration and impulsive choice between Lewis and Fischer 344 rats.Lewis 大鼠和 Fischer 344 大鼠吗啡自身给药和冲动选择的剂量反应关系的品系差异。
J Psychopharmacol. 2011 Jun;25(6):783-91. doi: 10.1177/0269881110367444. Epub 2010 May 20.
4
Two modes of intense cocaine bingeing: increased persistence after social defeat stress and increased rate of intake due to extended access conditions in rats.两种强烈的可卡因暴饮暴食模式:社交挫败应激后持续性增加以及因大鼠长期接触条件导致摄入速率增加。
Psychopharmacology (Berl). 2009 Sep;206(1):109-20. doi: 10.1007/s00213-009-1584-6. Epub 2009 Jun 10.
5
Opiate-agonist induced taste aversion learning in the Fischer 344 and Lewis inbred rat strains: evidence for differential mu opioid receptor activation.阿片类激动剂诱导的费希尔344和刘易斯近交系大鼠味觉厌恶学习:μ阿片受体差异激活的证据。
Pharmacol Biochem Behav. 2009 Oct;93(4):397-405. doi: 10.1016/j.pbb.2009.06.001. Epub 2009 Jun 7.
6
Strain differences between Lewis and Fischer 344 rats in the modulation of dopaminergic receptors after morphine self-administration and during extinction.吗啡自我给药及消退过程中,Lewis大鼠和Fischer 344大鼠在多巴胺能受体调节方面的品系差异。
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7
Strain differences in patterns of drug-intake during prolonged access to cocaine self-administration.长期可获得可卡因自我给药期间药物摄入模式的品系差异。
Behav Neurosci. 2009 Feb;123(1):156-64. doi: 10.1037/a0013727.
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Bidirectional translational research: Progress in understanding addictive diseases.双向转化研究:成瘾性疾病理解方面的进展
Neuropharmacology. 2009;56 Suppl 1(Suppl 1):32-43. doi: 10.1016/j.neuropharm.2008.07.042. Epub 2008 Aug 7.
9
Self-administration of drugs in animals and humans as a model and an investigative tool.将药物自我给药作为动物和人类的一种模型及研究工具。
Addiction. 2007 Dec;102(12):1863-70. doi: 10.1111/j.1360-0443.2007.02011.x.
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Stress, dysregulation of drug reward pathways, and the transition to drug dependence.压力、药物奖赏通路失调与向药物依赖的转变。
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延长_access 海洛因自我给药中 Lewis 和 Fischer 大鼠的剂量递增和剂量偏好。

Dose escalation and dose preference in extended-access heroin self-administration in Lewis and Fischer rats.

机构信息

The Rockefeller University, Laboratory of the Biology of Addictive Diseases, 1230 York Avenue, Box 171, New York, NY 10065, USA.

出版信息

Psychopharmacology (Berl). 2012 Mar;220(1):163-72. doi: 10.1007/s00213-011-2464-4. Epub 2011 Sep 6.

DOI:10.1007/s00213-011-2464-4
PMID:21894484
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3359091/
Abstract

RATIONALE

A genetic component may be involved in different stages of the progression of drug addiction. Heroin users escalate unit doses and frequency of self-administration events over time. Rats that self-administer drugs of abuse over extended sessions escalate the amount of drug infused over days.

OBJECTIVES

Using a recently developed model of extended-access self-administration allowing for subject-controlled dose escalation of the unit dose, thus potentially escalating the unit dose and number of infusions, we compared for the first time two genetically different inbred rat strains, Fischer and Lewis.

METHODS

Extended (18 h/day) self-administration lasted for 14 days. Rats had access to two active levers associated with two different unit doses of heroin. If a rat showed preference for the higher unit dose, then the available doses were escalated in the following session. Four heroin unit doses were available (20, 50, 125, 250 μg/kg per infusion).

RESULTS

Fischer rats did not escalate the unit dose of heroin self-administered; daily amount of heroin administered remained low, with a mean daily intake of 1.27 ± 0.22 mg/kg per session. In marked contrast, Lewis rats escalated the total daily amount of heroin self-administered from 3.94 ± 0.82 mg/kg on day 1 to 8.95 ± 2.2 mg/kg on day 14; almost half of the subjects preferred a higher heroin dose than Fischer rats.

CONCLUSION

These data are consistent with the hypothesis that Lewis rats are prone to opiate taking and escalation, and are in agreement with our previous data obtained with cocaine.

摘要

背景

遗传因素可能参与了药物成瘾进展的不同阶段。海洛因使用者随着时间的推移会增加单位剂量和自我给药事件的频率。滥用药物的大鼠在长时间内自我给药会增加多天内注入的药物量。

目的

使用最近开发的延长给药自我给药模型,允许受试者控制单位剂量的递增,从而有可能递增单位剂量和输注次数,我们首次比较了两种遗传上不同的近交系大鼠,即 Fischer 和 Lewis。

方法

延长(每天 18 小时)自我给药持续 14 天。大鼠可以接触到两个与两种不同单位剂量海洛因相关的主动杠杆。如果大鼠表现出对较高单位剂量的偏好,那么在下一个疗程中可增加可用剂量。有四个海洛因单位剂量可供选择(每次输注 20、50、125、250μg/kg)。

结果

Fischer 大鼠未递增自我给予的海洛因单位剂量;每日给予的海洛因量仍然较低,每个疗程的平均每日摄入量为 1.27±0.22mg/kg。相比之下,Lewis 大鼠从第 1 天的 3.94±0.82mg/kg 增加到第 14 天的 8.95±2.2mg/kg,递增了每日给予的海洛因总量;几乎一半的受试者更喜欢比 Fischer 大鼠更高的海洛因剂量。

结论

这些数据与 Lewis 大鼠易受阿片类药物摄入和递增影响的假设一致,并与我们以前用可卡因获得的数据一致。