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脑烟碱型乙酰胆碱受体可及性及其对戒烟治疗的反应:一项随机试验。

Brain nicotinic acetylcholine receptor availability and response to smoking cessation treatment: a randomized trial.

机构信息

Department of Research, VA Greater Los Angeles Healthcare System, Los Angeles, California2Department of Psychiatry, University of California, Los Angeles.

Department of Psychiatry, Duke University, Durham, North Carolina.

出版信息

JAMA Psychiatry. 2014 Jul 1;71(7):797-805. doi: 10.1001/jamapsychiatry.2014.138.

Abstract

IMPORTANCE

Cigarette smoking leads to upregulation of nicotinic acetylcholine receptors (nAChRs) in the human brain, including the common α4β2* nAChR subtype. While subjective aspects of tobacco dependence have been extensively examined as predictors of quitting smoking with treatment, no studies to our knowledge have yet reported the relationship between the extent of pretreatment upregulation of nAChRs and smoking cessation.

OBJECTIVE

To determine whether the degree of nAChR upregulation in smokers predicts quitting with a standard course of treatment.

DESIGN, SETTING, AND PARTICIPANTS: Eighty-one tobacco-dependent cigarette smokers (volunteer sample) underwent positron emission tomographic (PET) scanning of the brain with the radiotracer 2-FA followed by 10 weeks of double-blind, placebo-controlled treatment with nicotine patch (random assignment). Pretreatment specific binding volume of distribution (VS/fP) on PET images (a value that is proportional to α4β2* nAChR availability) was determined for 8 brain regions of interest, and participant-reported ratings of nicotine dependence, craving, and self-efficacy were collected. Relationships between these pretreatment measures, treatment type, and outcome were then determined. The study took place at academic PET and clinical research centers.

MAIN OUTCOMES AND MEASURES

Posttreatment quit status after treatment, defined as a participant report of 7 or more days of continuous abstinence and an exhaled carbon monoxide level of 3 ppm or less.

RESULTS

Smokers with lower pretreatment VS/fP values (a potential marker of less severe nAChR upregulation) across all brain regions studied were more likely to quit smoking (multivariate analysis of covariance, F8,69 = 4.5; P < .001), regardless of treatment group assignment. Furthermore, pretreatment average VS/fP values provided additional predictive power for likelihood of quitting beyond the self-report measures (stepwise binary logistic regression, likelihood ratio χ21 = 19.8; P < .001).

CONCLUSIONS AND RELEVANCE

Smokers with less upregulation of available α4β2* nAChRs have a greater likelihood of quitting with treatment than smokers with more upregulation. In addition, the biological marker studied here provided additional predictive power beyond subjectively rated measures known to be associated with smoking cessation outcome. While the costly, time-consuming PET procedure used here is not likely to be used clinically, simpler methods for examining α4β2* nAChR upregulation could be tested and applied in the future to help determine which smokers need more intensive and/or lengthier treatment.

TRIAL REGISTRATION

clinicaltrials.gov Identifier: NCT01526005.

摘要

重要性

吸烟会导致人类大脑中的烟碱型乙酰胆碱受体(nAChRs)上调,包括常见的α4β2* nAChR 亚型。尽管已经广泛研究了烟草依赖的主观方面作为治疗戒烟的预测因素,但据我们所知,还没有研究报告预处理 nAChR 上调程度与戒烟之间的关系。

目的

确定吸烟者的 nAChR 上调程度是否可以预测标准疗程的戒烟。

设计、地点和参与者:81 名依赖香烟的吸烟者(志愿者样本)接受了放射性示踪剂 2-FA 的正电子发射断层扫描(PET),然后进行了 10 周的尼古丁贴片双盲、安慰剂对照治疗(随机分配)。在 8 个感兴趣的脑区中,确定了 PET 图像上特定结合容积分布(VS/fP)的预处理值(与α4β2* nAChR 可用性成正比的数值),并收集了参与者报告的尼古丁依赖、渴望和自我效能感评分。然后确定这些预处理测量值、治疗类型和结果之间的关系。该研究在学术 PET 和临床研究中心进行。

主要结果和测量

治疗后的戒烟状态,定义为参与者报告 7 天或以上的连续戒断和呼出的一氧化碳水平为 3ppm 或以下。

结果

在所有研究的脑区中,预处理 VS/fP 值较低(nAChR 上调程度较低的潜在标志物)的吸烟者更有可能戒烟(多变量协方差分析,F8,69=4.5;P<.001),而不管治疗组的分配如何。此外,预处理平均 VS/fP 值除了自我报告的测量值外,还为戒烟的可能性提供了额外的预测能力(逐步二元逻辑回归,似然比 χ21=19.8;P<.001)。

结论和相关性

与 nAChR 上调程度较高的吸烟者相比,α4β2* nAChR 可利用性上调程度较低的吸烟者更有可能通过治疗戒烟。此外,与已知与戒烟结果相关的主观评分相比,这里研究的生物标志物提供了额外的预测能力。虽然这里使用的昂贵、耗时的 PET 程序不太可能在临床上使用,但未来可以测试和应用更简单的方法来检查α4β2* nAChR 的上调情况,以帮助确定哪些吸烟者需要更密集和/或更长时间的治疗。

试验注册

clinicaltrials.gov 标识符:NCT01526005。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b2ff/4634637/84e53dc72b90/nihms732405f1.jpg

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