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Alcohol's Negative Emotional Side: The Role of Stress Neurobiology in Alcohol Use Disorder. 酒精的消极情绪面:应激神经生物学在酒精使用障碍中的作用。
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2022-01-01 DOI: 10.35946/arcr.v42.1.12
Rajita Sinha

This article is part of a Festschrift commemorating the 50th anniversary of the National Institute on Alcohol Abuse and Alcoholism (NIAAA). Established in 1970, first as part of the National Institute of Mental Health and later as an independent institute of the National Institutes of Health, NIAAA today is the world's largest funding agency for alcohol research. In addition to its own intramural research program, NIAAA supports the entire spectrum of innovative basic, translational, and clinical research to advance the diagnosis, prevention, and treatment of alcohol use disorder and alcohol-related problems. To celebrate the anniversary, NIAAA hosted a 2-day symposium, "Alcohol Across the Lifespan: 50 Years of Evidence-Based Diagnosis, Prevention, and Treatment Research," devoted to key topics within the field of alcohol research. This article is based on Dr. Sinha's presentation at the event. NIAAA Director George F. Koob, Ph.D., serves as editor of the Festschrift.

本文是纪念美国国家酒精滥用和酒精中毒研究所(NIAAA)成立50周年纪念活动的一部分。NIAAA成立于1970年,最初是国家精神卫生研究所的一部分,后来成为国家卫生研究所的一个独立研究所,今天是世界上最大的酒精研究资助机构。除了自己的内部研究项目外,NIAAA还支持所有创新的基础、转化和临床研究,以推进酒精使用障碍和酒精相关问题的诊断、预防和治疗。为了庆祝周年纪念日,NIAAA举办了为期两天的研讨会,“酒精在生命中的作用:50年的循证诊断、预防和治疗研究”,致力于酒精研究领域的关键话题。这篇文章是根据Sinha博士在会议上的发言写成的。NIAAA主任George F. Koob博士担任该杂志的编辑。
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引用次数: 3
Alcohol Use Disorder and Alcohol-Associated Liver Disease. 酒精使用障碍和酒精相关肝脏疾病
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2022-01-01 DOI: 10.35946/arcr.v42.1.13
Resham Ramkissoon, Vijay H Shah

This article is part of a Festschrift commemorating the 50th anniversary of the National Institute on Alcohol Abuse and Alcoholism (NIAAA). Established in 1970, first as part of the National Institute of Mental Health and later as an independent institute of the National Institutes of Health, NIAAA today is the world's largest funding agency for alcohol research. In addition to its own intramural research program, NIAAA supports the entire spectrum of innovative basic, translational, and clinical research to advance the diagnosis, prevention, and treatment of alcohol use disorder and alcohol-related problems. To celebrate the anniversary, NIAAA hosted a 2-day symposium, "Alcohol Across the Lifespan: 50 Years of Evidence-Based Diagnosis, Prevention, and Treatment Research," devoted to key topics within the field of alcohol research. This article is based on Dr. Shah's presentation at the event. NIAAA Director George F. Koob, Ph.D., serves as editor of the Festschrift.

本文是纪念美国国家酒精滥用和酒精中毒研究所(NIAAA)成立50周年纪念活动的一部分。NIAAA成立于1970年,最初是国家精神卫生研究所的一部分,后来成为国家卫生研究所的一个独立研究所,今天是世界上最大的酒精研究资助机构。除了自己的内部研究项目外,NIAAA还支持所有创新的基础、转化和临床研究,以推进酒精使用障碍和酒精相关问题的诊断、预防和治疗。为了庆祝周年纪念日,NIAAA举办了为期两天的研讨会,“酒精在生命中的作用:50年的循证诊断、预防和治疗研究”,致力于酒精研究领域的关键话题。这篇文章是根据沙阿博士在会议上的发言写成的。NIAAA主任George F. Koob博士担任该杂志的编辑。
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引用次数: 5
Alcohol and Cannabinoids - From the Editors. 酒精和大麻素——来自编辑。
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2022-01-01 DOI: 10.35946/arcr.v42.1.10
Jane Metrik, Sachin Patel
Alcohol is frequently used in association with cannabis, with co-use now perceived as normative with expanding cannabis legalization. Cannabinoid products are increasingly used for a number of medical and recreational purposes, including to enhance alcohol-reinforcing properties or in some cases to substitute for alcohol. Rates of alcohol use disorder (AUD) are higher among cannabis users relative to nonusers, with approximately 60% of individuals with current cannabis use disorder also meeting criteria for current AUD. 1,2 Co-use is linked with heavy and problematic alcohol consumption, which in turn increases risk of alcohol-related diseases such as alcohol-associated liver disease. Co-use is also linked with a number of negative consequences, including behavioral risks, 3 risk for driving safety, psychiatric comorbidity,
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引用次数: 2
Age, Period, and Cohort Effects in Alcohol Use in the United States in the 20th and 21st Centuries: Implications for the Coming Decades. 20世纪和21世纪美国酒精使用的年龄、时期和队列效应:对未来几十年的影响
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2022-01-01 DOI: 10.35946/arcr.v42.1.02
Katherine M Keyes

This article is part of a Festschrift commemorating the 50th anniversary of the National Institute on Alcohol Abuse and Alcoholism (NIAAA). Established in 1970, first as part of the National Institute of Mental Health and later as an independent institute of the National Institutes of Health, NIAAA today is the world's largest funding agency for alcohol research. In addition to its own intramural research program, NIAAA supports the entire spectrum of innovative basic, translational, and clinical research to advance the diagnosis, prevention, and treatment of alcohol use disorder and alcohol-related problems. To celebrate the anniversary, NIAAA hosted a 2-day symposium, "Alcohol Across the Lifespan: 50 Years of Evidence-Based Diagnosis, Prevention, and Treatment Research," devoted to key topics within the field of alcohol research. This article is based on Dr. Keyes' presentation at the event. NIAAA Director George F. Koob, Ph.D., serves as editor of the Festschrift.

本文是纪念美国国家酒精滥用和酒精中毒研究所(NIAAA)成立50周年纪念活动的一部分。NIAAA成立于1970年,最初是国家精神卫生研究所的一部分,后来成为国家卫生研究所的一个独立研究所,今天是世界上最大的酒精研究资助机构。除了自己的内部研究项目外,NIAAA还支持所有创新的基础、转化和临床研究,以推进酒精使用障碍和酒精相关问题的诊断、预防和治疗。为了庆祝周年纪念日,NIAAA举办了为期两天的研讨会,“酒精在生命中的作用:50年的循证诊断、预防和治疗研究”,致力于酒精研究领域的关键话题。这篇文章是根据凯斯博士在会议上的发言写成的。NIAAA主任George F. Koob博士担任该杂志的编辑。
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引用次数: 7
Looking Back, Looking Forward: Current Medications and Innovative Potential Medications to Treat Alcohol Use Disorder. 回顾过去,展望未来:治疗酒精使用障碍的现有药物和创新潜在药物。
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2022-01-01 DOI: 10.35946/arcr.v42.1.11
Barbara J Mason

This article is part of a Festschrift commemorating the 50th anniversary of the National Institute on Alcohol Abuse and Alcoholism (NIAAA). Established in 1970, first as part of the National Institute of Mental Health and later as an independent institute of the National Institutes of Health, NIAAA today is the world's largest funding agency for alcohol research. In addition to its own intramural research program, NIAAA supports the entire spectrum of innovative basic, translational, and clinical research to advance the diagnosis, prevention, and treatment of alcohol use disorder and alcohol-related problems. To celebrate the anniversary, NIAAA hosted a 2-day symposium, "Alcohol Across the Lifespan: 50 Years of Evidence-Based Diagnosis, Prevention, and Treatment Research," devoted to key topics within the field of alcohol research. This article is based on Dr. Mason's presentation at the event. NIAAA Director George F. Koob, Ph.D., serves as editor of the Festschrift.

本文是纪念美国国家酒精滥用和酒精中毒研究所(NIAAA)成立50周年纪念活动的一部分。NIAAA成立于1970年,最初是国家精神卫生研究所的一部分,后来成为国家卫生研究所的一个独立研究所,今天是世界上最大的酒精研究资助机构。除了自己的内部研究项目外,NIAAA还支持所有创新的基础、转化和临床研究,以推进酒精使用障碍和酒精相关问题的诊断、预防和治疗。为了庆祝周年纪念日,NIAAA举办了为期两天的研讨会,“酒精在生命中的作用:50年的循证诊断、预防和治疗研究”,致力于酒精研究领域的关键话题。这篇文章是根据梅森博士在会议上的发言写成的。NIAAA主任George F. Koob博士担任该杂志的编辑。
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引用次数: 1
Alcohol-Endocannabinoid Interactions: Implications for Addiction-Related Behavioral Processes. 酒精-内源性大麻素相互作用:成瘾相关行为过程的含义。
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2022-01-01 DOI: 10.35946/arcr.v42.1.09
Antonia Serrano, Luis A Natividad

Purpose: The endogenous cannabinoid system is involved in several physiological functions in the central nervous system including the modulation of brain reward circuitry and emotional homeostasis. Substantial evidence implicates brain endocannabinoid signaling in the processing of drug-induced reward states, wherein repeated exposure besets pathological changes in activity that contribute to the progression of alcohol use disorder. This review provides a narrative summary of recent studies exploring the interaction between alcohol exposure and changes in endocannabinoid signaling that may underlie the development of alcohol use disorder.

Search methods: The authors began with an initial search for review articles to assist in the identification of relevant literature. This was followed by separate searches for primary literature and recent studies. The search terms "alcohol/ethanol" and "endocannabinoids" were applied, along with terms that covered specific objectives in reinforcement and addiction behavior. The content was further refined by excluding articles containing a broad focus on psychiatric disorders, polysubstance abuse, non-cannabinoid signaling lipids, and other criteria.

Search results: The initial search yielded a total of 49 review articles on PubMed, 13 on ScienceDirect, and 17 on Wiley Online, from which the authors garnered information from a total of 16 reviews. In addition to independent searches, this review provides information from a collection of 212 publications, including reviews and original research articles.

Discussion and conclusions: The review discusses the effects of alcohol consumption on brain endocannabinoid signaling, including alcohol-based perturbations in endocannabinoid-mediated synaptic transmission, the modulation of alcohol-related behaviors by manipulating signaling elements of the endocannabinoid system, and the influence of dysregulated endocannabinoid function in promoting withdrawal-induced anxiety-like behavior. Notable emphasis is placed on studies exploring the possible therapeutic relevance of bolstering brain endocannabinoid tone at different stages of alcohol use disorder.

目的:内源性大麻素系统参与中枢神经系统的多种生理功能,包括调节大脑奖赏回路和情绪稳态。大量证据表明,大脑内源性大麻素信号在药物诱导的奖赏状态的处理过程中起作用,其中反复暴露会导致活动的病理变化,从而导致酒精使用障碍的进展。这篇综述提供了近期研究的叙述性总结,探讨了酒精暴露与内源性大麻素信号变化之间的相互作用,这可能是酒精使用障碍发展的基础。检索方法:作者首先对综述文章进行初步检索,以协助识别相关文献。随后分别对原始文献和最新研究进行了搜索。搜索词“酒精/乙醇”和“内源性大麻素”,以及涵盖强化和成瘾行为的特定目标的术语。通过排除包含广泛关注精神疾病、多药物滥用、非大麻素信号脂质和其他标准的文章,进一步完善了内容。搜索结果:最初的搜索在PubMed上总共获得了49篇评论文章,在ScienceDirect上获得了13篇,在Wiley Online上获得了17篇,作者从总共16篇评论中获得了信息。除了独立检索之外,本综述还提供了来自212篇出版物的信息,包括综述和原始研究文章。讨论与结论:本文讨论了饮酒对脑内源性大麻素信号传导的影响,包括酒精对内源性大麻素介导的突触传递的干扰,通过操纵内源性大麻素系统的信号元件调节酒精相关行为,以及内源性大麻素功能失调对促进戒断诱导的焦虑样行为的影响。值得注意的是,重点放在研究探索在酒精使用障碍的不同阶段增强脑内源性大麻素张力的可能治疗相关性。
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引用次数: 4
NIAAA 50th Anniversary Festschrift: From the Editor. NIAAA 50周年庆典:来自编辑。
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2022-01-01 DOI: 10.35946/arcr.v42.1.14
George F Koob
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引用次数: 0
The Convergent Neuroscience of Affective Pain and Substance Use Disorder. 情感性疼痛和物质使用障碍的融合神经科学。
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2021-12-16 eCollection Date: 2021-01-01 DOI: 10.35946/arcr.v41.1.14
Amanda R Pahng, Scott Edwards

Opioids and alcohol are widely used to relieve pain, with their analgesic efficacy stemming from rapid actions on both spinal and supraspinal nociceptive centers. As an extension of these relationships, both substances can be misused in attempts to manage negative affective symptoms stemming from chronic pain. Moreover, excessive use of opioids or alcohol facilitates the development of substance use disorder (SUD) as well as hyperalgesia, or enhanced pain sensitivity. Shared neurobiological mechanisms that promote hyperalgesia development in the context of SUD represent viable candidates for therapeutic intervention, with the ideal strategy capable of reducing both excessive substance use as well as pain symptoms simultaneously. Neurocognitive symptoms associated with SUD, ranging from poor risk management to the affective dimension of pain, are likely mediated by altered activities of key anatomical elements that modulate executive and interoceptive functions, including contributions from key frontocortical regions. To aid future discoveries, novel and translationally valid animal models of chronic pain and SUD remain under intense development and continued refinement. With these tools, future research strategies targeting severe SUD should focus on the common neurobiology between negative reinforcement and affective elements of pain, possibly by reducing excessive stress hormone and neurotransmitter activity within shared circuitry.

阿片类药物和酒精被广泛用于缓解疼痛,其镇痛效果源于对脊柱和椎管上伤害感觉中枢的快速作用。作为这些关系的延伸,这两种物质都可能被滥用于试图控制由慢性疼痛引起的负面情感症状。此外,过量使用阿片类药物或酒精会促进物质使用障碍(SUD)以及痛觉过敏或疼痛敏感性增强的发展。在SUD的背景下,促进痛觉过敏发展的共同神经生物学机制代表了治疗干预的可行候选者,具有能够同时减少过度药物使用和疼痛症状的理想策略。与SUD相关的神经认知症状,从风险管理不善到疼痛的情感维度,可能是由调节执行和内感受功能的关键解剖元件的活动改变介导的,包括关键额皮质区域的作用。为了帮助未来的发现,新的和翻译有效的慢性疼痛和SUD动物模型仍在大力发展和不断完善。有了这些工具,未来针对严重SUD的研究策略应该集中在负强化和疼痛的情感因素之间的共同神经生物学上,可能通过减少共享电路中过多的应激激素和神经递质活性。
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引用次数: 5
Forebrain-Midbrain Circuits and Peptides Involved in Hyperalgesia After Chronic Alcohol Exposure. 慢性酒精暴露后前脑-中脑回路和多肽参与痛觉过敏。
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2021-10-14 eCollection Date: 2021-01-01 DOI: 10.35946/arcr.v41.1.13
Nicholas W Gilpin, Waylin Yu, Thomas L Kash

People living with pain report drinking alcohol to relieve pain. Acute alcohol use reduces pain, and chronic alcohol use facilitates the emergence or exaggeration of pain. Recently, funding agencies and neuroscientists involved in basic research have turned their attention to understanding the neurobiological mechanisms that underlie pain-alcohol interactions, with a focus on circuit and molecular mediators of alcohol-induced changes in pain-related behavior. This review briefly discusses some examples of work being done in this area, with a focus on reciprocal projections between the midbrain and extended amygdala, as well as some neurochemical mediators of pain-related phenotypes after alcohol exposure. Finally, as more work accumulates on this topic, the authors highlight the need for the neuroscience field to carefully consider sex and age in the design and analysis of pain-alcohol interaction experiments.

患有疼痛的人说他们通过饮酒来缓解疼痛。急性酒精使用可减轻疼痛,而慢性酒精使用可促进疼痛的出现或加重。最近,参与基础研究的资助机构和神经科学家已经将注意力转向理解疼痛-酒精相互作用的神经生物学机制,重点关注酒精引起的疼痛相关行为变化的电路和分子介质。本文简要讨论了在这一领域所做的一些工作,重点是中脑和扩展杏仁核之间的相互投射,以及酒精暴露后疼痛相关表型的一些神经化学介质。最后,随着对这一课题的研究越来越多,作者强调,神经科学领域在设计和分析疼痛-酒精相互作用实验时,需要仔细考虑性别和年龄。
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引用次数: 2
Hepatic Cannabinoid Signaling in the Regulation of Alcohol-Associated Liver Disease. 肝大麻素信号在酒精相关肝病中的调节作用。
IF 9.4 1区 医学 Q1 SUBSTANCE ABUSE Pub Date : 2021-09-23 eCollection Date: 2021-01-01 DOI: 10.35946/arcr.v41.1.12
Keungmo Yang, Sung Eun Choi, Won-Il Jeong

Purpose: The endocannabinoid system has emerged as a key regulatory signaling pathway in the pathophysiology of alcohol-associated liver disease (ALD). More than 30 years of research have established different roles of endocannabinoids and their receptors in various aspects of liver diseases, such as steatosis, inflammation, and fibrosis. However, pharmacological applications of the endocannabinoid system for the treatment of ALD have not been successful because of psychoactive side effects, despite some beneficial effects. Thus, a more delicate and detailed elucidation of the mechanism linking the endocannabinoid system and ALD may be of paramount significance in efforts to apply the system to the treatment of ALD.

Search methods: Three electronic databases (PubMed, MEDLINE, and Cochrane Library) were used for literature search from November 1988 to April 2021. Major keywords used for literature searches were "cannabinoid," "cannabinoid receptor," "ALD," "steatosis," and "fibrosis."

Search results: According to the inclusion and exclusion criteria, the authors selected 47 eligible full-text articles out of 2,691 searched initially. Studies in the past 3 decades revealed the opposite effects of cannabinoid receptors CB1R and CB2R on steatosis, inflammation, and fibrosis in ALD.

Discussion and conclusions: This review summarizes the endocannabinoid signaling in the general physiology of the liver, the pathogenesis of ALD, and some of the potential therapeutic implications of cannabinoid-based treatments for ALD.

目的:内源性大麻素系统已成为酒精相关性肝病(ALD)病理生理中的关键调控信号通路。30多年来的研究已经确定了内源性大麻素及其受体在肝脏疾病的各个方面的不同作用,如脂肪变性、炎症和纤维化。然而,尽管有一些有益的作用,内源性大麻素系统用于治疗ALD的药理学应用尚未成功,因为精神活性副作用。因此,更细致和详细地阐明内源性大麻素系统与ALD之间的联系机制,可能对将该系统应用于ALD的治疗具有至关重要的意义。检索方法:1988年11月至2021年4月,使用PubMed、MEDLINE和Cochrane Library三个电子数据库进行文献检索。用于文献检索的主要关键词是“大麻素”、“大麻素受体”、“ALD”、“脂肪变性”和“纤维化”。搜索结果:根据纳入和排除标准,作者从最初搜索的2691篇文章中选择了47篇符合条件的全文文章。过去30年的研究揭示了大麻素受体CB1R和CB2R对ALD中脂肪变性、炎症和纤维化的相反作用。讨论与结论:本文综述了内源性大麻素信号在肝脏一般生理中的作用,ALD的发病机制,以及以大麻素为基础的ALD治疗的一些潜在治疗意义。
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引用次数: 6
期刊
Alcohol Research : Current Reviews
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