Impact of Serine Racemase Deletion on Nicotine Discrimination.

IF 3 2区 医学 Q2 PUBLIC, ENVIRONMENTAL & OCCUPATIONAL HEALTH Nicotine & Tobacco Research Pub Date : 2024-11-22 DOI:10.1093/ntr/ntae156
Isabel L Yu, Joseph T Coyle, Rajeev I Desai
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Abstract

Introduction: The high comorbidity between schizophrenia and cigarette smoking points to a possible shared heritable factor predisposing individuals with schizophrenia to nicotine addiction. The N-methyl-d-aspartate (NMDA) receptor has been highly implicated in both schizophrenia and nicotine addiction.

Methods: In the present study, we used mice with a null mutation on the serine racemase gene (srr), an established risk gene for schizophrenia, which encodes the enzyme to produce the NMDA receptor co-agonist d-serine, to model the pathology of schizophrenia and to determine whether NMDA receptor hypofunction reduced the ability of srr-/- mice to identify nicotine's subjective effects. Established nicotine discrimination procedures were used to train srr-/- and wild-type (WT) mice to discriminate 0.4 mg/kg nicotine under a 10-response fixed-ratio (FR10) schedule of food reinforcement.

Results: Results show that WT mice reliably acquired 0.4 mg/kg nicotine discrimination in about 54 training sessions, whereas srr-/- mice failed to acquire robust 0.4 mg/kg nicotine discrimination even after extended (>70) training sessions. These results show that NDMA receptor hypofunction in srr-/- mice decreased sensitivity to the interoceptive effects of nicotine.

Conclusions: Projected to humans, NMDA receptor hypofunction caused by mutations to the serine racemase gene in schizophrenia may reduce sensitivity to nicotine's subjective effects leading to increased nicotine consumption to produce the same effects as those unaffected by schizophrenia.

Implications: There is high comorbidity between schizophrenia and nicotine dependence as well as possible shared genetic risk factors between the two. The serine racemase knockout mouse (srr-/-) with NMDA receptor hypofunction has been developed as a model for schizophrenia. We found that srr-/- mice were unable to acquire 0.4 mg/kg nicotine discrimination, while WT mice readily discriminated nicotine. These results show that decreased NMDA receptor function present in srr-/- mice and patients with schizophrenia may result in reduced sensitivity to nicotine's interoceptive effects, leading to increased nicotine consumption to produce the same subjective effects as those unaffected by schizophrenia.

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丝氨酸消旋酶缺失对尼古丁辨别能力的影响
导言:精神分裂症与吸烟之间的高度共病性表明,精神分裂症患者可能存在尼古丁成瘾的共同遗传因素。N-甲基-D-天冬氨酸(NMDA)受体与精神分裂症和尼古丁成瘾都有很大关系:在本研究中,我们使用丝氨酸消旋酶基因(srr)发生无效突变的小鼠来模拟精神分裂症的病理变化,该基因是精神分裂症的一个既定风险基因,它编码产生NMDA受体协同物D-丝氨酸的酶,并确定NMDA受体功能低下是否会降低srr-/-小鼠识别尼古丁主观效应的能力。在食物强化的10次反应固定比率(FR10)计划下,使用既定的尼古丁辨别程序训练srr-/-和野生型(WT)小鼠辨别0.4毫克/千克尼古丁:结果表明,WT小鼠在大约54次训练中可靠地获得了0.4毫克/千克尼古丁的辨别能力,而srr-/-小鼠即使在延长(>70次)训练后也未能获得稳健的0.4毫克/千克尼古丁辨别能力。这些结果表明,srr-/-小鼠的NDMA受体功能减退降低了对尼古丁间感觉效应的敏感性:推测到人类身上,精神分裂症患者丝氨酸消旋酶基因突变导致的 NMDA 受体功能低下可能会降低对尼古丁主观效应的敏感性,从而导致尼古丁消耗量增加,以产生与未受精神分裂症影响的人相同的效果:意义:精神分裂症与尼古丁依赖之间存在高度的共病性,而且两者之间可能存在共同的遗传风险因素。具有 NMDA 受体功能低下的丝氨酸消旋酶基因敲除小鼠(srr-/-)已被开发为精神分裂症的模型。我们发现,srr-/-小鼠无法辨别0.4毫克/千克的尼古丁,而野生型小鼠则很容易辨别尼古丁。这些结果表明,srr-/-小鼠和精神分裂症患者的NMDA受体功能下降,可能会导致对尼古丁的感受效应敏感性降低,从而增加尼古丁的消耗量,以产生与未受精神分裂症影响的患者相同的主观效应。
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来源期刊
Nicotine & Tobacco Research
Nicotine & Tobacco Research 医学-公共卫生、环境卫生与职业卫生
CiteScore
8.10
自引率
10.60%
发文量
268
审稿时长
3-8 weeks
期刊介绍: Nicotine & Tobacco Research is one of the world''s few peer-reviewed journals devoted exclusively to the study of nicotine and tobacco. It aims to provide a forum for empirical findings, critical reviews, and conceptual papers on the many aspects of nicotine and tobacco, including research from the biobehavioral, neurobiological, molecular biologic, epidemiological, prevention, and treatment arenas. Along with manuscripts from each of the areas mentioned above, the editors encourage submissions that are integrative in nature and that cross traditional disciplinary boundaries. The journal is sponsored by the Society for Research on Nicotine and Tobacco (SRNT). It publishes twelve times a year.
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