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基于静息态 fMRI 的去氯氯氮平在恒河猴中的筛选可预测剂量依赖性的行为效应。

Resting-State fMRI-Based Screening of Deschloroclozapine in Rhesus Macaques Predicts Dosage-Dependent Behavioral Effects.

机构信息

Nash Family Department of Neuroscience and Friedman Brain Institute, Icahn School of Medicine at Mount Sinai, New York, New York 10029.

BioMedical Engineering and Imaging Institute, Icahn School of Medicine at Mount Sinai, New York, New York 10029.

出版信息

J Neurosci. 2022 Jul 20;42(29):5705-5716. doi: 10.1523/JNEUROSCI.0325-22.2022. Epub 2022 Jun 14.

Abstract

Chemogenetic techniques, such as designer receptors exclusively activated by designer drugs (DREADDs), enable transient, reversible, and minimally invasive manipulation of neural activity Their development in nonhuman primates is essential for uncovering neural circuits contributing to cognitive functions and their translation to humans. One key issue that has delayed the development of chemogenetic techniques in primates is the lack of an accessible drug-screening method. Here, we use resting-state fMRI, a noninvasive neuroimaging tool, to assess the impact of deschloroclozapine (DCZ) on brainwide resting-state functional connectivity in 7 rhesus macaques (6 males and 1 female) without DREADDs. We found that systemic administration of 0.1 mg/kg DCZ did not alter the resting-state functional connectivity. Conversely, 0.3 mg/kg of DCZ was associated with a prominent increase in functional connectivity that was mainly confined to the connections of frontal regions. Additional behavioral tests confirmed a negligible impact of 0.1 mg/kg DCZ on socio-emotional behaviors as well as on reaction time in a probabilistic learning task; 0.3 mg/kg DCZ did, however, slow responses in the probabilistic learning task, suggesting attentional or motivational deficits associated with hyperconnectivity in fronto-temporo-parietal networks. Our study highlights both the excellent selectivity of DCZ as a DREADD actuator, and the side effects of its excess dosage. The results demonstrate the translational value of resting-state fMRI as a drug-screening tool to accelerate the development of chemogenetics in primates. Chemogenetics, such as designer receptors exclusively activated by designer drugs (DREADDs), can afford control over neural activity with unprecedented spatiotemporal resolution. Accelerating the translation of chemogenetic neuromodulation from rodents to primates requires an approach to screen novel DREADD actuators Here, we assessed brainwide activity in response to a DREADD actuator deschloroclozapine (DCZ) using resting-state fMRI in macaque monkeys. We demonstrated that low-dose DCZ (0.1 mg/kg) did not change whole-brain functional connectivity or affective behaviors, while a higher dose (0.3 mg/kg) altered frontal functional connectivity and slowed response in a learning task. Our study highlights the excellent selectivity of DCZ at proper dosing, and demonstrates the utility of resting-state fMRI to screen novel chemogenetic actuators in primates.

摘要

化学遗传学技术,如仅被设计药物激活的设计受体(DREADD),能够实现神经活动的短暂、可逆和微创操纵。它们在非人类灵长类动物中的发展对于揭示认知功能相关的神经回路以及将其转化到人类中至关重要。一个阻碍化学遗传学技术在灵长类动物中发展的关键问题是缺乏可访问的药物筛选方法。在这里,我们使用静息态 fMRI,一种非侵入性的神经影像学工具,在没有 DREADD 的情况下评估氯氮平(DCZ)对 7 只恒河猴(6 只雄性和 1 只雌性)全脑静息态功能连接的影响。我们发现,系统给予 0.1mg/kg 的 DCZ 不会改变静息态功能连接。相反,0.3mg/kg 的 DCZ 与功能连接的显著增加有关,主要局限于额区的连接。额外的行为测试证实,0.1mg/kg 的 DCZ 对社会情感行为以及概率学习任务中的反应时间几乎没有影响;然而,0.3mg/kg 的 DCZ 确实会减缓概率学习任务中的反应,这表明与额颞顶叶网络的过度连接相关的注意力或动机缺陷。我们的研究强调了 DCZ 作为 DREADD 激活剂的优异选择性,以及其过量剂量的副作用。结果表明,静息态 fMRI 作为一种药物筛选工具具有转化价值,可加速灵长类动物中化学遗传学的发展。化学遗传学,如仅被设计药物激活的设计受体(DREADD),可以以前所未有的时空分辨率控制神经活动。将化学遗传神经调节从啮齿动物加速转化为灵长类动物需要一种筛选新型 DREADD 激活剂的方法。在这里,我们使用恒河猴的静息态 fMRI 评估了对 DREADD 激活剂氯氮平(DCZ)的全脑活动反应。我们证明,低剂量的 DCZ(0.1mg/kg)不会改变全脑功能连接或情感行为,而高剂量(0.3mg/kg)则改变了额部功能连接并减缓了学习任务的反应。我们的研究强调了 DCZ 在适当剂量下的优异选择性,并证明了静息态 fMRI 在筛选灵长类动物新型化学遗传激活剂方面的实用性。

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