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环境光通过激活小鼠中表达Brn3b的内在光敏视网膜神经节细胞来控制呼吸的日常节律。

Environmental Light Controls the Daily Organization of Breathing by Activating Brn3b-expressing Intrinsically Photosensitive Retinal Ganglion Cells in Mice.

作者信息

Jones Aaron A, Spears Allison R, Arble Deanna M

机构信息

Department of Biological Sciences, Klinger College of Arts and Sciences, Marquette University, Milwaukee, Wisconsin.

Breathing Research and Therapeutics Center, Department of Physical Therapy, McKnight Brain Institute, University of Florida, Gainesville, Florida.

出版信息

J Biol Rhythms. 2024 Dec;39(6):568-580. doi: 10.1177/07487304241276888. Epub 2024 Sep 12.

Abstract

Rhythmic, daily fluctuations in minute ventilation are controlled by the endogenous circadian clock located in the suprachiasmatic nucleus (SCN). While light serves as a potent synchronizer for the SCN, it also influences physiology and behavior by activating Brn3b-expressing, intrinsically photosensitive retinal ganglion cells (ipRGCs). It is currently unclear the extent to which the external light environment shapes daily ventilatory patterns independent of the SCN. To determine the relative influence of environmental light versus circadian timing on the organization of daily rhythms in minute ventilation, we used whole-body plethysmography to measure the breathing of mice housed on a non-entraining T28 cycle (14 h light:14 h dark). Using this protocol, we found that minute ventilation exhibits a ~28-h rhythm with a peak at dark onset that coincides with the light:dark cycle and the animals' locomotor activity. To determine if this 28-h rhythm in minute ventilation was mediated by Brn3b-expressing ipRGCs, we measured the breathing of Brn3bDTA mice housed under the T28 cycle. Brn3bDTA mice lack the Brn3b-expressing ipRGCs that project to many non-SCN brain regions. We found that despite rhythmic light cues occurring on a 28-h basis, Brn3bDTA mice exhibited 24-h rhythms in minute ventilation, locomotor activity, and core body temperature consistent with organization by the SCN. The 24-h minute ventilation rhythm of Brn3bDTA mice was found to be driven predominantly by tidal volume rather than respiratory rate. These data indicate that the external light:dark cycle can directly drive daily patterns in minute ventilation by way of Brn3b-expressing ipRGCs. In addition, these data strongly suggest that the activation of Brn3b-expressing ipRGCs principally organizes daily patterns in breathing and locomotor activity when light:dark cues are presented in opposition to endogenous clock timing.

摘要

分钟通气量的节律性每日波动受位于视交叉上核(SCN)的内源性昼夜节律时钟控制。虽然光作为SCN的有效同步器,但它也通过激活表达Brn3b的内在光敏视网膜神经节细胞(ipRGCs)来影响生理和行为。目前尚不清楚外部光环境在多大程度上独立于SCN塑造每日通气模式。为了确定环境光与昼夜节律定时对分钟通气量每日节律组织的相对影响,我们使用全身体积描记法测量饲养在非同步T28周期(14小时光照:14小时黑暗)的小鼠的呼吸。使用该方案,我们发现分钟通气量表现出约28小时的节律,在黑暗开始时达到峰值,这与明暗周期和动物的运动活动一致。为了确定分钟通气量的这种28小时节律是否由表达Brn3b的ipRGCs介导,我们测量了饲养在T28周期下的Brn3bDTA小鼠的呼吸。Brn3bDTA小鼠缺乏投射到许多非SCN脑区的表达Brn3b的ipRGCs。我们发现,尽管有节奏的光信号以28小时为基础出现,但Brn3bDTA小鼠在分钟通气量、运动活动和核心体温方面表现出24小时的节律,与SCN的组织一致。发现Brn3bDTA小鼠的24小时分钟通气量节律主要由潮气量而非呼吸频率驱动。这些数据表明,外部明暗周期可以通过表达Brn3b的ipRGCs直接驱动分钟通气量的每日模式。此外,这些数据强烈表明,当明暗信号与内源性时钟定时相反时,表达Brn3b的ipRGCs的激活主要组织呼吸和运动活动的每日模式。

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