Cellular architecture and transmitter phenotypes of neurons of the mouse median raphe region

Sos, Katalin E.; Mayer, Márton I.; Cserép, Csaba; Takács, Flóra; Szőnyi, András; Freund, Tamás F.; Nyíri, Gábor

doi:10.1007/s00429-016-1217-x

Cited by 53 publications

(67 citation statements)

References 66 publications

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“…Thus, DRL displays fairly specific connections, for example, with the IP and MnR, present findings (Lima et al, ), and has been selectively implicated in social stress (Crawford, Rahman, & Beck, ) and panic behavior (Johnson, Hollis, Moratalla, Lightman, & Lowry, ). Furthermore, our combined immunohistochemical/retrograde tracing findings suggest that all major neuronal populations present in the DR/MnR (Hioki et al, ; Sos et al, ) provide inputs to the LDTg, with a predominance of glutamatergic and GABAergic neurons, the later indicated indirectly by the elevated number of single labeled CTb neurons. An explicit role of the MnR in mechanisms of fear/anxiety has only been fully recognized during the last two decades.…”

Section: Discussionmentioning

confidence: 70%

“…For this purpose, injections of retrograde and anterograde tracers were made into the LDTg, LHb, IP, or MnR. Since LDTg (Wang & Morales, ), IP (Quina et al, ), and MnR (Sos et al, ) are now known to be neurochemically heterogeneous, we also characterized the transmitter phenotype of the projections between LDTg‐IP, and MnR‐LDTg. To this end, we combined retrograde tracing from IP or LDTg with immunofluorescence staining for choline acetyltransferase (ChAT), serotonin (5‐HT), and the Type 3 vesicular glutamate transporter (VGLUT3), and also with in situ hybridization for glutamate decarboxylase 67 kDA (GAD67), as well as the Type 2 vesicular glutamate transporter (VGLUT2).…”

Section: Introductionmentioning

confidence: 99%

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Connections of the laterodorsal tegmental nucleus with the habenular‐interpeduncular‐raphe system

Bueno

Lima

Souza

et al. 2019

J of Comparative Neurology

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The laterodorsal tegmental nucleus (LDTg) is a hindbrain cholinergic cell group thought to be involved in mechanisms of arousal and the control of midbrain dopamine cells. Nowadays, there is increasing evidence that LDTg is also engaged in mechanisms of anxiety/fear and promotion of emotional arousal under adverse conditions. Interestingly, LDTg appears to be connected with other regulators of aversive motivational states, including the lateral habenula (LHb), medial habenula (MHb), interpeduncular nucleus (IP), and median raphe nucleus (MnR). However, the circuitry between these structures has hitherto not been systematically investigated. Here, we placed injections of retrograde or anterograde tracers into LDTg, LHb, IP, and MnR.We also examined the transmitter phenotype of LDTg afferents to IP by combining retrograde tracing with immunofluorescence and in situ hybridization techniques.We found LHb inputs to LDTg mainly emerging from the medial division of the LHb (LHbM), which also receives axonal input from LDTg. The bidirectional connections between IP and LDTg displayed a lateralized organization, with LDTg inputs to IP being predominantly GABAergic or cholinergic and mainly directed to the contralateral IP. Moreover, we disclosed reciprocal LDTg connections with structures involved Abbreviations: 3V, third ventricle; 4V, fourth ventricle; 4n, trochlear nerve; A13, A13 dopamine cell group; ac, anterior commissure; AcbRP, nucleus accumbens, rostral pole; AD, anterodorsal thalamic nucleus; AID, agranular insular cortex, dorsal part; AIV, agranular insular cortex, ventral part; AM, anteromedial thalamic nucleus; BAC, bed nucleus of the anterior commissure; BST, bed nucleus of the stria terminalis; Cg1, cingulate cortex 1in the modulation of hippocampal theta rhythm including MnR, nucleus incertus, and supramammillary nucleus. Our findings indicate that the habenula is linked with LDTg either by direct reciprocal projections from/to LHbM or indirectly via the MHb-IP axis, supporting a functional role of LDTg in the regulation of aversive behaviors, and further characterizing LHb as a master controller of ascending brainstem state-setting modulatory projection systems.

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Section: Discussionmentioning

confidence: 70%

Section: Introductionmentioning

confidence: 99%

Connections of the laterodorsal tegmental nucleus with the habenular‐interpeduncular‐raphe system

Bueno

Lima

Souza

et al. 2019

J of Comparative Neurology

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“…Yet, it was not clear which neuronal pathway orchestrates the coordinated activation of these networks. Although the MRR was known to play a central role in processing negative experience (15,54), its known cell types did not project to the LHb, and the transmitter phenotypes and targets of almost 25% of the MRR neurons were not even known (22).…”

Section: Discussionmentioning

confidence: 99%

Median raphe controls acquisition of negative experience in the mouse

Szőnyi

Zichó

Barth

et al. 2019

Science

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Adverse events need to be quickly evaluated and memorized, yet how these processes are coordinated is poorly understood. We discovered a large population of excitatory neurons in mouse median raphe region (MRR) expressing vesicular glutamate transporter 2 (vGluT2) that received inputs from several negative experience–related brain centers, projected to the main aversion centers, and activated the septohippocampal system pivotal for learning of adverse events. These neurons were selectively activated by aversive but not rewarding stimuli. Their stimulation induced place aversion, aggression, depression-related anhedonia, and suppression of reward-seeking behavior and memory acquisition–promoting hippocampal theta oscillations. By contrast, their suppression impaired both contextual and cued fear memory formation. These results suggest that MRR vGluT2 neurons are crucial for the acquisition of negative experiences and may play a central role in depression-related mood disorders.

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“…The number of Pet-1+ cells without detectable 5-HT identity was reported to be about 27% in the MRN while in the B7 and B6 portions of the DRN this number was only 1% (Pelosi et al, 2014). These findings were interpreted as evidence that not all Pet-1+ cells are 5-HT neurons (Sos et al, 2016). However, recent single cell RNA seq studies have revealed that all of the single Pet-1+ cells sequenced in the DRN and MRN express Tph2 , although some had a much lower number of Tph2 reads that other Pet-1+ cells (Okaty et al, 2015).…”

Section: Maturation Of Pet-1+/5-ht Neuronsmentioning

confidence: 99%

Regulatory Mechanisms Controlling Maturation of Serotonin Neuron Identity and Function

Spencer

Deneris

2017

Front. Cell. Neurosci.

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The brain serotonin (5-hydroxytryptamine; 5-HT) system has been extensively studied for its role in normal physiology and behavior, as well as, neuropsychiatric disorders. The broad influence of 5-HT on brain function, is in part due to the vast connectivity pattern of 5-HT-producing neurons throughout the CNS. 5-HT neurons are born and terminally specified midway through embryogenesis, then enter a protracted period of maturation, where they functionally integrate into CNS circuitry and then are maintained throughout life. The transcriptional regulatory networks controlling progenitor cell generation and terminal specification of 5-HT neurons are relatively well-understood, yet the factors controlling 5-HT neuron maturation are only recently coming to light. In this review, we first provide an update on the regulatory network controlling 5-HT neuron development, then delve deeper into the properties and regulatory strategies governing 5-HT neuron maturation. In particular, we discuss the role of the 5-HT neuron terminal selector transcription factor (TF) Pet-1 as a key regulator of 5-HT neuron maturation. Pet-1 was originally shown to positively regulate genes needed for 5-HT synthesis, reuptake and vesicular transport, hence 5-HT neuron-type transmitter identity. It has now been shown to regulate, both positively and negatively, many other categories of genes in 5-HT neurons including ion channels, GPCRs, transporters, neuropeptides, and other transcription factors. Its function as a terminal selector results in the maturation of 5-HT neuron excitability, firing characteristics, and synaptic modulation by several neurotransmitters. Furthermore, there is a temporal requirement for Pet-1 in the control of postmitotic gene expression trajectories thus indicating a direct role in 5-HT neuron maturation. Proper regulation of the maturation of cellular identity is critical for normal neuronal functioning and perturbations in the gene regulatory networks controlling these processes may result in long-lasting changes in brain function in adulthood. Further study of 5-HT neuron gene regulatory networks is likely to provide additional insight into how neurons acquire their mature identities and how terminal selector-type TFs function in postmitotic vertebrate neurons.

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Cellular architecture and transmitter phenotypes of neurons of the mouse median raphe region

Cited by 53 publications

References 66 publications

Connections of the laterodorsal tegmental nucleus with the habenular‐interpeduncular‐raphe system

Connections of the laterodorsal tegmental nucleus with the habenular‐interpeduncular‐raphe system

Median raphe controls acquisition of negative experience in the mouse

Regulatory Mechanisms Controlling Maturation of Serotonin Neuron Identity and Function

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