Midbrain Gene Screening Identifies a New Mesoaccumbal Glutamatergic Pathway and a Marker for Dopamine Cells Neuroprotected in Parkinson’s Disease

Viereckel, Thomas; Dumas, Sylvie; Smith-Anttila, Casey J. A.; Vlcek, Bianca; Bimpisidis, Zisis; Lagerström, Malin C.; Konradsson-Geuken, Åsa; Wallén-Mackenzie, Åsa

doi:10.1038/srep35203

Cited by 50 publications

(75 citation statements)

References 71 publications

(116 reference statements)

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“…Nurr1 null mice die within 24h after birth and conditional knockout of Nr4a2 in DA neurons in adult animals caused decreased expression of DA markers, including Th and Slc6a3 (DAT), followed by progressive loss of DA (Castillo et al 1998;Kadkhodaei et al 2009Kadkhodaei et al , 2013 (Chang et al 2019;Lindefors and Ungerstedt 1990;Rodríguez-Puertas et al 1999). There are additional levels of crosstalk between glutamate and dopamine-glutamate neurons and their local synapses within the midbrain DA regions (Dobi et al 2010;Morales and Root 2014;Viereckel et al 2016;Wang and Morales 2009;Yamaguchi et al 2015). In our study we detect increased levels of metabotropic glutamate receptor 1 and ionotropic glutamate receptor NMDA 3A.…”

Section: Vta and Snc Transcriptomes Respond Distinctly To Da Deficiencysupporting

confidence: 50%

Transcriptome responses to reduced dopamine in the Substantia Nigra Pars Compacta reveals a potential protective role for dopamine

Koltun

Cichewicz

Gibbs

et al. 2018

Preprint

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Parkinson's Disease (PD), is a neurodegenerative disorder affecting both cognitive and motor functions. It is characterized by decreased brain dopamine (DA) and a selective and progressive loss of dopaminergic neurons in the substantia nigra pars compacta (SNc), whereas dopaminergic neurons in the ventral tegmental area (VTA) show reduced vulnerability. The majority of animal models of PD are genetic lesion or neurotoxin exposure models that lead to death of dopaminergic neurons. Here we use a DAT:TH KO mouse model that by inactivation of the tyrosine hydroxylase (Th) gene in dopamine transporter-expressing neurons, causes selective depletion of striatal dopamine without affecting DA neuron survival. We analyzed transcriptome responses to decreased DA in both pre-and post-synaptic dopaminergic brain regions of DAT:TH KO animals. We detected only few differentially expressed genes in the post-synaptic regions as a function of DA deficiency. This suggests that the broad striatal transcriptional changes in neurodegeneration-based PD models are not direct effects of DA depletion, but are rather a result of DA neuronal death. However, we find a number of dopaminergic genes differentially expressed in SNc, and to a lesser extent in VTA, as a function of DA deficiency, providing evidence for a DA-dependent feedback loop. Of particular interest, expression of Nr4a2, a crucial transcription factor maintaining DA neuron identity, is significantly decreased in SNc, but not VTA, of DAT:TH KO mice, implying a potential protective role for DA in the SNc.

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Section: Vta and Snc Transcriptomes Respond Distinctly To Da Deficiencysupporting

confidence: 50%

Transcriptome responses to reduced dopamine in the Substantia Nigra Pars Compacta reveals a potential protective role for dopamine

Koltun

Cichewicz

Gibbs

et al. 2018

Preprint

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“…47,50 In addition, we identified four P7 MB DA subset clusters ( Figure 2D). Marker gene analysis confirmed that three of the clusters correspond to DA neurons from the VTA (Otx2 and Neurod6; P7.MB.1), 51,52 the periaqueductal gray area (PAG; Vip and Pnoc; P7.MB.3), 53,54 and the SN (Sox6, Aldh1a7, Ndnf, Serpine2, Rbp4, and Fgf20; P7.MB.4) 38,51,55,56 (Tables 1, S2, and S3). These data are consistent with recent scRNA-seq studies of similar populations.…”

Section: Scrna-seq Reveals Biologically and Temporally Discriminatingmentioning

confidence: 82%

Single-Cell RNA-Seq of Mouse Dopaminergic Neurons Informs Candidate Gene Selection for Sporadic Parkinson Disease

Hook

McClymont

Cannon

et al. 2018

The American Journal of Human Genetics

110

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Genetic variation modulating risk of sporadic Parkinson disease (PD) has been primarily explored through genome-wide association studies (GWASs). However, like many other common genetic diseases, the impacted genes remain largely unknown. Here, we used single-cell RNA-seq to characterize dopaminergic (DA) neuron populations in the mouse brain at embryonic and early postnatal time points. These data facilitated unbiased identification of DA neuron subpopulations through their unique transcriptional profiles, including a postnatal neuroblast population and substantia nigra (SN) DA neurons. We use these population-specific data to develop a scoring system to prioritize candidate genes in all 49 GWAS intervals implicated in PD risk, including genes with known PD associations and many with extensive supporting literature. As proof of principle, we confirm that the nigrostriatal pathway is compromised in Cplx1-null mice. Ultimately, this systematic approach establishes biologically pertinent candidates and testable hypotheses for sporadic PD, informing a new era of PD genetic research.

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“…) and we have recently reported the possibility to record glutamate release in the nucleus accumbens following optogenetic stimulation (Viereckel et al . ; Wang et al . ).…”

Section: Discussionmentioning

confidence: 99%

Validated multi‐step approach for in vivo recording and analysis of optogenetically evoked glutamate in the mouse globus pallidus

Viereckel

Konradsson-Geuken

Wallén-Mackenzie

2018

Journal of Neurochemistry

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Precise quantification of extracellular glutamate concentrations upon neuronal activation is crucial for the understanding of brain function and neurological disorders. While optogenetics is an outstanding method for the correlation between distinct neurons and their role in circuitry and behavior, the electrochemically inactive nature of glutamate has proven challenging for recording upon optogenetic stimulations. This difficulty is due to the necessity for using enzyme-coated microelectrodes and the risk for light-induced artifacts. In this study, we establish a method for the combination of in vivo optogenetic stimulation with selective measurement of glutamate concentrations using enzyme-coated multielectrode arrays and amperometry. The glutamatergic subthalamic nucleus (STN), which is the main electrode target site in deep brain stimulation treatment of advanced Parkinson's disease, has recently proven opotogenetically targetable in Pitx2-Cre-transgenic mice and was here used as model system. Upon stereotactic injection of viral Channelrhodopsin2-eYFP constructs into the STN, amperometric recordings were performed at a range of optogenetic stimulation frequencies in the globus pallidus, the main STN target area, in anesthetized mice. Accurate quantification was enabled through a multi-step analysis approach based on self-referencing microelectrodes and repetition of the experimental protocol at two holding potentials, which allowed for the identification, isolation and removal of photoelectric and photoelectrochemical artifacts. This study advances the field of in vivo glutamate detection with combined optogenetics and amperometric recordings by providing a validated analysis framework for application in a wide variety of glutamate-based approaches in neuroscience.

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Midbrain Gene Screening Identifies a New Mesoaccumbal Glutamatergic Pathway and a Marker for Dopamine Cells Neuroprotected in Parkinson’s Disease

Cited by 50 publications

References 71 publications

Transcriptome responses to reduced dopamine in the Substantia Nigra Pars Compacta reveals a potential protective role for dopamine

Transcriptome responses to reduced dopamine in the Substantia Nigra Pars Compacta reveals a potential protective role for dopamine

Single-Cell RNA-Seq of Mouse Dopaminergic Neurons Informs Candidate Gene Selection for Sporadic Parkinson Disease

Validated multi‐step approach for in vivo recording and analysis of optogenetically evoked glutamate in the mouse globus pallidus

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