A novel floor plate boundary defined by adjacent<i>En1</i>and<i>Dbx1</i>microdomains distinguishes midbrain dopamine and hypothalamic neurons

Nouri, Navid; Awatramani, Rajeshwar

doi:10.1242/dev.144949

Cited by 27 publications

(32 citation statements)

References 101 publications

(146 reference statements)

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“…Furthermore, single cell RNA sequencing of Lmx1a+ precursors in the mouse suggests that the midbrain floor-plate markers FOXA2 and LMX1A are not specific to just mDA progenitors, but also mark the more anterior, subthalamic nucleus (STN) precursors which go on to give rise to glutamatergic neurons ( Kee et al, 2017 ). Those results are in agreement with the idea that the midbrain-diencephalic floor-plate region is subdivided into two distinct domains by En1 for posterior, midbrain (mDA) identity, and Dbx1 for STN neuron population ( Nouri and Awatramani, 2017 ). Importantly, lowering CHIR exposure (0.4–0.6 μM) resulted in a bias toward Lmx1a+/Pitx2+ positive cells (STN neuron) while the percentage of STN neurons was greatly decreased at higher concentrations of CHIR (0.8–1 μM) with increased efficiencies of mDA neuron differentiation ( Kee et al, 2017 ).…”

Section: What Cell Type-related Factors Are Critical For Clinical Trasupporting

confidence: 91%

Pluripotent Stem Cell Therapies for Parkinson Disease: Present Challenges and Future Opportunities

Kim

Koo

Studer

2020

Front. Cell Dev. Biol.

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In Parkinson's disease (PD), there are currently no effective therapies to prevent or slow down disease progression. Cell replacement therapy using human pluripotent stem cell (hPSC)-derived dopamine neurons holds considerable promise. It presents a novel, regenerative strategy, building on the extensive history of fetal tissue grafts and capturing the potential of hPSCs to serve as a scalable and standardized cell source. Progress in establishing protocols for the direct differentiation to midbrain dopamine (mDA) neurons from hPSC have catalyzed the development of cell-based therapies for PD. Consequently, several groups have derived clinical-grade mDA neuron precursors under clinical good manufacture practice condition, which are progressing toward clinical testing in PD patients. Here we will review the current status of the field, discuss the remaining key challenges, and highlight future areas for further improvements of hPSC-based technologies in the clinical translation to PD.

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Section: What Cell Type-related Factors Are Critical For Clinical Trasupporting

confidence: 91%

Pluripotent Stem Cell Therapies for Parkinson Disease: Present Challenges and Future Opportunities

Kim

Koo

Studer

2020

Front. Cell Dev. Biol.

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“…The Dat locus has the advantage of being largely restricted to midbrain DA neurons 16 , barring few other neuronal populations (e.g. ventral premmamillary nucleus, PMv 20 ). Together these complementary approaches form a powerful arsenal to target molecularly distinct DA neurons.…”

Section: Resultsmentioning

confidence: 99%

“…Adults mice (more than 8 weeks of age) were perfused with cold 4% PFA in PBS, the brains were dissected and fixed overnight in the same solution, cryoprotected in 30% sucrose PBS solution, sectioned at 25μm using a freezing microtome, and stored in −20°C in cryoprotectant solution. For immunofluorescence on free-floating sections, we initially rinsed in PBS, blocked in 5% donkey serum, 0.3% Triton X-100 in PBS, and incubated overnight at 4°C with primary antibodies diluted in blocking solution: rabbit anti-ALDH1A1 (Cat# ab23375; Abcam; 1:200) 8 , goat anti-βgal (Cat# 4600–1409; Biogenesis; 1:1500) 20 , rabbit anti-βgal (Cat# 55976; Cappel; 1:1500) 63 , goat anti-FOXA2 (Cat# sc-6554; Santa Cruz; 1:50) 64 , chicken anti-GFP (Cat# ab13970; abcam; 1:1,500) 20 , rabbit anti-NURR1 (Cat# sc-990; Santa Cruz; 1:500) 8 , goat anti-OTX2 (Cat# GT15095; Neuromics; 1:200) 8 , rabbit anti-SOX6 (Cat# ab30455; Abcam; 1:500) 8 , rabbit anti-TH (Cat# P40101; Pel-Freez; 1:500) 20 , sheep anti-TH (Cat# P60101–0; Pel-Freez; 1:500) 8 , and rabbit anti-VIP (Cat# ab43841; Abcam; 1:500) 8 . Sections were rinsed in PBS+0.05% Tween20 solution and incubated with secondary antibodies generated in donkey and conjugated with appropriate fluorophores (Alexa488, Alexa555, Alexa647; Molecular Probes) diluted 1:250 in blocking solution and counterstained with DAPI (Sigma), rinsed in PBS+0.05% Tween20, and finally coverslipped with Gelvatol.…”

Section: Methodsmentioning

confidence: 99%

Mapping projections of molecularly defined dopamine neuron subtypes using intersectional genetic approaches

et al. 2018

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Midbrain dopamine (DA) neurons have diverse functions that can in part be explained by their heterogeneity. Although molecularly distinct subtypes of DA neurons have been identified by single-cell gene expression profiling, fundamental features such as their projection patterns have not been elucidated. Progress in this regard has been hindered by the lack of genetic tools for studying DA neuron subtypes. Here we develop intersectional genetic labeling strategies, based on combinatorial gene expression, to map the projections of molecularly defined DA neuron subtypes. We reveal distinct genetically defined dopaminergic pathways arising from the substantia nigra pars compacta and from the ventral tegmental area that innervate specific regions of the caudate putamen, nucleus accumbens and amygdala. Together, the genetic toolbox and DA neuron subtype projections presented here constitute a resource that will accelerate the investigation of this clinically significant neurotransmitter system.

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“…The principles discussed here apply to all genetically targeted recombinase systems, including lox variants, Flp-frt, and Drerox systems. For example, the En1-Dre KI mouse line shows variable paternal germline recombination (Nouri and Awatramani, 2017). Moreover, the problem of unwanted recombination may be compounded by intersectional strategies involving multiple recombinases.…”

Section: Broader Implications-other Recombinase Systems and Organismsmentioning

confidence: 99%

Optimizing Nervous System-Specific Gene Targeting with Cre Driver Lines: Prevalence of Germline Recombination and Influencing Factors

Luo¹,

Ambrozkiewicz²,

Benseler³

et al. 2020

Neuron

142

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A novel floor plate boundary defined by adjacentEn1andDbx1microdomains distinguishes midbrain dopamine and hypothalamic neurons

Cited by 27 publications

References 101 publications

Pluripotent Stem Cell Therapies for Parkinson Disease: Present Challenges and Future Opportunities

Pluripotent Stem Cell Therapies for Parkinson Disease: Present Challenges and Future Opportunities

Mapping projections of molecularly defined dopamine neuron subtypes using intersectional genetic approaches

Optimizing Nervous System-Specific Gene Targeting with Cre Driver Lines: Prevalence of Germline Recombination and Influencing Factors

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