Stimulation of L-type calcium channels increases tyrosine hydroxylase and dopamine in ventral midbrain cells induced from somatic cells

Author:

Jefri Malvin12,Bell Scott12,Peng Huashan12,Hettige Nuwan12,Maussion Gilles3,Soubannier Vincent3,Wu Hanrong12,Silveira Heika12,Theroux Jean-Francois12,Moquin Luc2,Zhang Xin12,Aouabed Zahia12,Krishnan Jeyashree4,O’Leary Liam A.2,Antonyan Lilit,Zhang Ying12,McCarty Vincent12,Mechawar Naguib2,Gratton Alain2,Schuppert Andreas4,Durcan Thomas M.3,Fon Edward A.3,Ernst Carl12

Affiliation:

1. Psychiatric Genetics Group McGill University, Montreal, Quebec, Canada

2. Department of Psychiatry McGill University and Douglas Hospital Research Institute, Montreal, Quebec, Canada

3. Department of Neurology and Neurosurgery Montreal Neurological Institute, Montreal, Quebec, Canada

4. Institute for Computational Biomedicine, Aachen University, Aachen, Germany

Abstract

Abstract Making high-quality dopamine (DA)-producing cells for basic biological or small molecule screening studies is critical for the development of novel therapeutics for disorders of the ventral midbrain. Currently, many ventral midbrain assays have low signal-to-noise ratio due to low levels of cellular DA and the rate-limiting enzyme of DA synthesis, tyrosine hydroxylase (TH), hampering discovery efforts. Using intensively characterized ventral midbrain cells derived from human skin, which demonstrate calcium pacemaking activity and classical electrophysiological properties, we show that an L-type calcium agonist can significantly increase TH protein levels and DA content and release. Live calcium imaging suggests that it is the immediate influx of calcium occurring simultaneously in all cells that drives this effect. Genome-wide expression profiling suggests that L-type calcium channel stimulation has a significant effect on specific genes related to DA synthesis and affects expression of L-type calcium receptor subunits from the CACNA1 and CACNA2D families. Together, our findings provide an advance in the ability to increase DA and TH levels to improve the accuracy of disease modeling and small molecule screening for disorders of the ventral midbrain, including Parkinson’s disease. Significance statement A single molecule provides a major boost to both tyrosine hydroxylase and dopamine in stem cell-derived human ventral midbrain cells.

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Developmental Biology,General Medicine

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