Aberrant Tonic Inhibition of Dopaminergic Neuronal Activity Causes Motor Symptoms in Animal Models of Parkinson's Disease

Jun Young Heo; Min Ho Nam; Hyung Ho Yoon; Jeongyeon Kim; Yu Jin Hwang; Woojin Won; Dong Ho Woo; Ji Ae Lee; Hyun Jung Park; Seonmi Jo; Min Joung Lee; Sunpil Kim; Jeong Eun Shim; Dong Pyo Jang; Kyoung I. Kim; Sue H. Huh; Jae Y. Jeong; Neil W. Kowall; Junghee Lee; Hyeonjoo Im; Jong Hyun Park; Bo Ko Jang; Ki Duk Park; Hyunjoo J. Lee; Hyogeun Shin; Il Joo Cho; Eun Mi Hwang; Young Soo Kim; Hye Yun Kim; Soo Jin Oh; Seung Eun Lee; Sun Ha Paek; Jong Hyuk Yoon; Byung K. Jin; Gi Ryang Kweon; Insop Shim; Onyou Hwang; Hoon Ryu; Sang Ryong Jeon; C. Justin Lee

doi:10.1016/j.cub.2019.11.079

Aberrant Tonic Inhibition of Dopaminergic Neuronal Activity Causes Motor Symptoms in Animal Models of Parkinson's Disease

Jun Young Heo, Min Ho Nam, Hyung Ho Yoon, Jeongyeon Kim, Yu Jin Hwang, Woojin Won, Dong Ho Woo, Ji Ae Lee, Hyun Jung Park, Seonmi Jo, Min Joung Lee, Sunpil Kim, Jeong Eun Shim, Dong Pyo Jang, Kyoung I. Kim, Sue H. Huh, Jae Y. Jeong, Neil W. Kowall, Junghee Lee, Hyeonjoo ImJong Hyun Park, Bo Ko Jang, Ki Duk Park, Hyunjoo J. Lee, Hyogeun Shin, Il Joo Cho, Eun Mi Hwang, Young Soo Kim, Hye Yun Kim, Soo Jin Oh, Seung Eun Lee, Sun Ha Paek, Jong Hyuk Yoon, Byung K. Jin, Gi Ryang Kweon, Insop Shim, Onyou Hwang, Hoon Ryu, Sang Ryong Jeon, C. Justin Lee

Department of Pharmacy

Research output: Contribution to journal › Article › peer-review

41 Citations (Scopus)

Abstract

Current pharmacological treatments for Parkinson's disease (PD) are focused on symptomatic relief, but not on disease modification, based on the strong belief that PD is caused by irreversible dopaminergic neuronal death. Thus, the concept of the presence of dormant dopaminergic neurons and its possibility as the disease-modifying therapeutic target against PD have not been explored. Here we show that optogenetic activation of substantia nigra pars compacta (SNpc) neurons alleviates parkinsonism in acute PD animal models by recovering tyrosine hydroxylase (TH) from the TH-negative dormant dopaminergic neurons, some of which still express DOPA decarboxylase (DDC). The TH loss depends on reduced dopaminergic neuronal firing under aberrant tonic inhibition, which is attributed to excessive astrocytic GABA. Blocking the astrocytic GABA synthesis recapitulates the therapeutic effect of optogenetic activation. Consistently, SNpc of postmortem PD patients shows a significant population of TH-negative/DDC-positive dormant neurons surrounded by numerous GABA-positive astrocytes. We propose that disinhibiting dormant dopaminergic neurons by blocking excessive astrocytic GABA could be an effective therapeutic strategy against PD. Heo et al. report that astrocytic GABA-mediated aberrant tonic inhibition of DA neurons leads to a reduction in TH expression and dopamine production, causing dormant DA neurons and motor deficits. Blocking astrocytic GABA synthesis by MAO-B inhibition or optogenetic activation of dormant DA neurons reverses PD pathology.

Original language	English
Pages (from-to)	276-291.e9
Journal	Current Biology
Volume	30
Issue number	2
DOIs	https://doi.org/10.1016/j.cub.2019.11.079
Publication status	Published - 2020 Jan 20

Bibliographical note

Funding Information:
The AAV-A53T viral vector was kindly provided by Dr. Jun-ichi Miyazaki at Kumamoto University. This work was supported by the Creative Research Initiative Program ( 2015R1A3A2066619 ) of the National Research Foundation (NRF) of Korea funded by the Ministry of Science and ICT of Korea and Institute for Basic Science (IBS), Center for Cognition and Sociality ( IBS-R001-D2 ) to C.J.L.; Asan Life Science Institute grants ( 18-241 and 19-241 ) funded by the Asan Medical Center to S.R.J.; Brain Science Program ( 2018M3C7A1056894 ) funded by NRF of Korea to H.R.; KIST institutional program (Project No. 2E29221 ) and Brain Science Program ( 2018M3C7A1056897 ) funded by the NRF of Korea to M.H.N.; MRC program ( 2017R1A5A2015385 ) funded by the Ministry of Science and ICT of Korea to J.Y.H.; and KBRI basic research program (20-BR-02-05) through Korea Brain Research Institute funded by the Ministry of Science and ICT of Korea to J.K.

Funding Information:
The AAV-A53T viral vector was kindly provided by Dr. Jun-ichi Miyazaki at Kumamoto University. This work was supported by the Creative Research Initiative Program (2015R1A3A2066619) of the National Research Foundation (NRF) of Korea funded by the Ministry of Science and ICT of Korea and Institute for Basic Science (IBS), Center for Cognition and Sociality (IBS-R001-D2) to C.J.L.; Asan Life Science Institute grants (18-241 and 19-241) funded by the Asan Medical Center to S.R.J.; Brain Science Program (2018M3C7A1056894) funded by NRF of Korea to H.R.; KIST institutional program (Project No. 2E29221) and Brain Science Program (2018M3C7A1056897) funded by the NRF of Korea to M.H.N.; MRC program (2017R1A5A2015385) funded by the Ministry of Science and ICT of Korea to J.Y.H.; and KBRI basic research program (20-BR-02-05) through Korea Brain Research Institute funded by the Ministry of Science and ICT of Korea to J.K. Conceptualization, J.Y.H. M.-H.N. H.R. S.R.J. and C.J.L.; Methodology, S.H.H. S.J. J.Y.J. K.I.K. D.-P.J. and S.H.P.; Investigation, J.Y.H. M.-H.N. H.H.Y. J.K. Y.J.H. W.W. J.A.L. D.H.W. M.J.L. S.K. S.J. H.Y.K. J.-E.S. J.H.Y. and H.-J.P.; Resources, K.D.P. B.K. Jin, E.M.H. J.L. N.W.K. H.R. H.J.L. H.S. S.-J.O. S.E.L. and I.-J.C.; Writing ? Original Draft, M.H.N. and C.J.L.; Writing ? Review & Editing, M.-H.N. J.Y.H. J.K. and C.J.L.; Visualization, M.-H.N. and J.K.; Supervision, O.H. B.K. Jin, S.H.P. G.R.K. I.S. H.R. S.R.J. and C.J.L.; Funding Acquisition, J.Y.H. M.-H.N. J.K. H.R. S.R.J. and C.J.L. The authors declare no competing financial interests.

Publisher Copyright:
© 2019 Elsevier Ltd

All Science Journal Classification (ASJC) codes

Biochemistry, Genetics and Molecular Biology(all)
Agricultural and Biological Sciences(all)

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10.1016/j.cub.2019.11.079

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Heo, J. Y., Nam, M. H., Yoon, H. H., Kim, J., Hwang, Y. J., Won, W., Woo, D. H., Lee, J. A., Park, H. J., Jo, S., Lee, M. J., Kim, S., Shim, J. E., Jang, D. P., Kim, K. I., Huh, S. H., Jeong, J. Y., Kowall, N. W., Lee, J., ... Lee, C. J. (2020). Aberrant Tonic Inhibition of Dopaminergic Neuronal Activity Causes Motor Symptoms in Animal Models of Parkinson's Disease. Current Biology, 30(2), 276-291.e9. https://doi.org/10.1016/j.cub.2019.11.079

@article{c48c02626c214bdc9cfe1711501d2047,

title = "Aberrant Tonic Inhibition of Dopaminergic Neuronal Activity Causes Motor Symptoms in Animal Models of Parkinson's Disease",

abstract = "Current pharmacological treatments for Parkinson's disease (PD) are focused on symptomatic relief, but not on disease modification, based on the strong belief that PD is caused by irreversible dopaminergic neuronal death. Thus, the concept of the presence of dormant dopaminergic neurons and its possibility as the disease-modifying therapeutic target against PD have not been explored. Here we show that optogenetic activation of substantia nigra pars compacta (SNpc) neurons alleviates parkinsonism in acute PD animal models by recovering tyrosine hydroxylase (TH) from the TH-negative dormant dopaminergic neurons, some of which still express DOPA decarboxylase (DDC). The TH loss depends on reduced dopaminergic neuronal firing under aberrant tonic inhibition, which is attributed to excessive astrocytic GABA. Blocking the astrocytic GABA synthesis recapitulates the therapeutic effect of optogenetic activation. Consistently, SNpc of postmortem PD patients shows a significant population of TH-negative/DDC-positive dormant neurons surrounded by numerous GABA-positive astrocytes. We propose that disinhibiting dormant dopaminergic neurons by blocking excessive astrocytic GABA could be an effective therapeutic strategy against PD. Heo et al. report that astrocytic GABA-mediated aberrant tonic inhibition of DA neurons leads to a reduction in TH expression and dopamine production, causing dormant DA neurons and motor deficits. Blocking astrocytic GABA synthesis by MAO-B inhibition or optogenetic activation of dormant DA neurons reverses PD pathology.",

author = "Heo, {Jun Young} and Nam, {Min Ho} and Yoon, {Hyung Ho} and Jeongyeon Kim and Hwang, {Yu Jin} and Woojin Won and Woo, {Dong Ho} and Lee, {Ji Ae} and Park, {Hyun Jung} and Seonmi Jo and Lee, {Min Joung} and Sunpil Kim and Shim, {Jeong Eun} and Jang, {Dong Pyo} and Kim, {Kyoung I.} and Huh, {Sue H.} and Jeong, {Jae Y.} and Kowall, {Neil W.} and Junghee Lee and Hyeonjoo Im and Park, {Jong Hyun} and Jang, {Bo Ko} and Park, {Ki Duk} and Lee, {Hyunjoo J.} and Hyogeun Shin and Cho, {Il Joo} and Hwang, {Eun Mi} and Kim, {Young Soo} and Kim, {Hye Yun} and Oh, {Soo Jin} and Lee, {Seung Eun} and Paek, {Sun Ha} and Yoon, {Jong Hyuk} and Jin, {Byung K.} and Kweon, {Gi Ryang} and Insop Shim and Onyou Hwang and Hoon Ryu and Jeon, {Sang Ryong} and Lee, {C. Justin}",

note = "Funding Information: The AAV-A53T viral vector was kindly provided by Dr. Jun-ichi Miyazaki at Kumamoto University. This work was supported by the Creative Research Initiative Program ( 2015R1A3A2066619 ) of the National Research Foundation (NRF) of Korea funded by the Ministry of Science and ICT of Korea and Institute for Basic Science (IBS), Center for Cognition and Sociality ( IBS-R001-D2 ) to C.J.L.; Asan Life Science Institute grants ( 18-241 and 19-241 ) funded by the Asan Medical Center to S.R.J.; Brain Science Program ( 2018M3C7A1056894 ) funded by NRF of Korea to H.R.; KIST institutional program (Project No. 2E29221 ) and Brain Science Program ( 2018M3C7A1056897 ) funded by the NRF of Korea to M.H.N.; MRC program ( 2017R1A5A2015385 ) funded by the Ministry of Science and ICT of Korea to J.Y.H.; and KBRI basic research program (20-BR-02-05) through Korea Brain Research Institute funded by the Ministry of Science and ICT of Korea to J.K. Funding Information: The AAV-A53T viral vector was kindly provided by Dr. Jun-ichi Miyazaki at Kumamoto University. This work was supported by the Creative Research Initiative Program (2015R1A3A2066619) of the National Research Foundation (NRF) of Korea funded by the Ministry of Science and ICT of Korea and Institute for Basic Science (IBS), Center for Cognition and Sociality (IBS-R001-D2) to C.J.L.; Asan Life Science Institute grants (18-241 and 19-241) funded by the Asan Medical Center to S.R.J.; Brain Science Program (2018M3C7A1056894) funded by NRF of Korea to H.R.; KIST institutional program (Project No. 2E29221) and Brain Science Program (2018M3C7A1056897) funded by the NRF of Korea to M.H.N.; MRC program (2017R1A5A2015385) funded by the Ministry of Science and ICT of Korea to J.Y.H.; and KBRI basic research program (20-BR-02-05) through Korea Brain Research Institute funded by the Ministry of Science and ICT of Korea to J.K. Conceptualization, J.Y.H. M.-H.N. H.R. S.R.J. and C.J.L.; Methodology, S.H.H. S.J. J.Y.J. K.I.K. D.-P.J. and S.H.P.; Investigation, J.Y.H. M.-H.N. H.H.Y. J.K. Y.J.H. W.W. J.A.L. D.H.W. M.J.L. S.K. S.J. H.Y.K. J.-E.S. J.H.Y. and H.-J.P.; Resources, K.D.P. B.K. Jin, E.M.H. J.L. N.W.K. H.R. H.J.L. H.S. S.-J.O. S.E.L. and I.-J.C.; Writing ? Original Draft, M.H.N. and C.J.L.; Writing ? Review & Editing, M.-H.N. J.Y.H. J.K. and C.J.L.; Visualization, M.-H.N. and J.K.; Supervision, O.H. B.K. Jin, S.H.P. G.R.K. I.S. H.R. S.R.J. and C.J.L.; Funding Acquisition, J.Y.H. M.-H.N. J.K. H.R. S.R.J. and C.J.L. The authors declare no competing financial interests. Publisher Copyright: {\textcopyright} 2019 Elsevier Ltd",

year = "2020",

month = jan,

day = "20",

doi = "10.1016/j.cub.2019.11.079",

language = "English",

volume = "30",

pages = "276--291.e9",

journal = "Current Biology",

issn = "0960-9822",

publisher = "Cell Press",

number = "2",

}

Heo, JY, Nam, MH, Yoon, HH, Kim, J, Hwang, YJ, Won, W, Woo, DH, Lee, JA, Park, HJ, Jo, S, Lee, MJ, Kim, S, Shim, JE, Jang, DP, Kim, KI, Huh, SH, Jeong, JY, Kowall, NW, Lee, J, Im, H, Park, JH, Jang, BK, Park, KD, Lee, HJ, Shin, H, Cho, IJ, Hwang, EM, Kim, YS, Kim, HY, Oh, SJ, Lee, SE, Paek, SH, Yoon, JH, Jin, BK, Kweon, GR, Shim, I, Hwang, O, Ryu, H, Jeon, SR & Lee, CJ 2020, 'Aberrant Tonic Inhibition of Dopaminergic Neuronal Activity Causes Motor Symptoms in Animal Models of Parkinson's Disease', Current Biology, vol. 30, no. 2, pp. 276-291.e9. https://doi.org/10.1016/j.cub.2019.11.079

TY - JOUR

T1 - Aberrant Tonic Inhibition of Dopaminergic Neuronal Activity Causes Motor Symptoms in Animal Models of Parkinson's Disease

AU - Heo, Jun Young

AU - Nam, Min Ho

AU - Yoon, Hyung Ho

AU - Kim, Jeongyeon

AU - Hwang, Yu Jin

AU - Won, Woojin

AU - Woo, Dong Ho

AU - Lee, Ji Ae

AU - Park, Hyun Jung

AU - Jo, Seonmi

AU - Lee, Min Joung

AU - Kim, Sunpil

AU - Shim, Jeong Eun

AU - Jang, Dong Pyo

AU - Kim, Kyoung I.

AU - Huh, Sue H.

AU - Jeong, Jae Y.

AU - Kowall, Neil W.

AU - Lee, Junghee

AU - Im, Hyeonjoo

AU - Park, Jong Hyun

AU - Jang, Bo Ko

AU - Park, Ki Duk

AU - Lee, Hyunjoo J.

AU - Shin, Hyogeun

AU - Cho, Il Joo

AU - Hwang, Eun Mi

AU - Kim, Young Soo

AU - Kim, Hye Yun

AU - Oh, Soo Jin

AU - Lee, Seung Eun

AU - Paek, Sun Ha

AU - Yoon, Jong Hyuk

AU - Jin, Byung K.

AU - Kweon, Gi Ryang

AU - Shim, Insop

AU - Hwang, Onyou

AU - Ryu, Hoon

AU - Jeon, Sang Ryong

AU - Lee, C. Justin

N1 - Funding Information: The AAV-A53T viral vector was kindly provided by Dr. Jun-ichi Miyazaki at Kumamoto University. This work was supported by the Creative Research Initiative Program ( 2015R1A3A2066619 ) of the National Research Foundation (NRF) of Korea funded by the Ministry of Science and ICT of Korea and Institute for Basic Science (IBS), Center for Cognition and Sociality ( IBS-R001-D2 ) to C.J.L.; Asan Life Science Institute grants ( 18-241 and 19-241 ) funded by the Asan Medical Center to S.R.J.; Brain Science Program ( 2018M3C7A1056894 ) funded by NRF of Korea to H.R.; KIST institutional program (Project No. 2E29221 ) and Brain Science Program ( 2018M3C7A1056897 ) funded by the NRF of Korea to M.H.N.; MRC program ( 2017R1A5A2015385 ) funded by the Ministry of Science and ICT of Korea to J.Y.H.; and KBRI basic research program (20-BR-02-05) through Korea Brain Research Institute funded by the Ministry of Science and ICT of Korea to J.K. Funding Information: The AAV-A53T viral vector was kindly provided by Dr. Jun-ichi Miyazaki at Kumamoto University. This work was supported by the Creative Research Initiative Program (2015R1A3A2066619) of the National Research Foundation (NRF) of Korea funded by the Ministry of Science and ICT of Korea and Institute for Basic Science (IBS), Center for Cognition and Sociality (IBS-R001-D2) to C.J.L.; Asan Life Science Institute grants (18-241 and 19-241) funded by the Asan Medical Center to S.R.J.; Brain Science Program (2018M3C7A1056894) funded by NRF of Korea to H.R.; KIST institutional program (Project No. 2E29221) and Brain Science Program (2018M3C7A1056897) funded by the NRF of Korea to M.H.N.; MRC program (2017R1A5A2015385) funded by the Ministry of Science and ICT of Korea to J.Y.H.; and KBRI basic research program (20-BR-02-05) through Korea Brain Research Institute funded by the Ministry of Science and ICT of Korea to J.K. Conceptualization, J.Y.H. M.-H.N. H.R. S.R.J. and C.J.L.; Methodology, S.H.H. S.J. J.Y.J. K.I.K. D.-P.J. and S.H.P.; Investigation, J.Y.H. M.-H.N. H.H.Y. J.K. Y.J.H. W.W. J.A.L. D.H.W. M.J.L. S.K. S.J. H.Y.K. J.-E.S. J.H.Y. and H.-J.P.; Resources, K.D.P. B.K. Jin, E.M.H. J.L. N.W.K. H.R. H.J.L. H.S. S.-J.O. S.E.L. and I.-J.C.; Writing ? Original Draft, M.H.N. and C.J.L.; Writing ? Review & Editing, M.-H.N. J.Y.H. J.K. and C.J.L.; Visualization, M.-H.N. and J.K.; Supervision, O.H. B.K. Jin, S.H.P. G.R.K. I.S. H.R. S.R.J. and C.J.L.; Funding Acquisition, J.Y.H. M.-H.N. J.K. H.R. S.R.J. and C.J.L. The authors declare no competing financial interests. Publisher Copyright: © 2019 Elsevier Ltd

PY - 2020/1/20

Y1 - 2020/1/20

N2 - Current pharmacological treatments for Parkinson's disease (PD) are focused on symptomatic relief, but not on disease modification, based on the strong belief that PD is caused by irreversible dopaminergic neuronal death. Thus, the concept of the presence of dormant dopaminergic neurons and its possibility as the disease-modifying therapeutic target against PD have not been explored. Here we show that optogenetic activation of substantia nigra pars compacta (SNpc) neurons alleviates parkinsonism in acute PD animal models by recovering tyrosine hydroxylase (TH) from the TH-negative dormant dopaminergic neurons, some of which still express DOPA decarboxylase (DDC). The TH loss depends on reduced dopaminergic neuronal firing under aberrant tonic inhibition, which is attributed to excessive astrocytic GABA. Blocking the astrocytic GABA synthesis recapitulates the therapeutic effect of optogenetic activation. Consistently, SNpc of postmortem PD patients shows a significant population of TH-negative/DDC-positive dormant neurons surrounded by numerous GABA-positive astrocytes. We propose that disinhibiting dormant dopaminergic neurons by blocking excessive astrocytic GABA could be an effective therapeutic strategy against PD. Heo et al. report that astrocytic GABA-mediated aberrant tonic inhibition of DA neurons leads to a reduction in TH expression and dopamine production, causing dormant DA neurons and motor deficits. Blocking astrocytic GABA synthesis by MAO-B inhibition or optogenetic activation of dormant DA neurons reverses PD pathology.

AB - Current pharmacological treatments for Parkinson's disease (PD) are focused on symptomatic relief, but not on disease modification, based on the strong belief that PD is caused by irreversible dopaminergic neuronal death. Thus, the concept of the presence of dormant dopaminergic neurons and its possibility as the disease-modifying therapeutic target against PD have not been explored. Here we show that optogenetic activation of substantia nigra pars compacta (SNpc) neurons alleviates parkinsonism in acute PD animal models by recovering tyrosine hydroxylase (TH) from the TH-negative dormant dopaminergic neurons, some of which still express DOPA decarboxylase (DDC). The TH loss depends on reduced dopaminergic neuronal firing under aberrant tonic inhibition, which is attributed to excessive astrocytic GABA. Blocking the astrocytic GABA synthesis recapitulates the therapeutic effect of optogenetic activation. Consistently, SNpc of postmortem PD patients shows a significant population of TH-negative/DDC-positive dormant neurons surrounded by numerous GABA-positive astrocytes. We propose that disinhibiting dormant dopaminergic neurons by blocking excessive astrocytic GABA could be an effective therapeutic strategy against PD. Heo et al. report that astrocytic GABA-mediated aberrant tonic inhibition of DA neurons leads to a reduction in TH expression and dopamine production, causing dormant DA neurons and motor deficits. Blocking astrocytic GABA synthesis by MAO-B inhibition or optogenetic activation of dormant DA neurons reverses PD pathology.

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DO - 10.1016/j.cub.2019.11.079

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VL - 30

SP - 276-291.e9

JO - Current Biology

JF - Current Biology

IS - 2

ER -

Aberrant Tonic Inhibition of Dopaminergic Neuronal Activity Causes Motor Symptoms in Animal Models of Parkinson's Disease

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