Pharmacological validation of TDO as a target for Parkinson’s disease

Paula Perez-Pardo; Yvonne Grobben; Nicole Willemsen-Seegers; Mitch Hartog; Michaela Tutone; Michelle Muller; Youri Adolfs; Ronald Jeroen Pasterkamp; Diep Vu-Pham; Antoon M. van Doornmalen; Freek van Cauter; Joeri de Wit; Jan Gerard Sterrenburg; Joost C.M. Uitdehaag; Jos de Man; Rogier C. Buijsman; Guido J.R. Zaman; Aletta D. Kraneveld

doi:10.1111/febs.15721

Pharmacological validation of TDO as a target for Parkinson’s disease

Paula Perez-Pardo, Yvonne Grobben, Nicole Willemsen-Seegers, Mitch Hartog, Michaela Tutone, Michelle Muller, Youri Adolfs, Ronald Jeroen Pasterkamp, Diep Vu-Pham, Antoon M. van Doornmalen, Freek van Cauter, Joeri de Wit, Jan Gerard Sterrenburg, Joost C.M. Uitdehaag, Jos de Man, Rogier C. Buijsman, Guido J.R. Zaman^*, Aletta D. Kraneveld

^*Corresponding author for this work

Netherlands Translational Research Center B.V.

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

Abstract

Parkinson’s disease patients suffer from both motor and nonmotor impairments. There is currently no cure for Parkinson’s disease, and the most commonly used treatment, levodopa, only functions as a temporary relief of motor symptoms. Inhibition of the expression of the L-tryptophan-catabolizing enzyme tryptophan 2,3-dioxygenase (TDO) has been shown to inhibit aging-related α-synuclein toxicity in Caenorhabditis elegans. To evaluate TDO inhibition as a potential therapeutic strategy for Parkinson’s disease, a brain-penetrable, small molecule TDO inhibitor was developed, referred to as NTRC 3531-0. This compound potently inhibits human and mouse TDO in biochemical and cell-based assays and is selective over IDO1, an evolutionary unrelated enzyme that catalyzes the same reaction. In mice, NTRC 3531-0 increased plasma and brain L-tryptophan levels after oral administration, demonstrating inhibition of TDO activity in vivo. The effect on Parkinson’s disease symptoms was evaluated in a rotenone-induced Parkinson’s disease mouse model. A structurally dissimilar TDO inhibitor, LM10, was evaluated in parallel. Both inhibitors had beneficial effects on rotenone-induced motor and cognitive dysfunction as well as rotenone-induced dopaminergic cell loss and neuroinflammation in the substantia nigra. Moreover, both inhibitors improved intestinal transit and enhanced colon length, which indicates a reduction of the rotenone-induced intestinal dysfunction. Consistent with this, mice treated with TDO inhibitor showed decreased expression of rotenone-induced glial fibrillary acidic protein, which is a marker of enteric glial cells, and decreased α-synuclein accumulation in the enteric plexus. Our data support TDO inhibition as a potential therapeutic strategy to decrease motor, cognitive, and gastrointestinal symptoms in Parkinson’s disease.

Original language	English
Pages (from-to)	4311-4331
Number of pages	21
Journal	FEBS Journal
Volume	288
Issue number	14
Early online date	20 Jan 2021
DOIs	https://doi.org/10.1111/febs.15721
Publication status	Published - Jul 2021

Bibliographical note

Funding Information:
This work was supported by grants from the Michael J. Fox Foundation (grant number 9951 to RCB) and the Netherlands Organization of Scientific Research (NWO) (KIEM 731.014.110 to ADK). The authors thank Helma van den Hurk, Steven van Helden and their colleagues from the Pivot Park Screening Centre, Oss, the Netherlands for high‐throughput screening, and the MIND facility of the UMC Utrecht Brain Center for support with iDISCO. The graphical abstract was created with BioRender.com.

Publisher Copyright:
© 2021 The Authors. The FEBS Journal published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.

Funding

This work was supported by grants from the Michael J. Fox Foundation (grant number 9951 to RCB) and the Netherlands Organization of Scientific Research (NWO) (KIEM 731.014.110 to ADK). The authors thank Helma van den Hurk, Steven van Helden and their colleagues from the Pivot Park Screening Centre, Oss, the Netherlands for high‐throughput screening, and the MIND facility of the UMC Utrecht Brain Center for support with iDISCO. The graphical abstract was created with BioRender.com.

Keywords

blood–brain barrier
enzyme inhibitors
L-tryptophan
rotenone
tryptophan 2,3-dioxygenase

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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The FEBS Journal - 2021 - Perez‐Pardo - Pharmacological validation of TDO as a target for Parkinson s diseaseFinal published version, 1.39 MBLicence: CC BY

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Perez-Pardo, P., Grobben, Y., Willemsen-Seegers, N., Hartog, M., Tutone, M., Muller, M., Adolfs, Y., Pasterkamp, R. J., Vu-Pham, D., van Doornmalen, A. M., van Cauter, F., de Wit, J., Gerard Sterrenburg, J., Uitdehaag, J. C. M., de Man, J., Buijsman, R. C., Zaman, G. J. R., & Kraneveld, A. D. (2021). Pharmacological validation of TDO as a target for Parkinson’s disease. FEBS Journal, 288(14), 4311-4331. https://doi.org/10.1111/febs.15721

@article{04124937cce141a89aef0b55d35ecaec,

title = "Pharmacological validation of TDO as a target for Parkinson{\textquoteright}s disease",

abstract = "Parkinson{\textquoteright}s disease patients suffer from both motor and nonmotor impairments. There is currently no cure for Parkinson{\textquoteright}s disease, and the most commonly used treatment, levodopa, only functions as a temporary relief of motor symptoms. Inhibition of the expression of the L-tryptophan-catabolizing enzyme tryptophan 2,3-dioxygenase (TDO) has been shown to inhibit aging-related α-synuclein toxicity in Caenorhabditis elegans. To evaluate TDO inhibition as a potential therapeutic strategy for Parkinson{\textquoteright}s disease, a brain-penetrable, small molecule TDO inhibitor was developed, referred to as NTRC 3531-0. This compound potently inhibits human and mouse TDO in biochemical and cell-based assays and is selective over IDO1, an evolutionary unrelated enzyme that catalyzes the same reaction. In mice, NTRC 3531-0 increased plasma and brain L-tryptophan levels after oral administration, demonstrating inhibition of TDO activity in vivo. The effect on Parkinson{\textquoteright}s disease symptoms was evaluated in a rotenone-induced Parkinson{\textquoteright}s disease mouse model. A structurally dissimilar TDO inhibitor, LM10, was evaluated in parallel. Both inhibitors had beneficial effects on rotenone-induced motor and cognitive dysfunction as well as rotenone-induced dopaminergic cell loss and neuroinflammation in the substantia nigra. Moreover, both inhibitors improved intestinal transit and enhanced colon length, which indicates a reduction of the rotenone-induced intestinal dysfunction. Consistent with this, mice treated with TDO inhibitor showed decreased expression of rotenone-induced glial fibrillary acidic protein, which is a marker of enteric glial cells, and decreased α-synuclein accumulation in the enteric plexus. Our data support TDO inhibition as a potential therapeutic strategy to decrease motor, cognitive, and gastrointestinal symptoms in Parkinson{\textquoteright}s disease.",

keywords = "blood–brain barrier, enzyme inhibitors, L-tryptophan, rotenone, tryptophan 2,3-dioxygenase",

author = "Paula Perez-Pardo and Yvonne Grobben and Nicole Willemsen-Seegers and Mitch Hartog and Michaela Tutone and Michelle Muller and Youri Adolfs and Pasterkamp, {Ronald Jeroen} and Diep Vu-Pham and {van Doornmalen}, {Antoon M.} and {van Cauter}, Freek and {de Wit}, Joeri and {Gerard Sterrenburg}, Jan and Uitdehaag, {Joost C.M.} and {de Man}, Jos and Buijsman, {Rogier C.} and Zaman, {Guido J.R.} and Kraneveld, {Aletta D.}",

note = "Funding Information: This work was supported by grants from the Michael J. Fox Foundation (grant number 9951 to RCB) and the Netherlands Organization of Scientific Research (NWO) (KIEM 731.014.110 to ADK). The authors thank Helma van den Hurk, Steven van Helden and their colleagues from the Pivot Park Screening Centre, Oss, the Netherlands for high‐throughput screening, and the MIND facility of the UMC Utrecht Brain Center for support with iDISCO. The graphical abstract was created with BioRender.com. Publisher Copyright: {\textcopyright} 2021 The Authors. The FEBS Journal published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.",

year = "2021",

month = jul,

doi = "10.1111/febs.15721",

language = "English",

volume = "288",

pages = "4311--4331",

journal = "FEBS Journal",

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Perez-Pardo, P, Grobben, Y, Willemsen-Seegers, N, Hartog, M, Tutone, M, Muller, M, Adolfs, Y, Pasterkamp, RJ, Vu-Pham, D, van Doornmalen, AM, van Cauter, F, de Wit, J, Gerard Sterrenburg, J, Uitdehaag, JCM, de Man, J, Buijsman, RC, Zaman, GJR & Kraneveld, AD 2021, 'Pharmacological validation of TDO as a target for Parkinson’s disease', FEBS Journal, vol. 288, no. 14, pp. 4311-4331. https://doi.org/10.1111/febs.15721

TY - JOUR

T1 - Pharmacological validation of TDO as a target for Parkinson’s disease

AU - Perez-Pardo, Paula

AU - Grobben, Yvonne

AU - Willemsen-Seegers, Nicole

AU - Hartog, Mitch

AU - Tutone, Michaela

AU - Muller, Michelle

AU - Adolfs, Youri

AU - Pasterkamp, Ronald Jeroen

AU - Vu-Pham, Diep

AU - van Doornmalen, Antoon M.

AU - van Cauter, Freek

AU - de Wit, Joeri

AU - Gerard Sterrenburg, Jan

AU - Uitdehaag, Joost C.M.

AU - de Man, Jos

AU - Buijsman, Rogier C.

AU - Zaman, Guido J.R.

AU - Kraneveld, Aletta D.

N1 - Funding Information: This work was supported by grants from the Michael J. Fox Foundation (grant number 9951 to RCB) and the Netherlands Organization of Scientific Research (NWO) (KIEM 731.014.110 to ADK). The authors thank Helma van den Hurk, Steven van Helden and their colleagues from the Pivot Park Screening Centre, Oss, the Netherlands for high‐throughput screening, and the MIND facility of the UMC Utrecht Brain Center for support with iDISCO. The graphical abstract was created with BioRender.com. Publisher Copyright: © 2021 The Authors. The FEBS Journal published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.

PY - 2021/7

Y1 - 2021/7

N2 - Parkinson’s disease patients suffer from both motor and nonmotor impairments. There is currently no cure for Parkinson’s disease, and the most commonly used treatment, levodopa, only functions as a temporary relief of motor symptoms. Inhibition of the expression of the L-tryptophan-catabolizing enzyme tryptophan 2,3-dioxygenase (TDO) has been shown to inhibit aging-related α-synuclein toxicity in Caenorhabditis elegans. To evaluate TDO inhibition as a potential therapeutic strategy for Parkinson’s disease, a brain-penetrable, small molecule TDO inhibitor was developed, referred to as NTRC 3531-0. This compound potently inhibits human and mouse TDO in biochemical and cell-based assays and is selective over IDO1, an evolutionary unrelated enzyme that catalyzes the same reaction. In mice, NTRC 3531-0 increased plasma and brain L-tryptophan levels after oral administration, demonstrating inhibition of TDO activity in vivo. The effect on Parkinson’s disease symptoms was evaluated in a rotenone-induced Parkinson’s disease mouse model. A structurally dissimilar TDO inhibitor, LM10, was evaluated in parallel. Both inhibitors had beneficial effects on rotenone-induced motor and cognitive dysfunction as well as rotenone-induced dopaminergic cell loss and neuroinflammation in the substantia nigra. Moreover, both inhibitors improved intestinal transit and enhanced colon length, which indicates a reduction of the rotenone-induced intestinal dysfunction. Consistent with this, mice treated with TDO inhibitor showed decreased expression of rotenone-induced glial fibrillary acidic protein, which is a marker of enteric glial cells, and decreased α-synuclein accumulation in the enteric plexus. Our data support TDO inhibition as a potential therapeutic strategy to decrease motor, cognitive, and gastrointestinal symptoms in Parkinson’s disease.

AB - Parkinson’s disease patients suffer from both motor and nonmotor impairments. There is currently no cure for Parkinson’s disease, and the most commonly used treatment, levodopa, only functions as a temporary relief of motor symptoms. Inhibition of the expression of the L-tryptophan-catabolizing enzyme tryptophan 2,3-dioxygenase (TDO) has been shown to inhibit aging-related α-synuclein toxicity in Caenorhabditis elegans. To evaluate TDO inhibition as a potential therapeutic strategy for Parkinson’s disease, a brain-penetrable, small molecule TDO inhibitor was developed, referred to as NTRC 3531-0. This compound potently inhibits human and mouse TDO in biochemical and cell-based assays and is selective over IDO1, an evolutionary unrelated enzyme that catalyzes the same reaction. In mice, NTRC 3531-0 increased plasma and brain L-tryptophan levels after oral administration, demonstrating inhibition of TDO activity in vivo. The effect on Parkinson’s disease symptoms was evaluated in a rotenone-induced Parkinson’s disease mouse model. A structurally dissimilar TDO inhibitor, LM10, was evaluated in parallel. Both inhibitors had beneficial effects on rotenone-induced motor and cognitive dysfunction as well as rotenone-induced dopaminergic cell loss and neuroinflammation in the substantia nigra. Moreover, both inhibitors improved intestinal transit and enhanced colon length, which indicates a reduction of the rotenone-induced intestinal dysfunction. Consistent with this, mice treated with TDO inhibitor showed decreased expression of rotenone-induced glial fibrillary acidic protein, which is a marker of enteric glial cells, and decreased α-synuclein accumulation in the enteric plexus. Our data support TDO inhibition as a potential therapeutic strategy to decrease motor, cognitive, and gastrointestinal symptoms in Parkinson’s disease.

KW - blood–brain barrier

KW - enzyme inhibitors

KW - L-tryptophan

KW - rotenone

KW - tryptophan 2,3-dioxygenase

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U2 - 10.1111/febs.15721

DO - 10.1111/febs.15721

M3 - Article

C2 - 33471408

AN - SCOPUS:85101100439

SN - 1742-464X

VL - 288

SP - 4311

EP - 4331

JO - FEBS Journal

JF - FEBS Journal

IS - 14

ER -

Pharmacological validation of TDO as a target for Parkinson’s disease

Abstract

Bibliographical note

Funding

Keywords

UN SDGs

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