Arginine is a disease modifier for polyQ disease models that stabilizes polyQ protein conformation.

Minakawa, Eiko N; Popiel, Helena Akiko; Tada, Masayoshi; Takahashi, Toshiaki; Yamane, Hiroshi; Saitoh, Yuji; Takahashi, Yasuo; Ozawa, Daisaku; Takeda, Akiko; Takeuchi, Toshihide; Okamoto, Yuma; Yamamoto, Kazuhiro; Suzuki, Mari; Fujita, Hiromi; Ito, Chiyomi; Yagihara, Hiroko; Saito, Yuko; Watase, Kei; Adachi, Hiroaki; Katsuno, Masahisa; Mochizuki, Hideki; Shiraki, Kentaro; Sobue, Gen; Toda, Tatsushi; Wada, Keiji; Onodera, Osamu; Nagai, Yoshitaka

Minakawa, Eiko N; Popiel, Helena Akiko; Tada, Masayoshi; Takahashi, Toshiaki; Yamane, Hiroshi; Saitoh, Yuji; Takahashi, Yasuo; Ozawa, Daisaku; Takeda, Akiko; Takeuchi, Toshihide; Okamoto, Yuma; Yamamoto, Kazuhiro; Suzuki, Mari; Fujita, Hiromi; Ito, Chiyomi; Yagihara, Hiroko; Saito, Yuko; Watase, Kei; Adachi, Hiroaki; Katsuno, Masahisa; Mochizuki, Hideki; Shiraki, Kentaro; Sobue, Gen; Toda, Tatsushi; Wada, Keiji; Onodera, Osamu; Nagai, Yoshitaka.

Affiliation

Minakawa EN; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Popiel HA; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Tada M; Division of Clinical Genetics, Osaka University Graduate School of Medicine, Suita, Osaka, Japan.
Takahashi T; Department of Neurology, Brain Research Institute, Niigata University, Niigata, Niigata, Japan.
Yamane H; Department of Neurology, Brain Research Institute, Niigata University, Niigata, Niigata, Japan.
Saitoh Y; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Takahashi Y; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Ozawa D; Olympus Corporation, Hachioji, Tokyo, Japan.
Takeda A; Department of Neurotherapeutics, Osaka University Graduate School of Medicine, Suita, Osaka, Japan.
Takeuchi T; Department of Neurotherapeutics, Osaka University Graduate School of Medicine, Suita, Osaka, Japan.
Okamoto Y; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Yamamoto K; Department of Neurotherapeutics, Osaka University Graduate School of Medicine, Suita, Osaka, Japan.
Suzuki M; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Fujita H; Division of Clinical Genetics, Osaka University Graduate School of Medicine, Suita, Osaka, Japan.
Ito C; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Yagihara H; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Saito Y; Department of Neurotherapeutics, Osaka University Graduate School of Medicine, Suita, Osaka, Japan.
Watase K; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Adachi H; Division of Clinical Genetics, Osaka University Graduate School of Medicine, Suita, Osaka, Japan.
Katsuno M; Department of Degenerative Neurological Diseases, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Mochizuki H; Department of Pathology and Laboratory Medicine, National Center Hospital, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.
Shiraki K; Center for Brain Integration Research, Tokyo Medical and Dental University, Bunkyo-ku, Tokyo, Japan.
Sobue G; Department of Neurology, Nagoya University Graduate School of Medicine, Nagoya, Aichi, Japan.
Toda T; Department of Neurology, Nagoya University Graduate School of Medicine, Nagoya, Aichi, Japan.
Wada K; Department of Neurology, Osaka University Graduate School of Medicine, Suita, Osaka, Japan.
Onodera O; Faculty of Pure and Applied Sciences, University of Tsukuba, Tsukuba, Ibaraki, Japan.
Nagai Y; Department of Neurology, Nagoya University Graduate School of Medicine, Nagoya, Aichi, Japan.

Brain ; 143(6): 1811-1825, 2020 06 01.

Article in En | MEDLINE | ID: mdl-32436573

ABSTRACT

ABSTRACT

The polyglutamine (polyQ) diseases are a group of inherited neurodegenerative diseases that include Huntington's disease, various spinocerebellar ataxias, spinal and bulbar muscular atrophy, and dentatorubral pallidoluysian atrophy. They are caused by the abnormal expansion of a CAG repeat coding for the polyQ stretch in the causative gene of each disease. The expanded polyQ stretches trigger abnormal ß-sheet conformational transition and oligomerization followed by aggregation of the polyQ proteins in the affected neurons, leading to neuronal toxicity and neurodegeneration. Disease-modifying therapies that attenuate both symptoms and molecular pathogenesis of polyQ diseases remain an unmet clinical need. Here we identified arginine, a chemical chaperone that facilitates proper protein folding, as a novel compound that targets the upstream processes of polyQ protein aggregation by stabilizing the polyQ protein conformation. We first screened representative chemical chaperones using an in vitro polyQ aggregation assay, and identified arginine as a potent polyQ aggregation inhibitor. Our in vitro and cellular assays revealed that arginine exerts its anti-aggregation property by inhibiting the toxic ß-sheet conformational transition and oligomerization of polyQ proteins before the formation of insoluble aggregates. Arginine exhibited therapeutic effects on neurological symptoms and protein aggregation pathology in Caenorhabditis elegans, Drosophila, and two different mouse models of polyQ diseases. Arginine was also effective in a polyQ mouse model when administered after symptom onset. As arginine has been safely used for urea cycle defects and for mitochondrial myopathy, encephalopathy, lactic acid and stroke syndrome patients, and efficiently crosses the blood-brain barrier, a drug-repositioning approach for arginine would enable prompt clinical application as a promising disease-modifier drug for the polyQ diseases.

Subject(s)

Arginine/metabolism; Arginine/pharmacology; Peptides/metabolism; Animals; Caenorhabditis elegans/metabolism; Disease Models, Animal; Drosophila/metabolism; Female; Heredodegenerative Disorders, Nervous System/genetics; Huntington Disease/genetics; Male; Mice; Mice, Inbred Strains; Molecular Chaperones/genetics; Peptides/genetics; Protein Aggregation, Pathological; Protein Conformation/drug effects; Protein Folding/drug effects; Spinocerebellar Ataxias/genetics

Key words

arginine; chemical chaperone; disease-modifying therapy; polyglutamine diseases; protein conformation

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