Your search keyword '"polyglutamine disease"' showing total 19 results

1. Ribosomal protein SA is a common component of neuronal intranuclear inclusions in polyglutamine diseases and Marinesco bodies.

Author

Yagita, Kaoru, Sadashima, Shoko, Koyama, Sachiko, Noguchi, Hideko, Hamasaki, Hideomi, Sasagasako, Naokazu, and Honda, Hiroyuki

Abstract

Neuronal intranuclear inclusions (NIIs) are common key structures in polyglutamine (polyQ) diseases such as Huntington disease (HD), spinocerebellar ataxia type 1 (SCA1), and SCA3. Marinesco bodies (MBs) of dopaminergic neurons in the substantia nigra are also intranuclear structures and are frequently seen in normal elderly people. Ribosomal dysfunction is closely related to two differential processes; therefore, we aimed to identify the pathological characteristics of ribosomal protein SA (RPSA), a ribosomal protein, in both states. To this end, we evaluated the autopsy findings in four patients with HD, two SCA3, and five normal elderly cases (NCs). Immunohistochemical studies demonstrated that both NIIs and MBs contain RPSA. In polyQ diseases, RPSA was co‐localized with polyQ aggregations, and 3D‐reconstructed images revealed their mosaic‐like distribution. Assessments of the organization of RPSA and p62 in NIIs showed that RPSA was more localized toward the center than p62 and that this unique organization was more evident in the MBs. Immunoblotting of the temporal cortices revealed that the nuclear fraction of HD patients contained more RPSA than that of NCs. In conclusion, our study revealed that RPSA is a common component of both NIIs and MBs, indicating that a similar mechanism contributes to the formation of polyQ NIIs and MBs. [ABSTRACT FROM AUTHOR]

Published

2024

2. Expression profile analysis in cells overexpressing DRPLA cDNA to explore the roles of DRPLAp as a transcriptional coregulator.

Author

Hatano, Keiko, Date, Hidetoshi, Ishiura, Hiroyuki, Matsukawa, Takashi, Tanaka, Masaki, Mitsui, Jun, Goto, Jun, Yoshimura, Jun, Doi, Koichiro, Morishita, Shinichi, and Tsuji, Shoji

Subjects

*SPINOCEREBELLAR ataxia, *CELL analysis, *COMPLEMENTARY DNA, *RNA metabolism, *GENETIC overexpression, *GENETIC transcription regulation

Abstract

Background: Dentatorubral‐pallidoluysian atrophy (DRPLA) is an autosomal dominant neurodegenerative disorder caused by the unstable expansion of CAG repeats encoding polyglutamine stretches in DRPLA gene (ATN1). DRPLAp, the gene product of ATN1, is located in the nucleus and has been shown to function as a transcriptional coregulator. Its target genes, however, remain largely unknown. Aim: To elucidate the physiological functions of DRPLAp based on determination of the target genes regulated by wild‐type DRPLAp. Methods: Using the cultured cells expressing wild‐type full‐length DRPLA cDNA (Q19) encoding DRPLAp under the control of the doxycycline (Dox)‐On system, we searched for genes whose expression levels were regulated by wild‐type DRPLAp (Q19). Results: On the basis of detailed RNA‐seq analyses, we identified seven up‐regulated genes and five down‐regulated genes in Q19 cells. In gene ontology analysis, the up‐regulated differentially expressed genes formed clusters featuring skeletal system morphogenesis, transcriptional regulation, and RNA metabolism, which is consistent with the recent report that the mutations in ATN1 lead to recognizable facial form and variable congenital anomalies. Conclusion: These findings support that DRPLAp may play a role as a transcriptional coregulator involved in the regulation of development. [ABSTRACT FROM AUTHOR]

Published

2022

3. Coexistence of dentatorubral‐pallidoluysian atrophy and Parkinson's disease: An autopsy case report.

Author

Kim, Seong‐Ik, Kim, Hyunhee, Park, Jin Woo, Choi, Ji‐Hyun, Kim, Han Joon, Won, Jae Kyung, Jeon, Beomseok, and Park, Sung‐Hye

Subjects

*PARKINSON'S disease, *DENTATE nucleus, *AUTOPSY, *ATROPHY, *WHITE matter (Nerve tissue), *GRAY matter (Nerve tissue)

Abstract

We report an autopsy case of a 56‐year‐old male patient with the coexistence of dentatorubral‐pallidoluysian atrophy (DRPLA) and Parkinson's disease (PD). He presented with gait instability and dysarthria for 10 years. The removed brain showed general atrophy (988 g) with depigmentation of the substantia nigra. The neocortex and deep gray matter, including the red nucleus, subthalamic nuclei, and globus pallidus, were atrophic, and grumose degeneration of the cerebellar dentate nucleus was observed. Polyglutamine‐ and p62‐positive neuronal inclusions were present and widespread in the areas mentioned above. Interestingly, this case also had brainstem‐predominant PD pathology with α‐synuclein‐positive Lewy bodies and Lewy neurites. Generalized white matter atrophy with patchy loss of astrocytes in the white matter suggested glial dysfunction by elongated CAG repeats in the atrophin 1 gene (atrophin 1). Polymerase chain reaction (PCR) fragment analysis revealed increased CAG repeats (61) on atrophin 1 encoding atrophin 1. The patient had a family history of DRPLA, including his daughter, who was confirmed positive on genetic testing (CAG repeat: 65). His father, brother, and niece were suspected of having the disease. Clinicopathologically, all of the above findings are consistent with the coexistence of DRPLA and PD. So far, various overlapping neurodegenerative disorders have been reported, but the coexistence of DRPLA and PD has never been demonstrated in the published literature. Even though the exact time of PD development is unknown in this case, PD might develop after DRPLA, and the overwhelming symptoms of DRPLA might mask those of PD. Here, we report a clinicopathologically definite case of the coexistence of DRPLA and PD. White matter degeneration with patchy loss of astrocytes was another remarkable finding of this case. [ABSTRACT FROM AUTHOR]

Published

2021

4. Muscle BDNF improves synaptic and contractile muscle strength in Kennedy's disease mice in a muscle‐type specific manner.

Author

Halievski, Katherine, Xu, Youfen, Haddad, Yazeed W., Tang, Yu Ping, Yamada, Shinichiro, Katsuno, Masahisa, Adachi, Hiroaki, Sobue, Gen, Breedlove, S. Marc, and Jordan, Cynthia L.

Subjects

*MUSCLE strength, *MOUSE diseases, *BRAIN-derived neurotrophic factor, *MUSCLES, *SKELETAL muscle

Abstract

Key points: Muscle‐derived neurotrophic factors may offer therapeutic promise for treating neuromuscular diseases.We report that a muscle‐derived neurotrophic factor, BDNF, rescues synaptic and muscle function in a muscle‐type specific manner in mice modelling Kennedy's disease (KD).We also find that BDNF rescues select molecular mechanisms in slow and fast muscle that may underlie the improved cellular function.We also report for the first time that expression of BDNF, but not other members of the neurotrophin family, is perturbed in muscle from patients with KD.Given that muscle BDNF had divergent therapeutic effects that depended on muscle type, a combination of neurotrophic factors may optimally rescue neuromuscular function via effects on both pre‐ and postsynaptic function, in the face of disease. Deficits in muscle brain‐derived neurotrophic factor (BDNF) correlate with neuromuscular deficits in mouse models of Kennedy's disease (KD), suggesting that restoring muscle BDNF might restore function. To test this possibility, transgenic mice expressing human BDNF in skeletal muscle were crossed with '97Q' KD mice. We found that muscle BDNF slowed disease, doubling the time between symptom onset and endstage. BDNF also improved expression of genes in muscle known to play key roles in neuromuscular function, including counteracting the expression of neonatal isoforms induced by disease. Intriguingly, BDNF's ameliorative effects differed between muscle types: synaptic strength was rescued only in slow‐twitch muscle, while contractile strength was improved only in fast‐twitch muscle. In sum, muscle BDNF slows disease progression, rescuing select cellular and molecular mechanisms that depend on fibre type. Muscle BDNF expression was also affected in KD patients, reinforcing its translational and therapeutic potential for treating this disorder. Key points: Muscle‐derived neurotrophic factors may offer therapeutic promise for treating neuromuscular diseases.We report that a muscle‐derived neurotrophic factor, BDNF, rescues synaptic and muscle function in a muscle‐type specific manner in mice modelling Kennedy's disease (KD).We also find that BDNF rescues select molecular mechanisms in slow and fast muscle that may underlie the improved cellular function.We also report for the first time that expression of BDNF, but not other members of the neurotrophin family, is perturbed in muscle from patients with KD.Given that muscle BDNF had divergent therapeutic effects that depended on muscle type, a combination of neurotrophic factors may optimally rescue neuromuscular function via effects on both pre‐ and postsynaptic function, in the face of disease. [ABSTRACT FROM AUTHOR]

Published

2020

5. Bulbospinal muscular atrophy (Kennedy disease) responsive to immunoglobulins?

Author

Poustka, Katharina, Pollanz‐Petrovic, Sabine, Lindeck‐Pozza, Elisabeth, and Finsterer, Josef

Subjects

*MUSCULAR atrophy, *GYNECOMASTIA, *MUSCLE weakness, *MOTOR neuron diseases

Abstract

A 61 year old man with facial diplegia, quadruparesis, tongue atrophy/fasciculations, bulbar speech, muscle weakness/wasting, hypotonia, tremor, dysdiadochokinesia, absent tendon reflexes, fasciculations, and gynecomastia, received immunoglobulins for suspected immune‐neuropathy with limited benefit. After reconsideration, Kennedy disease was diagnosed upon 44 CAG repeats in AR. In conclusion, immunoglobulins exhibit limited benefit on immune‐neuropathy in patients with coexisting KD. [ABSTRACT FROM AUTHOR]

Published

2020

6. In vivo assessment of riluzole as a potential therapeutic drug for spinocerebellar ataxia type 3.

Author

Schmidt, Jana, Schmidt, Thorsten, Golla, Matthias, Lehmann, Lisa, Weber, Jonasz Jeremiasz, Hübener‐Schmid, Jeannette, and Riess, Olaf

Subjects

*RILUZOLE, *ANTICONVULSANTS, *SPINOCEREBELLAR ataxia, *NEURODEGENERATION, *POLYGLUTAMINE, *THERAPEUTICS

Abstract

Spinocerebellar ataxia type 3 ( SCA3) is an autosomal dominantly inherited neurodegenerative disorder for which no curative therapy is available. The cause of this disease is the expansion of a CAG repeat in the so-called ATXN3 gene leading to an expanded polyglutamine stretch in the ataxin-3 protein. Although the function of ataxin-3 has been defined as a deubiquitinating enzyme, the pathogenic pathway underlying SCA3 remains to be deciphered. Besides others, also the glutamatergic system seems to be altered in SCA3. The antiglutamatergic substance riluzole has thus been suggested as a potential therapeutic agent for SCA3. To assess whether riluzole is effective in the treatment of SCA3 in vivo, we used a phenotypically well-characterized conditional mouse model previously generated by us. Treatment with 10 mg/kg riluzole in the drinking water was started when mice showed impairment in rotarod performance. Post-symptomatic treatment with riluzole carried out for a period of 10 months led to reduction of the soluble ataxin-3 level and an increase in ataxin-3 positive accumulations, but did not improve motor deficits measured by rotarod. There was also no positive effect on home cage behavior or body weight. We even observed a pronounced reduction of calbindin expression in Purkinje cells in riluzole-treated mice. Thus, long-term treatment with riluzole was not able to alleviate disease symptoms observed in transgenic SCA3 mice and should be considered with caution in the treatment of human patients. [ABSTRACT FROM AUTHOR]

Published

2016

7. G protein-coupled receptor 26 immunoreactivity in intranuclear inclusions associated with polyglutamine and intranuclear inclusion body diseases.

Author

Mori, Fumiaki, Tanji, Kunikazu, Miki, Yasuo, Toyoshima, Yasuko, Yoshida, Mari, Kakita, Akiyoshi, Takahashi, Hitoshi, Utsumi, Jun, Sasaki, Hidenao, and Wakabayashi, Koichi

Subjects

*G protein coupled receptors, *POLYGLUTAMINE, *MEMBRANE proteins, *NEUROTRANSMITTERS, *NEURODEGENERATION

Abstract

G protein-coupled receptor 26 (GPR26) is one of the G-protein-coupled receptors (GPCRs), which comprise the largest family of membrane proteins and mediate most of the physiological responses to hormones, neurotransmitters and environmental stimulants. Although GPCRs are considered to play an important role in the pathophysiology of neurodegenerative disorders, it is uncertain whether GPR26 is involved in the pathogenesis of polyglutamine and intranuclear inclusion body diseases. We immunohistochemically examined the brain tissues of patients with four polyglutamine diseases (Huntington's disease, dentatorubral-pallidoluysian atrophy, and spinocerebellar ataxia types 1 and 3) and intranuclear inclusion body disease, and normal control subjects. In controls, anti-GPR26 antibody immunolabeled the neuronal cytoplasm in a diffuse granular pattern. Neuronal nuclear inclusions in polyglutamine diseases were immunopositive for GPR26. In intranuclear inclusion body disease, GPR26-positive nuclear inclusions were found in both neurons and glial cells. Marinesco bodies in aged control subjects were also positive for GPR26. Double immunofluorescence analysis revealed co-localization of GPR26 with polyglutamine or ubiquitin in these nuclear inclusions. These findings suggest that GPR26 may have a common role in the formation or degradation of intranuclear inclusions in several neurodegenerative diseases. [ABSTRACT FROM AUTHOR]

Published

2016

8. Novel candidate blood-based transcriptional biomarkers of machado-joseph disease.

Author

Raposo, Mafalda, Bettencourt, Conceição, Maciel, Patrícia, Gao, Fuying, Ramos, Amanda, Kazachkova, Nadiya, Vasconcelos, João, Kay, Teresa, Rodrigues, Ana João, Bettencourt, Bruno, Bruges‐Armas, Jácome, Geschwind, Daniel, Coppola, Giovanni, and Lima, Manuela

Abstract

ABSTRACT Background Machado-Joseph disease (or spinocerebellar ataxia type 3) is a late-onset polyglutamine neurodegenerative disorder caused by a mutation in the ATXN3 gene, which encodes for the ubiquitously expressed protein ataxin-3. Previous studies on cell and animal models have suggested that mutated ataxin-3 is involved in transcriptional dysregulation. Starting with a whole-transcriptome profiling of peripheral blood samples from patients and controls, we aimed to confirm abnormal expression profiles in Machado-Joseph disease and to identify promising up-regulated genes as potential candidate biomarkers of disease status. Methods The Illumina Human V4-HT12 array was used to measure transcriptome-wide gene expression in peripheral blood samples from 12 patients and 12 controls. Technical validation and validation in an independent set of samples were performed by quantitative real-time polymerase chain reaction (PCR). Results Based on the results from the microarray, twenty six genes, found to be up-regulated in patients, were selected for technical validation by quantitative real-time PCR (validation rate of 81% for the up-regulation trend). Fourteen of these were further tested in an independent set of 42 patients and 35 controls; 10 genes maintained the up-regulation trend ( FCGR3B, CSR2RA, CLC, TNFSF14, SLA, P2RY13, FPR2, SELPLG, YIPF6, and GPR96); FCGR3B, P2RY13, and SELPLG were significantly up-regulated in patients when compared with controls. Conclusions Our findings support the hypothesis that mutated ataxin-3 is associated with transcription dysregulation, detectable in peripheral blood cells. Furthermore, this is the first report suggesting a pool of up-regulated genes in Machado-Joseph disease that may have the potential to be used for fine phenotyping of this disease. © 2015 International Parkinson and Movement Disorder Society [ABSTRACT FROM AUTHOR]

Published

2015

9. Accumulation of the sigma-1 receptor is common to neuronal nuclear inclusions in various neurodegenerative diseases.

Author

Miki, Yasuo, Mori, Fumiaki, Kon, Tomoya, Tanji, Kunikazu, Toyoshima, Yasuko, Yoshida, Mari, Sasaki, Hidenao, Kakita, Akiyoshi, Takahashi, Hitoshi, and Wakabayashi, Koichi

Subjects

*MOLECULAR chaperones, *ENDOPLASMIC reticulum, *POLYGLUTAMINE, *MOLECULAR weights

Abstract

The sigma-1 receptor ( SIGMAR1) is now known to be one of the endoplasmic reticulum ( ER) chaperones, which participate in the degradation of misfolded proteins in cells via the ER-related degradation machinery linked to the ubiquitin-proteasome pathway. Mutations of the SIGMAR1 gene are implicated in the pathogenesis of familial frontotemporal lobar degeneration and motor neuron disease. Involvement of ER dysfunction in the formation of inclusion bodies in various neurodegenerative diseases has also become evident. We performed immunohistochemical staining to clarify the localization of SIGMAR1 in the brains of patients with neurodegenerative disorders, including trans-activation response DNA protein 43 ( TDP-43) proteinopathy, tauopathy, α-synucleinopathy, polyglutamine disease and intranuclear inclusion body disease ( INIBD). Double-immunocytofluorescence and Western blot analyses of cultured cells were also performed to investigate the role of SIGMAR1 using a specific exportin 1 inhibitor, leptomycin B and an ER stress inducer, thapsigargin. SIGMAR1 was consistently shown to be co-localized with neuronal nuclear inclusions in TDP-43 proteinopathy, five polyglutamine diseases and INIBD, as well as in intranuclear Marinesco bodies in aged normal controls. Cytoplasmic inclusions in neurons and glial cells were unreactive for SIGMAR1. In cultured cells, immunocytofluorescent study showed that leptomycin B and thapsigargin were shown to sequester SIGMAR1 within the nucleus, acting together with p62. This finding was also supported by immunoblot analysis. These results indicate that SIGMAR1 might shuttle between the nucleus and the cytoplasm. Neurodegenerative diseases characterized by neuronal nuclear inclusions might utilize the ER-related degradation machinery as a common pathway for the degradation of aberrant proteins. [ABSTRACT FROM AUTHOR]

Published

2014

10. TDP-43 pathology in polyglutamine diseases: With reference to amyotrphic lateral sclerosis.

Author

Toyoshima, Yasuko and Takahashi, Hitoshi

Subjects

*POLYGLUTAMINE, *AMYOTROPHIC lateral sclerosis, *NEURODEGENERATION, *NEUROMUSCULAR diseases, *MOTOR neuron diseases

Abstract

A nuclear protein, transactivation response ( TAR) DNA binding protein 43 kDa ( TDP-43), is the major component of neuronal cytoplasmic inclusions ( NCIs) in frontotemporal lobar degeneration with ubiquitin inclusions ( FTLD- U) and sporadic amyotrophic lateral sclerosis ( SALS). While initially thought to be relatively specific to FTLD- U and ALS, TDP-43 pathology has now been detected in a number of other neurodegenerative diseases, including Alzheimer's disease and Parkinson's disease. In such tauopathies and α-synucleinopathies, occurrence of TDP-43-positive neuronal cytoplasmic inclusions may be associated with other distinct molecular pathologic processes primarily involving their own pathological proteins, tau and α-synuclein, respectively (secondary TDP-43 proteinopathies). On the other hand, in several polyglutamine ( polyQ) diseases, TDP-43 appears to play an important pathomechanistic role. Interestingly, intermediate-length polyQ expansions (27-33 Qs) in ataxin 2, the causative gene of spinocerebellar ataxia type 2, have recently been reported to be a genetic risk factor for SALS. Here, with a review of the literature, we discuss the relationship between ALS and polyQ diseases from the viewpoint of TDP-43 neuropathology. [ABSTRACT FROM AUTHOR]

Published

2014

11. Valosin-containing protein immunoreactivity in tauopathies, synucleinopathies, polyglutamine diseases and intranuclear inclusion body disease.

Author

Mori, Fumiaki, Tanji, Kunikazu, Toyoshima, Yasuko, Sasaki, Hidenao, Yoshida, Mari, Kakita, Akiyoshi, Takahashi, Hitoshi, and Wakabayashi, Koichi

Subjects

*PROTEIN genetics, *AMYOTROPHIC lateral sclerosis, *FRONTOTEMPORAL dementia, *NEURODEGENERATION, *POLYGLUTAMINE, *NEUROGLIA, *NEURAL physiology, *PHYSIOLOGY

Abstract

Valosin-containing protein ( VCP) is associated with multiple cellular functions, including ubiquitin-dependent protein degradation. Mutations in VCP are known to cause inclusion body myopathy with Paget's disease and frontotemporal dementia and familial amyotrophic lateral sclerosis ( fALS; ALS14), both of which are characterized by trans-activation response DNA protein 43 ( TDP-43)-positive neuronal cytoplasmic and nuclear inclusions. Recently, immunoreactivity for fALS-associated proteins ( TDP-43, fused in sarcoma ( FUS), optineurin and ubiquilin-2) were reported to be present in cytoplasmic and nuclear inclusions in various neurodegenerative diseases. However, the extent and frequency of VCP-immunoreactive structures in these neurodegenerative diseases are uncertain. We immunohistochemically examined the brains of 72 cases with neurodegenerative diseases and five control cases. VCP immunoreactivity was present in Lewy bodies in Parkinson's disease and dementia with Lewy bodies, and neuronal nuclear inclusions in five polyglutamine diseases and intranuclear inclusion body disease, as well as in Marinesco bodies in aged control subjects. However, other neuronal and glial cytoplasmic inclusions in tauopathies and TDP-43 proteinopathies were unstained. These findings suggest that VCP may have common mechanisms in the formation or degradation of cytoplasmic and nuclear inclusions of neurons, but not of glial cells, in several neurodegenerative conditions. [ABSTRACT FROM AUTHOR]

Published

2013

12. Genistein, a natural product derived from soybeans, ameliorates polyglutamine-mediated motor neuron disease.

Author

Qiang, Qiang, Adachi, Hiroaki, Huang, Zhe, Jiang, Yue‐Mei, Katsuno, Masahisa, Minamiyama, Makoto, Doi, Hideki, Matsumoto, Shinjiro, Kondo, Naohide, Miyazaki, Yu, Iida, Madoka, Tohnai, Genki, and Sobue, Gen

Subjects

*GENISTEIN, *NATURAL products, *SOYBEAN, *POLYGLUTAMINE, *MOTOR neuron diseases, *MUSCULAR atrophy, *ANDROGEN receptors

Abstract

Spinal and bulbar muscular atrophy ( SBMA) is an inherited motor neuron disease caused by the expansion of a polyglutamine (polyQ) tract within the androgen receptor ( AR) gene. The pathologic features of SBMA are motor neuron loss in the spinal cord and brainstem, and diffuse nuclear accumulation and nuclear inclusions of mutant AR in residual motor neurons and certain visceral organs. AR-associated coregulator 70 ( ARA70) was the first coregulator of AR to be identified, and it has been shown to interact with AR and increase its protein stability. Here, we report that genistein, an isoflavone found in soy, disrupts the interaction between AR and ARA70 and promotes the degradation of mutant AR in neuronal cells and transgenic mouse models of SBMA. We also demonstrate that dietary genistein ameliorates behavioral abnormalities, improves spinal cord and muscle pathology, and decreases the amounts of monomeric AR and high-molecular-weight mutant AR protein aggregates in SBMA transgenic mice. Thus, genistein treatment may be a potential therapeutic approach for alleviating the symptoms of SBMA by disrupting the interactions between AR and ARA70. [ABSTRACT FROM AUTHOR]

Published

2013

13. Pharmacological protein targets in polyglutamine diseases: Mutant polypeptides and their interactors.

Author

Margulis, Boris A., Vigont, Vladimir, Lazarev, Vladimir F., Kaznacheyeva, Elena V., and Guzhova, Irina V.

Subjects

*PHARMACOLOGY, *POLYGLUTAMINE, *GENETIC mutation, *POLYPEPTIDES, *PROTEIN-protein interactions, *CEREBRAL atrophy, *NEURONS, *CELL populations

Abstract

Abstract: Polyglutamine diseases are a group of pathologies affecting different parts of the brain and causing dysfunction and atrophy of certain neural cell populations. These diseases stem from mutations in various cellular genes that result in the synthesis of proteins with extended polyglutamine tracts. In particular, this concerns huntingtin, ataxins, and androgen receptor. These mutant proteins can form oligomers, aggregates, and, finally, aggresomes with distinct functions and different degrees of cytotoxicity. In this review, we analyze the effects of different forms of polyQ proteins on other proteins and their functions, which are considered as targets for therapeutic intervention. [Copyright &y& Elsevier]

Published

2013

14. Structure-oriented review of 14-3-3 protein isoforms in geriatric neuroscience.

Author

Umahara, Takahiko, Uchihara, Toshiki, and Iwamoto, Toshihiko

Subjects

*ALZHEIMER'S disease, *ANIMAL experimentation, *APOPTOSIS, *CELL differentiation, *CELLULAR signal transduction, *GERIATRICS, *HUNTINGTON disease, *MOLECULAR biology, *NEURODEGENERATION, *PARKINSON'S disease, *PROTEINS, *RODENTS, *SURVIVAL

Abstract

This review focuses on the possible relevance of 14-3-3 proteins in geriatric neuroscience. 14-3-3 proteins are mainly localized in the synapses and neuronal cytoplasm. These proteins regulate intracellular signal cascades for differentiation, development, growth, apoptosis and survival. Seven isoforms have so far been identified in mammals. The binding motifs and potential functions of 14-3-3 proteins are now recognized to have a wide range of functional relevance. First, we provide a brief summary of the molecular structure and multiple functions of 14-3-3 proteins. Second, we review the involvement of 14-3-3 proteins in common diseases of geriatric neurology, such as Alzheimer's disease and tauopathies, Parkinson's disease and α-synucleinopathies, Huntington's disease and polyglutamine diseases, Creutzfeldt-Jakob disease and prion diseases, cerebral infarction, and atherosclerosis. Finally, we discuss the immunohistochemical localization of 14-3-3 proteins and its isoforms during the postnatal development of rat brains as a basis for understanding adult neurogenesis. The elucidation of the isoform-dependent functions of 14-3-3 proteins with regard to brain development might be promising for the future development of novel therapeutic interventions for common diseases of geriatric neurology. Geriatr Gerontol Int 2012; ••: ••-••. [ABSTRACT FROM AUTHOR]

Published

2012

15. NIRF/UHRF2 occupies a central position in the cell cycle network and allows coupling with the epigenetic landscape

Author

Mori, Tsutomu, Ikeda, Daisuke D., Yamaguchi, Yoshiki, and Unoki, Motoko

Subjects

*CELL cycle, *EPIGENETICS, *CELL physiology, *UBIQUITIN ligases, *TUMOR suppressor genes, *CANCER genes, *GENETIC regulation

Abstract

Abstract: As predicted by systems biology, a paradigm shift will emerge through the integration of information about different layers of cellular processes. The cell cycle network is at the heart of the cellular computing system, and orchestrates versatile cellular functions. The NIRF/UHRF2 ubiquitin ligase is an “intermodular hub” that occupies a central position in the network, and facilitates coordination among the cell cycle machinery, the ubiquitin–proteasome system, and the epigenetic system. NIRF interacts with cyclins, CDKs, p53, pRB, PCNA, HDAC1, DNMTs, G9a, methylated histone H3 lysine 9, and methylated DNA. NIRF ubiquitinates cyclins D1 and E1, and induces G1 arrest. The NIRF gene is frequently lost in tumors and is a candidate tumor suppressor, while its paralog, the UHRF1 gene, is hardly altered. Thus, investigations of NIRF are essential to understand the entire biological systems. Through integration of the enormous information flows, NIRF may contribute to the coupling between the cell cycle network and the epigenetic landscape. We propose the new paradigm that NIRF produces the extreme diversity in the network wiring that helps the diversity of Waddington’s canals. [Copyright &y& Elsevier]

Published

2012

16. Bax-like protein Drob-1 protects neurons from expanded polyglutamine-induced toxicity in Drosophila.

Author

Senoo-Matsuda, Nanami, Igaki, Tatsushi, and Miura, Masayuki

Subjects

*CARRIER proteins, *PROTEINS, *CELL differentiation, *CELL death, *APOPTOSIS, *MITOCHONDRIAL DNA, *NEURODEGENERATION, *NEUROSCIENCES

Abstract

Bcl-2 family proteins regulate cell death through the mitochondrial apoptotic pathway. Here, we show that the Drosophila Bax-like Bcl-2 family protein Drob-1 maintains mitochondrial function to protect cells from neurodegeneration. A pan-neuronal knockdown of Drob-1 results in lower locomotor activity and a shorter lifespan in adult flies. Either the RNAi-mediated downregulation of Drob-1 or overexpression of Drob-1 antagonist Buffy strongly enhances the polyglutamine-induced accumulation of ubiquitinated proteins and subsequent neurodegeneration. Furthermore, ectopic expression of Drob-1 suppresses the neurodegeneration and premature death of flies caused by expanded polyglutamine. Drob-1 knockdown decreases cellular ATP levels, and enhances respiratory inhibitor-induced mitochondrial defects such as loss of membrane potential (Δψm), morphological abnormalities, and reductions in activities of complex I+III and complex II+III, as well as cell death. Taken together, these results suggest that Drob-1 is essential for neuronal cell function, and that Drob-1 protects neurons from expanded polyglutamine-mediated neurodegeneration through the regulation of mitochondrial homeostasis. [ABSTRACT FROM AUTHOR]

Published

2005

17. Caspase-mediated proteolysis of the polyglutamine disease protein ataxin-3.

Author

Berke, Sarah J. Shoesmith, Schmied, Francisca A. Flores, Brunt, Ewout R., Ellerby, Lisa M., and Paulson, Henry L.

Subjects

*ATAXIA, *PROTEOLYSIS, *CELL death, *MUTAGENESIS, *UBIQUITIN, *PROTEINS

Abstract

Spinocerebellar ataxia type-3, also known as Mach- ado-Joseph Disease, is one of many inherited neurodegenerative disorders caused by polyglutamine-encoding GAG repeat expansions in otherwise unrelated disease genes. Polyglutamine disorders are characterized by disease protein misfolding and aggregation; often within the nuclei of affected neurons. Although the precise mechanism of polyglutamine-mediated cell death remains elusive, evidence suggests that proteolysis of polyglutamine disease proteins by caspases contributes to pathogenesis. Using cellular models we now show that the endogenous spinocerebellar ataxia type-3 disease protein, ataxin-3, is proteolyzed in apoptotic paradigms, resulting in the loss of full-length ataxin-3 and the corresponding appearance of an approximately 28-kDa fragment containing the glutamine repeat. Broad-spectrum caspase inhibitors block ataxin-3 proteolysis and studies suggest that caspase-1 is a primary mediator of cleavage. Site-directed mutagenesis experiments eliminating three, six or nine potential caspase cleavage sites in the protein suggest redundancy in the site(s) at which cleavage can occur, as previously described for other disease proteins; but also map a major cleavage event to a cluster of aspartate residues within the ubiquitin-binding domain of ataxin-3 near the poly- glutamine tract. Finally, caspase-mediated cleavage of expanded ataxin-3 resulted in increased ataxin-3 aggregation, suggesting a potential role for caspase-mediated proteolysis in spinocerebellar ataxia type-3 Pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2004

18. Domain architecture of the polyglutamine protein ataxin-3: a globular domain followed by a flexible tail

Author

Masino, Laura, Musi, Valeria, Menon, Rajesh P., Fusi, Paola, Kelly, Geoff, Frenkiel, Thomas A., Trottier, Yvon, and Pastore, Annalisa

Subjects

*ATAXIA, *GLUTAMINE, *CELL death

Abstract

Anomalous expansion of a polyglutamine (polyQ) tract in the protein ataxin-3 causes spinocerebellar ataxia type 3, an autosomal dominant neurodegenerative disease. Very little is known about the structure and the function of ataxin-3, although this information would undoubtedly help to understand why the expanded protein forms insoluble nuclear aggregates and causes neuronal cell death. With the aim of establishing the domain architecture of ataxin-3 and the role of the polyQ tract within the protein context, we have studied the human and murine orthologues using a combination of techniques, which range from limited proteolysis to circular dichroism (CD) and nuclear magnetic resonance (NMR) spectroscopies. The two protein sequences share a highly conserved N-terminus and differ only in the length of the glutamine repeats and in the C-terminus. Our data conclusively indicate that ataxin-3 is composed by a structured N-terminal domain, followed by a flexible tail. Moreover, [15N]glutamine selectively labelled samples allowed us to have a direct insight by NMR into the structure of the polyQ region. [Copyright &y& Elsevier]

Published

2003

19. Dentatorubral-pallidoluysian atrophy (DRPLA) with a small ganglioglioma component containing neurofibrillary tangles and polyglutamine aggregation.

Author

Yamada, Seiji, Yamazaki, Tatsuya, Nakata, Satoshi, Nobusawa, Sumihito, Ikota, Hayato, Ide, Munenori, Mizushima, Kazuyuki, Harigaya, Yasuo, Hirato, Junko, and Yokoo, Hideaki

Subjects

*POLYGLUTAMINE, *CENTRAL nervous system diseases, *AGING, *BRAIN, *AUTOPSY, *PHOSPHORYLATION, *ALZHEIMER'S disease

Abstract

Dentatorubral-pallidoluysian atrophy (DRPLA), one of the polyglutamine diseases, has not been reported in combination with ganglioglioma (GG). Herein, we report an autopsy case of a 72-year-old man with DRPLA with a small GG component harboring neurofibrillary tangles (NFTs) and polyglutamine aggregates. NFTs, cytoplasmic accumulations of hyper-phosphorylated tau, are mainly observed in Alzheimer's disease (AD) and other tau-associated neurodegenerative disorders. NFTs can also be present in normal aging, and are occasionally observed in low-grade central nervous system (CNS) neoplasms such as GG. In the present case, whole brain examination demonstrated widespread deposition of polyglutamine aggregates, including GG, whereas NFTs were restricted to the GG component. In addition, no other AD or aging-related neuropathological structures were detected throughout the CNS. These findings may provide us with clues to elucidate the pathogenetic mechanisms that neuronal neoplasms may have to develop NFTs regardless of aging, and that polyglutamine may accumulate in neoplastic neurons in polyglutamine disease. [ABSTRACT FROM AUTHOR]

Published

2017