Relocation of p25¿/tubulin polymerization promoting protein from the nucleus to the perinuclear cytoplasm in the oligodendroglia of sporadic and COQ2 mutant multiple system atrophy

Ota, Katsuya; Obayashi, Masato; Ozaki, Kokoro; Ichinose, Shizuko; Kakita, Akiyoshi; Tada, Mari; Takahashi, Hitoshi; Ando, Noboru; Eishi, Yoshinobu; Mizusawa, Hidehiro; Ishikawa, Kinya

doi:10.1186/preaccept-3606739711332434

Cited by 16 publications

(21 citation statements)

References 35 publications

(61 reference statements)

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“…In addition, both TPPP/p25 [15] and SYN [60] were detected in the cerebrospinal fluid of human patients. Extracellular transmission of these proteins, therefore, is a plausible explanation for the development of pathological inclusions in the case of Parkinson's disease and multiple system atrophy [16,61,62].…”

Section: Discussionmentioning

confidence: 99%

“…Targeting by competitors/foldamers should impede/destruct the small soluble assemblies, the fatal species in the development of synucleinopathies. The pathological complex has been suggested functioning as an initiator in the etiology of Parkinson's disease and multiple system atrophy [16][17][18]61,62]. We explored the challenges associated with targeting chameleon proteins using the TPPP/p25-SYN complex as a case study.…”

Section: Discussionmentioning

confidence: 99%

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Challenging drug target for Parkinson's disease: Pathological complex of the chameleon TPPP/p25 and alpha-synuclein proteins

Szénási¹,

Oláh²,

Szabó³

et al. 2017

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

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The hallmarks of Parkinson's disease and other synucleinopathies, Tubulin Polymerization Promoting Protein (TPPP/p25) and α-synuclein (SYN) have two key features: they are disordered and co-enriched/co-localized in brain inclusions. These Neomorphic Moonlighting Proteins display both physiological and pathological functions due to their interactions with distinct partners. To achieve the selective targeting of the pathological TPPP/p25-SYN but not the physiological TPPP/ p25-tubulin complex, their interfaces were identified as a specific innovative strategy for the development of anti-Parkinson drugs. Therefore, the interactions of TPPP/p25 with tubulin and SYN were characterized which suggested the involvements of the 178-187 aa and 147-156 aa segments in the complexation of TPPP/p25 with tubulin and SYN, respectively. However, various truncated and deletion mutants reduced but did not abolish the interactions except one mutant; in addition synthetized fragments corresponding to the potential binding segments of TPPP/p25 failed to interact with SYN. In fact, the studies of the multiple interactions at molecular and cellular levels revealed the high conformational plasticity, chameleon feature, of TPPP/p25 that ensures exceptional functional resilience; the lack of previously identified binding segments could be replaced by other segments. The experimental results are underlined by distinct bioinformatics tools. All these data revealed that although targeting chameleon proteins is a challenging task, nevertheless, the validation of a drug target can be achieved by identifying the interface of complexes of the partner proteins existing at the given pathological conditions.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Challenging drug target for Parkinson's disease: Pathological complex of the chameleon TPPP/p25 and alpha-synuclein proteins

Szénási¹,

Oláh²,

Szabó³

et al. 2017

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

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“…In the rostral pons of MSA patients, significant changes in the expression of 254 genes were found, some similar to those in substantia nigra (SN) of patients with PD and others related to oligodendroglial function . Functionally impaired variants of parahydroxybenzoate‐polyprenyltransferase (COQ2) as a risk factor for MSA found in a Japanese family carrying homozygous mutations in the coenzyme Q2 gene (COQ2) have not been confirmed by others, and no association of glucosidase‐β‐acid (GBA) mutations and MSA, and no c9orf72 expansions have been found . An autosomal dominant inheritance within a German MSA family was reported .…”

Section: Comparisons Of Clinical and Neuropathologic And Subtypes Of Msamentioning

confidence: 99%

Neuropathology of multiple system atrophy: New thoughts about pathogenesis

Jellinger¹

2014

Movement Disorders

154

135

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Multiple system atrophy (MSA) is a fatal adult-onset neurodegenerative disorder of uncertain etiology, clinically manifesting with autonomic failure associated with parkinsonism, cerebellar dysfunction, and pyramidal signs in variable combination. The pathological process affects central autonomic, striatonigral, and olivopontocerebellar systems. These show varying degrees of neurodegeneration and underlie the stratification of the heterogenous disorder into MSA-P and MSA-C clinical variants, which correlate to the morphologic phenotypes of striatonigral degeneration and olivopontocerebellar atrophy (MSA-C). The lesions are not limited to these most consistently and severely affected systems but may involve many other parts of the central, peripheral, and autonomic nervous systems, underpinning the multisystem character of MSA. The histological core feature are glial cytoplasmic inclusions (GCIs, Papp-Lantos bodies) in all types of oligodendroglia that contain aggregates of misfolded α-Synuclein (α-Syn). In addition to the ectopic appearance of α-Syn in oligodendrocytes and other cells, oxidative stress, proteasomal and mitochondrial dysfunction, excitotoxiciy, neuroinflammation, metabolic changes, and energy failure are important contributors to the pathogenesis of MSA, as shown by various neurotoxic and transgenic animal models. Although the basic mechanisms of α-Syn-triggered neurodegeneration are not completely understood, neuron-to-oligodendrocyte transfer of α-Syn by prion-like spreading, inducing oligodendroglial and myelin dysfunction associated with chronic neuroinflammation, are suggested finally to lead to a system-specific pattern of neurodegeneration.

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“…The assembly of the unstructured SYN and TPPP/ p25 appears to be pathogenic leading to the etiology of synucleinopathies [99,103,104,107]. Indeed, their coenrichment and co-localization has been detected in both neurons and OLGs in the cases of PD and MSA, respectively, [99,103,104,107] (Fig.…”

Section: Design and Development Of Antiparkinson Medicationmentioning

confidence: 97%

“…TPPP/p25 and SYN co-localize and are co-enriched in both neurons and OLGs in PD and MSA, respectively (Fig. 2) [99,[103][104][105][106][107][108]. In OLG cell models of MSA that involve TPPP/p25 and SYN overexpression, TPPP/p25-induced SYN aggregation was detected [79,109].…”

Section: Tppp/p25: the New Hallmark Of Parkinsonismmentioning

confidence: 99%

Pharmacological targeting of α‐synuclein and TPPP/p25 in Parkinson's disease: challenges and opportunities in a Nutshell

Oláh

Ovádi

2019

FEBS Letters

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With the aging of population, neurological disorders, and especially disorders involving defects in protein conformation (also known as proteopathies) pose a serious socio‐economic problem. So far there is no effective treatment for most proteopathies, including Parkinson's disease (PD). The mechanism underlying PD pathogenesis is largely unknown, and the hallmark proteins, α‐synuclein (SYN) and tubulin polymerization promoting protein (TPPP/p25) are challenging drug targets. These proteins are intrinsically disordered with high conformational plasticity, and have diverse physiological and pathological functions. In the healthy brain, SYN and TPPP/p25 occur in neurons and oligodendrocytes, respectively; however, in PD and multiple system atrophy, they are co‐enriched and co‐localized in both cell types, thereby marking pathogenesis. Although large inclusions appear at a late disease stage, small, soluble assemblies of SYN promoted by TPPP/p25 are pathogenic. In the light of these issues, we established a new innovative strategy for the validation of a specific drug target based upon the identification of contact surfaces of the pathological SYN‐TPPP/p25 complex that may lead to the development of peptidomimetic foldamers suitable for pharmaceutical intervention.

show abstract

Relocation of p25¿/tubulin polymerization promoting protein from the nucleus to the perinuclear cytoplasm in the oligodendroglia of sporadic and COQ2 mutant multiple system atrophy

Cited by 16 publications

References 35 publications

Challenging drug target for Parkinson's disease: Pathological complex of the chameleon TPPP/p25 and alpha-synuclein proteins

Challenging drug target for Parkinson's disease: Pathological complex of the chameleon TPPP/p25 and alpha-synuclein proteins

Neuropathology of multiple system atrophy: New thoughts about pathogenesis

Pharmacological targeting of α‐synuclein and TPPP/p25 in Parkinson's disease: challenges and opportunities in a Nutshell

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