Your search keyword '"Misawa, Sonoko"' showing total 13 results

1. Chronic Inflammatory Demyelinating Polyneuropathy

Author

Kuwabara, Satoshi, Misawa, Sonoko, Crusio, Wim E., Series Editor, Lambris, John D., Series Editor, Rezaei, Nima, Series Editor, Sango, Kazunori, editor, Yamauchi, Junji, editor, Ogata, Toru, editor, and Susuki, Keiichiro, editor

Published

2019

2. Membrane property changes in most distal motor axons in chronic inflammatory demyelinating polyneuropathy.

Author

Amino, Hiroshi, Shibuya, Kazumoto, Misawa, Sonoko, Sekiguchi, Yukari, Beppu, Minako, Suichi, Tomoki, Suzuki, Yo‐ichi, Tsuneyama, Atsuko, Kuwabara, Satoshi, and Suzuki, Yo-Ichi

Subjects

ELECTRODIAGNOSIS, RESEARCH, NEURONS, DEMYELINATION, RESEARCH methodology, EVALUATION research, MEDICAL cooperation, NEURAL conduction, COMPARATIVE studies, GUILLAIN-Barre syndrome, ULNAR nerve, ELECTRIC stimulation, RESEARCH funding, MOTOR neurons, WRIST

Abstract

Introduction: Distal nerve terminals, where the blood-nerve barrier is anatomically deficient, are preferentially affected in immune-mediated neuropathies. Excitability alterations near the motor nerve terminals may be more prominent than the nerve trunk in typical chronic inflammatory demyelinating polyneuropathy (CIDP).Methods: In 20 patients with typical CIDP, motor nerve excitability testing was performed at the motor point and wrist of the ulnar nerve, and results were compared with those in 20 healthy persons.Results: Chronic inflammatory demyelinating polyneuropathy patients showed greater threshold changes in hyperpolarizing threshold electrotonus at the motor point (P < .05) but not at the wrist. Strength-duration time constant did not show significant differences between CIDP and controls at both sites.Discussion: Axonal property changes in CIDP are more prominent in distal portions of axons compared with the nerve trunk, presumably due to salient demyelination near the distal nerve terminals. Motor point excitability measurements could elucidate underlying pathophysiology in immune-mediated neuropathies. [ABSTRACT FROM AUTHOR]

Published

2020

3. Chronic inflammatory demyelinating polyneuropathy: The spectrum and immunopathogenesis deciphered by electrophysiology and neuroimaging.

Author

Kuwabara, Satoshi, Misawa, Sonoko, and Mori, Masahiro

Subjects

*ELECTROPHYSIOLOGY, *POLYNEUROPATHIES, *BRAIN imaging, *PHENOTYPES, *DEMYELINATION, *SPECTRUM analysis

Abstract

Abstract: Chronic inflammatory demyelinating polyneuropathy (CIDP) is a heterogeneous disorder having a wide range of clinical phenotypes, and is currently classified into “typical CIDP” and variants, such as multifocal acquired demyelinating sensory and motor neuropathy. Typical CIDP is clinically characterized by symmetric polyneuropathy involving proximal as well as distal muscle weakness, whereas electrophysiology shows evidence of demyelination predominant in the distal nerve terminals, and magnetic resonance neurography frequently shows prominent hypertrophy of the nerve roots. The pattern of demyelination distribution strongly suggests primary involvement of the nerve terminals and roots, where the blood–nerve barrier is anatomically deficient, and the importance of an antibody‐mediated mechanism. In contrast, multifocal acquired demyelinating sensory and motor neuropathy is multiple mononeuropathy or asymmetric polyneuropathy with multifocal conduction blocks and focal nerve enlargement in the intermediate nerve trunks at the site of conduction block; such distribution of lesions is reasonably explained by breakdown of the blood–nerve barrier by activated lymphocytes, suggesting a multiple sclerosis‐like cellular mechanism. Clinical features are likely to be determined by the immunopathogenesis, and therefore different immunological treatment would be required for each CIDP subtype. The present review focuses on current concepts of the disease spectrum of “CIDP syndrome” deciphered by electrophysiology and neuroimaging. [ABSTRACT FROM AUTHOR]

Published

2018

4. Different electrophysiological profiles and treatment response in 'typical' and 'atypical' chronic inflammatory demyelinating polyneuropathy.

Author

Satoshi Kuwabara, Sagiri Isose, Masahiro Mori, Satsuki Mitsuma, Setsu Sawai, Minako Beppu, Yukari Sekiguchi, Sonoko Misawa, Kuwabara, Satoshi, Isose, Sagiri, Mori, Masahiro, Mitsuma, Satsuki, Sawai, Setsu, Beppu, Minako, Sekiguchi, Yukari, and Misawa, Sonoko

Subjects

ELECTROPHYSIOLOGY, NEUROPATHY, INFLAMMATION, DATA analysis, DEMYELINATION, KAPLAN-Meier estimator, PLASMAPHERESIS, IMMUNOGLOBULINS, THERAPEUTIC use of immunoglobulins, TREATMENT of Guillain-Barre syndrome, ADRENOCORTICAL hormones, COMPARATIVE studies, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, NEURAL conduction, GUILLAIN-Barre syndrome, PROGNOSIS, RESEARCH, TIBIAL nerve, EVALUATION research, TREATMENT effectiveness, THERAPEUTICS

Abstract

Background: Chronic inflammatory demyelinating polyneuropathy (CIDP) is currently classified into 'typical' CIDP and 'atypical' subtypes such as multifocal acquired demyelinating sensory and motor neuropathy (MADSAM).Objectives: To assess the frequency of CIDP subtypes, and to elucidate clinical and electrophysiological features, and treatment response in each subtype.Methods: We reviewed data from 100 consecutive patients fulfilling criteria for CIDP proposed by the European Federation of Neurological Societies and the Peripheral Nerve Society. The Kaplan-Meier curve was used to estimate long-term outcome.Results: Patients were classified as having typical CIDP (60%), MADSAM (34%), demyelinating acquired distal symmetric neuropathy (8%) or pure sensory CIDP (1%). Compared with patients with MADSAM, patients with typical CIDP showed more rapid progression and severe disability, and demyelination predominant in the distal nerve segments. MADSAM was characterised by multifocal demyelination in the nerve trunks. Abnormal median-normal sural sensory responses were more frequently found for typical CIDP (53% vs 13%). Patients with typical CIDP invariably responded to corticosteroids, immunoglobulin or plasmapheresis, whereas patients with MADSAM were more refractory to these treatments. The Kaplan-Meier analyses showed that 64% of patients with typical CIDP and 41% of patients with MADSAM had a clinical remission 5 years later (p=0.02).Conclusions: Among the CIDP spectrum, typical CIDP and MADSAM are the major subtypes, and their pathophysiology appears to be distinct. In typical CIDP, the distal nerve terminals and possibly the nerve roots, where the blood-nerve barrier is anatomically deficient, are preferentially affected, raising the possibility of antibody-mediated demyelination, whereas cellular immunity with breakdown of the barrier may be important in MADSAM neuropathy. [ABSTRACT FROM AUTHOR]

Published

2015

5. Severity and Patterns of Blood-Nerve Barrier Breakdown in Patients with Chronic Inflammatory Demyelinating Polyradiculoneuropathy: Correlations with Clinical Subtypes.

Author

Shimizu, Fumitaka, Sawai, Setsu, Sano, Yasuteru, Beppu, Minako, Misawa, Sonoko, Nishihara, Hideaki, Koga, Michiaki, Kuwabara, Satoshi, and Kanda, Takashi

Subjects

BLOOD-brain barrier disorders, SEVERITY of illness index, INFLAMMATION, DEMYELINATION, POLYRADICULOPATHY, NEUROPATHY, TIGHT junctions

Abstract

Objective: Chronic inflammatory demyelinating polyradiculoneuropathy (CIDP) is currently classified into clinical subtypes, including typical and atypical forms (multifocal acquired demyelinating sensory and motor neuropathy (MADSAM) and distal acquired demyelinating symmetric neuropathy (DADS)). The aim of this study was to elucidate the patterns and severity of breakdown of the blood-nerve barrier (BNB) in each CIDP subtype. Methods: We evaluated the effects of sera obtained from patients with typical CIDP, MADSAM and DADS and control subjects on the expression levels of tight junction proteins and transendothelial electrical resistance (TEER) value in human peripheral nerve microvascular endothelial cells (PnMECs). Results: The sera obtained from the patients with the three clinical phenotypes of CIDP decreased the amount of claudin-5 protein levels and TEER values in the PnMECs. In addition, the sera obtained from typical CIDP patients more prominently reduced claudin-5 protein levels and TEER values in the PnMECs than did that obtained from the MADSAM and DADS patients. Furthermore, the severity of BNB disruption after exposure to the sera was associated with higher Hughes grade, lower MRC score, more pronounced slowing of motor nerve conduction in the median nerve and higher frequency of abnormal temporal dispersion. Conclusions: Sera derived from typical CIDP patients destroy the BNB more severely than those from MADSAM or DADS patients. The extent of BNB disruption in the setting of CIDP is associated with clinical disability and demyelination in the nerve trunk. These observations may explain the phenotypical differences between CIDP subtypes. [ABSTRACT FROM AUTHOR]

Published

2014

6. Different neurological and physiological profiles in POEMS syndrome and chronic inflammatory demyelinating polyneuropathy.

Author

Nasu, Saiko, Misawa, Sonoko, Sekiguchi, Yukari, Shibuya, Kazumoto, Kanai, Kazuaki, Fujimaki, Yumi, Ohmori, Shigeki, Mitsuma, Satsuki, Koga, Shunsuke, and Kuwabara, Satoshi

Subjects

*POEMS syndrome, *NEUROLOGY, *NEUROPATHY, *ELECTROPHYSIOLOGY, *DEMYELINATION, *DEVELOPMENTAL biology, *AUTOIMMUNE diseases

Abstract

Background POEMS (polyneuropathy, organomegaly, endocrinopathy, M protein and skin changes) syndrome, a rare cause of demyelinating neuropathy associated with multiorgan involvement, has been increasingly recognised. Polyneuropathy is often an initial manifestation and therefore the disorder can be misdiagnosed as chronic inflammatory demyelinating polyneuropathy (CIDP). Objective To elucidate whether POEMS syndrome and CIDP are differentiated based on profiles of neuropathy Methods Clinical and electrophysiological data were reviewed in consecutive POEMS syndrome (n¼51) and typical CIDP (n¼46) patients in a single Japanese hospital between 2000 and 2010 Results Both POEMS and CIDP patients showed symmetric polyneuropathy, physiological evidence of demyelination (70% of POEMS patients fulfilled the electrodiagnostic criteria for definite CIDP) and albuminocytological dissociation; 49% of the POEMS syndrome patients had neuropathy onset and 60% of them were initially diagnosed as having CIDP by neurologists. Clinically, POEMS neuropathy more frequently showed severe leg pain (76% vs 7%; p<0.001), muscle atrophy (52% vs 24%; p¼0.005) and distal dominant muscle weakness. Electrophysiologically, POEMS syndrome was characterised by less prolonged distal motor latency (mean 5.6 ms vs 8.1 ms; p<0.001) and higher terminal latency index (0.42 vs 0.33; p¼0.006) in the median nerves, and unrecordable tibial and sural responses (p<0.001), suggesting demyelination predominant in the nerve trunk rather than in the distal nerve terminals, and axonal loss in the lower limb nerves. Conclusions Before development of typical systemic manifestations, POEMS neuropathy can be distinguished from CIDP by the clinical profile and patterns of nerve conduction abnormalities. Recognition of these features leads to early diagnosis and proper treatment for POEMS syndrome. [ABSTRACT FROM AUTHOR]

Published

2012

7. Utility of the distal compound muscle action potential duration for diagnosis of demyelinating neuropathies.

Author

Isose, Sagiri, Kuwabara, Satoshi, Kokubun, Norito, Sato, Yasunori, Mori, Masahiro, Shibuya, Kazumoto, Sekiguchi, Yukari, Nasu, Saiko, Fujimaki, Yumi, Noto, Yuichi, Sawai, Setsu, Kanai, Kazuaki, Hirata, Koichi, and Misawa, Sonoko

Subjects

DEMYELINATION, ACTION potentials, NEUROPATHY, AMYOTROPHIC lateral sclerosis, DIABETIC neuropathies, RECEIVER operating characteristic curves, PATIENTS, THERAPEUTICS

Abstract

To assess the significance of distal compound muscle action potential (CMAP) duration for diagnosis of demyelinating neuropathies, electrophysiologic data were reviewed from 471 subjects, including 145 normal controls, 60 patients with chronic inflammatory demyelinating polyneuropathy (CIDP), 205 with other neuropathy, and 61 with amyotrophic lateral sclerosis (ALS). The duration of distally evoked CMAP was measured in the median, ulnar, tibial, and peroneal nerves. Optimal cut-off values were calculated with receiver-operating characteristic (ROC) curves. In comparison of normal controls and CIDP patients, ROC analyses showed the sufficient area under the curves (82-93%). When the cut-off values in the detection of demyelination were determined as the point with 98% specificity vs. normal on the ROC curves (median, 6.6 ms; ulnar, 6.7 ms; peroneal, 7.6 ms; tibial, 8.8 ms), the sensitivity was 77% for CIDP, with a specificity of 90% vs. ALS and 95% vs. diabetic neuropathy. The distal CMAP duration is a useful index for the detection of distal demyelination. We suggest the above cut-off values for each nerve as one of the electrodiagnostic criteria for demyelinating neuropathies, preferentially affecting the distal nerve terminals, such as CIDP. [ABSTRACT FROM AUTHOR]

Published

2009

8. Sensory Nerve Conduction in Demyelinating and Axonal Guillain-Barré Syndromes.

Author

Kuwabara, Satoshi, Ogawara, Kazue, Misawa, Sonoko, Mizobuchi, Keiko, Sung, Jia-Ying, Kitano, Yukiko, Mori, Masahiro, and Hattori, Takamichi

Subjects

NEURAL conduction, AXONS, DEMYELINATION, ULNAR nerve, ELECTRODIAGNOSIS, NEUROPATHY

Abstract

Guillain-Barré syndrome is divided into acute inflammatory demyelinating polyneuropathy (AIDP) and acute motor axonal neuropathy (AMAN) based on motor nerve conduction studies. We investigated whether sensory nerve conduction studies contribute to the electrodiagnosis of AIDP and AMAN. In consecutive 59 patients with AIDP (n = 26) or AMAN (n = 33), results of sensory nerve conduction studies in the median, ulnar and sural nerves were reviewed. Sensory nerve conduction abnormalities were found for 85% of AIDP patients and for only 6% of AMAN patients. In AIDP patients, the abnormalities were present in 85% of patients in the median nerves, 85% in the ulnar nerves and 38% in the sural nerves. AMAN is very rarely associated with sensory nerve involvement. Abnormal sensory nerve conduction is supportive of AIDP and is more frequently found for the median and ulnar nerves than sural nerves. Copyright © 2004 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2004

9. Serum cytokine and chemokine profiles in patients with chronic inflammatory demyelinating polyneuropathy.

Author

Beppu, Minako, Sawai, Setsu, Misawa, Sonoko, Sogawa, Kazuyuki, Mori, Masahiro, Ishige, Takayuki, Satoh, Mamoru, Nomura, Fumio, and Kuwabara, Satoshi

Subjects

*CYTOKINES, *CHEMOKINES, *INFLAMMATION, *DEMYELINATION, *NEUROPATHY, *BLOOD serum analysis, *PATIENTS

Abstract

To identify serum cytokine networks specific to chronic inflammatory demyelinating polyneuropathy (CIDP), serum samples of two subgroups (18 patients with typical CIDP and 12 patients with multifocal acquired demyelinating sensory and motor neuropathy [MADSAM]) were analyzed with multiplex magnetic bead-based cytokine assay. TNF-α, HGF, MIP-1β and IL-1β levels were significantly higher in total CIDP patients than in normal controls. Of these, HGF levels were elevated in typical CIDP patients, but not in MADSAM patients. Patients with high HGF levels showed good responses to steroid treatment. Different cytokine profiles among the CIDP subtypes presumably reflect differences in pathophysiology. [ABSTRACT FROM AUTHOR]

Published

2015

10. Superficial radial sensory nerve potentials in immune-mediated and diabetic neuropathies

Author

Tamura, Noriko, Kuwabara, Satoshi, Misawa, Sonoko, Mori, Masahiro, Nakata, Miho, and Hattori, Takamichi

Subjects

*NEUROPATHY, *DEMYELINATION, *DIABETIC neuropathies, *DIABETES complications, *NEUROLOGICAL disorders

Abstract

Abstract: Objective: The pattern of abnormal median-normal sural sensory nerve action potential (SNAP) is frequently found in acute/chronic inflammatory demyelinating polyneuropathy (AIDP/CIDP), whereas sural/radial SNAP amplitude ratio is sensitive to detect dying-back degeneration. To investigate whether radial SNAP and its amplitude ratio to median or sural SNAP provide additional particular patterns of sensory nerve involvement. Methods: Superficial radial, median, and sural SNAPs were recorded in 63 normal subjects and in 132 patients with AIDP/CIDP (n=22), diabetic neuropathy (n=83), or other axonal polyneuropathy (n=27). Median/radial and sural/radial amplitude ratios were examined. Results: In normal subjects, median/radial ratio was 0.96±0.05 (mean±SEM), and sural/radial ratio was 0.50±0.03. Compared with normal controls, the median/radial ratio was lower in patients with AIDP/CIDP (0.64±0.11; P&#60;0.001) or diabetic neuropathy (0.75±0.04; P=0.08), but similar in those with other neuropathy (0.94±0.10). The sural/radial ratio was higher in the AIDP/CIDP group (0.71±0.08; P=0.10), and lower in the diabetic (0.36±0.03; P&#60;0.001) and other axonal neuropathy groups (0.40±0.07; P=0.08). Conclusions: AIDP/CIDP is associated with a reduced median/radial ratio and increased sural/radial ratio, probably reflecting demyelination predominant in the distal nerve terminals. Diabetic neuropathy is characterized by decreases in both median/radial and sural/radial ratios, presumably due to coexistence of carpal tunnel pathology and dying-back degeneration. Significance: Comparison of multiple SNAP amplitudes provides information about characteristic distribution patterns of sensory nerve involvement in peripheral neuropathies. [Copyright &y& Elsevier]

Published

2005

11. Different distribution of demyelination in chronic inflammatory demyelinating polyneuropathy subtypes.

Author

Shibuya, Kazumoto, Tsuneyama, Atsuko, Misawa, Sonoko, Sekiguchi, Yukari, Beppu, Minako, Suichi, Tomoki, Suzuki, Yo-ichi, Nakamura, Keigo, Kano, Hiroki, and Kuwabara, Satoshi

Subjects

*CHRONIC inflammatory demyelinating polyradiculoneuropathy, *DEMYELINATION, *MOTOR neuron diseases, *ULNAR nerve, *NERVE endings, *MEDIAN nerve

Abstract

In demyelinating polyneuropathies, distribution patterns of demyelination reflect underlying pathogenesis. Median and ulnar nerve conduction studies were reviewed in 85 typical chronic inflammatory demyelinating polyneuropathy (CIDP) patients and 29 multifocal acquired demyelinating sensory and motor neuropathy (MADSAM). Distal latencies were prolonged in typical CIDP and near normal in MADSAM. Abnormal amplitude reductions in the nerve trunks were more frequent in MADSAM than typical CIDP. Presumably because the blood-nerve barrier is anatomically deficient at the distal nerve terminals, antibody-mediated demyelination is a major pathophysiology in typical CIDP. In contrast, blood-nerve barrier breakdown is likely to be predominant in MADSAM. Unlabelled Image • A total of 136 CIDP patients was included and classified, based on clinical subtypes. • The distribution pattern of demyelination in each subtype was investigated. • Demyelination patterns were different and may reflect underlying pathophysiology. [ABSTRACT FROM AUTHOR]

Published

2020

12. Autoantibodies against vinculin in patients with chronic inflammatory demyelinating polyneuropathy.

Author

Beppu, Minako, Sawai, Setsu, Satoh, Mamoru, Mori, Masahiro, Kazami, Takahiro, Misawa, Sonoko, Shibuya, Kazumoto, Ishibashi, Masumi, Sogawa, Kazuyuki, Kado, Sayaka, Kodera, Yoshio, Nomura, Fumio, and Kuwabara, Satoshi

Subjects

*AUTOANTIBODIES, *VINCULIN, *NEUROPATHY, *DEMYELINATION, *MYELIN sheath, *CELL adhesion, *PATIENTS

Abstract

To identify the target molecules of chronic inflammatory demyelinating polyneuropathy (CIDP), we used proteomic-based approach in the extracted proteins from porcine cauda equina. Two of 31 CIDP patients had markedly elevated serum autoantibodies against vinculin, a cell adhesion protein. Both of the patients with anti-vinculin antibodies had similar clinical manifestation, which are compatible with those of “typical” CIDP. Immunocytochemistry showed that vinculin was stained at the myelin sheath of the sciatic nerves by serum samples. Our results suggest that vinculin is a possible immunological target molecule in a subpopulation of typical CIDP patients. [ABSTRACT FROM AUTHOR]

Published

2015

13. Effects of low frequency filtering on distal compound muscle action potential duration for diagnosis of CIDP: A Japanese–European multicenter prospective study.

Author

Mitsuma, Satsuki, Van den Bergh, Peter, Rajabally, Yusuf A., Van Parijs, Vinciane, Martin-Lamb, Darren, Sonoo, Masahiro, Inaba, Akira, Shimizu, Toshio, Isose, Sagiri, Sato, Yasunori, Komori, Tetsuo, Misawa, Sonoko, and Kuwabara, Satoshi

Subjects

*ACTION potentials, *MUSCLE physiology, *POLYNEUROPATHIES, *JAPANESE people, *EUROPEANS, *DEMYELINATION, *DIAGNOSIS, *DISEASES

Abstract

Objective The duration of the distal compound muscle action potential (DCMAP) is a useful index to detect demyelination in the distal nerve segments. However in published electrodiagnostic criteria for chronic inflammatory demyelinating polyneuropathy (CIDP), the cut-off values of DCMAP duration are defined using an EMG low frequency filter of only 20 Hz. We aimed to provide widely-available reference data using several low cut filters. Methods In 13 Japanese and European tertiary centers, DCMAP duration data using 2, 5, 10, and 20 Hz low frequency filters were prospectively collected from 147 normal controls, 59 patients with typical CIDP, and 100 with diabetic polyneuropathy. Optimal cut-off values were calculated with receiver-operating characteristic curves, offering 100% specificity versus normal controls. Results The higher low frequency filter was associated with significantly shorter DCMAP duration in all groups. For CIDP diagnosis, the calculated cut-off values had a sensitivity ranging from 51% to 66%, and a specificity versus diabetic neuropathy from 96% to 98%. Conclusions Our results show that DCMAP duration is largely dependent on low frequency filter settings, but is a useful index for CIDP diagnosis when the cut-off values are properly determined at each filter setting. Significance Our data provide the systematic reference values of DCMAP duration for CIDP diagnosis available for most EMG laboratories. [ABSTRACT FROM AUTHOR]

Published

2015