Cerebellar ataxia in progressive supranuclear palsy: An autopsy study of PSP‐C

Koga, Shunsuke; Josephs, Keith A.; Ogaki, Kotaro; Labbé, Catherine; Uitti, Ryan J.; Graff‐Radford, Neill R.; Gerpen, Jay A. van; Cheshire, William P.; Aoki, Naoya; Rademakers, Rosa; Wszołek, Zbigniew K.; Ross, Owen A.; Dickson, Dennis W.

doi:10.1002/mds.26499

Cited by 62 publications

(36 citation statements)

References 40 publications

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“…In contrast to the ratio of three out of 22 consecutive patients reported in an earlier Japanese study, a recent Western autopsy study identified only 5 PSP-C in 1,085 pathologically confirmed PSP cases, four of which were clinically misdiagnosed as MSA-C. 23 Clinical features of PSP-C were similar to those of MSA-C, but lacking marked dysautonomia sufficient to meet criteria for a clinical diagnosis of MSA. 23 Because PSP-C is difficult to diagnose during life and ataxia is far more often suggestive of other neurodegenerative diseases rather than PSP, this variant is not included in the new MDS PSP criteria.…”

Section: Symptomatic Psp Phenotypesmentioning

confidence: 70%

“…1,14 Other vPSP syndromes named according to their predominant clinical features may account for about one third of earlier presentations in aggregate and include PSP with predominant parkinsonism (PSP-P), 16 pure akinesia with gait freezing (formerly PAGF, now PSP-PGF), 17 corticobasal syndrome (PSP-CBS), 14,18 primary progressive apraxia of speech or non-fluent variant primary progressive aphasia (nfvPPA; when caused by PSP: PSP with predominant speech/language disorder or PSP-SL), 19–21 behavioral variant frontotemporal dementia (bvFTD, when caused by PSP: PSP with predominant frontal presentation or PSP-F), 14,22 and PSP with predominant cerebellar ataxia (PSP-C) (Figure 2). 23 …”

Section: The Clinical Spectrum Of Pspmentioning

confidence: 99%

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Advances in progressive supranuclear palsy: new diagnostic criteria, biomarkers, and therapeutic approaches

Boxer

Golbe

et al. 2017

The Lancet Neurology

326

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Progressive supranuclear palsy (PSP), once simply considered a common cause of atypical parkinsonism is now recognized as a spectrum of motor and behavioral syndromes associated with a specific four repeat (4R) tau neuropathology at autopsy. There are currently no effective treatments for PSP, but because PSP is strongly linked biochemically and genetically to tau protein abnormalities, there is a growing interest in pursuing clinical trials of new tau-directed therapies for this disorder. Such new tau therapies are envisioned to have disease-modifying effects by reducing brain levels of toxic forms of tau or compensating for loss of tau function. To be most effective, these treatments will need to be initiated at early stages of disease. New research criteria that recognize early forms of PSP and operationalize diagnosis of the full spectrum of clinical phenotypes have recently been published. These criteria and new clinical trial designs have benefited from rapid advances in MRI, physiological and fluid biomarker development for PSP. As tau pathology is also central to Alzheimer’s disease and chronic traumatic encephalopathy, it is believed that a successful tau therapeutic for PSP would inform the treatment of other neurodegenerative diseases.

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Section: Symptomatic Psp Phenotypesmentioning

confidence: 70%

Section: The Clinical Spectrum Of Pspmentioning

confidence: 99%

Advances in progressive supranuclear palsy: new diagnostic criteria, biomarkers, and therapeutic approaches

Boxer

Golbe

et al. 2017

The Lancet Neurology

326

292

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“…Immunohistochemistry for phospho‐tau (CP13, 1:1000, from Dr. Peter Davies, Feinstein Institute, North Shore Hospital, NY) was used to establish neuropathological diagnosis of PSP . The regional tau burden, including pretangles/NFT, coiled bodies, tufted astrocytes, and tau‐positive threads, was graded semiquantitatively on a 4‐point scale (0 = absent, 1 = sparse, 2 = moderate, and 3 = frequent) . Select sections were processed for Gallyas silver stain and immunohistochemistry for 4‐repeat tau (RD4, 1:5,000; Millipore, Temecula, CA) to assist in neuropathological diagnosis of AGD .…”

Section: Methodsmentioning

confidence: 99%

“…We assessed clinical information in all PSP‐TDP cases and a subset of TDP‐43‐negative PSP cases (N = 88). The latter group was described as the Mayo Clinic patient series in our previous reports . Ante‐mortem clinical information for age at onset, clinical diagnosis, cognitive impairment, the last available Mini–Mental State Examination (MMSE) scores, and the duration between MMSE performed and death were gathered from clinical reports and/or a brain bank questionnaire filled out by a close family member.…”

Section: Methodsmentioning

confidence: 99%

Distribution and characteristics of transactive response DNA binding protein 43 kDa pathology in progressive supranuclear palsy

et al. 2016

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Introduction This study aimed to determine the frequency of transactive response DNA binding protein 43 kDa (TDP-43) pathology in PSP, the clinical features of patients with this pathology, and genetic risk factors for it.. Methods Hippocampal sections were screened with immunohistochemistry for TDP-43 in 945 PSP cases. A subset of 261 cases that were negative in hippocampus was screened in the amygdala. The density and disruption of this pathology, as well as regional tau burden, and clinical and genetic characteristics were analyzed. Results We observed TDP-43pathology in 47 cases in the hippocampus and an additional 9 cases that only affected the amygdala. Hippocampal sclerosis was the strongest risk factor, followed by Alzheimer’s disease pathology, argyrophilic grain disease, and older age at death. Five stages of TDP-43 pathology were identified in PSP: Stage A had pathology only in the amygdala (16%); stage I had pathology confined to the hippocampus and entorhinal cortex (9%); stage II included both regions of stage A and I (38%); stage III spread further to medial occipitotemporal gyrus (20%); and stage IV had pathology in the dorsolateral frontal lobe (18%). Anatomical areas vulnerable to PSP pathology had varying degrees of this pathology in stage II and later. PSP with TDP-43pathology were older at disease onset and had lower median MMSE scores; however, the latter was driven by concurrent pathologies. Conclusions Distribution and clinical characteristics of TDP-43pathology in PSP were influenced by concurrent pathologies. This is the first study to observe that PSP-vulnerable regions are also susceptible to this non-tau pathology.

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“…Morris et al described patients with PSP who resembled idiopathic Parkinson's disease (PSP‐P) . Other PSP variants/phenotypes with a predominantly subcortical burden of tau pathology have been recognized and include primary progressive freezing of gait (PGF), PSP with postural instability, and PSP with predominant cerebellar ataxia . Recognition of these diverse phenotypes in autopsy‐proven cohorts led to the development of the International Parkinson and Movement Disorder Society (MDS) criteria for diagnosis of PSP (Supplementary Table 1).…”

mentioning

confidence: 99%

Sensitivity and Specificity of Diagnostic Criteria for Progressive Supranuclear Palsy

et al. 2019

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Background: In 2017, the Movement Disorders Society put forward new clinical criteria for the diagnosis of PSP recognizing diverse PSP phenotypes. Objectives: In this study, we compare the sensitivity and specificity of the new criteria to the National Institutes of Neurological Disease and Society for Progressive Supranuclear Palsy (NINDS-SPSP) criteria at different time points. Methods: Patients with clinical parkinsonism, clinical and/or neuropathological diagnosis of PSP were identified from the Society for Progressive Supranuclear Palsy (SPSP) brain bank. All patients had neuropathologic diagnoses and detailed clinical examination performed by a neurologist at one of the three Mayo Clinic sites located in Florida, Arizona and Minnesota. Clinical symptoms and signs were abstracted retrospectively in a blinded fashion and used to determine whether or not patients met either diagnostic criterion. Patients were divided into early and late disease stage groups using a 3-year cut off. Results: A total of 129 patients were included of which 66 (51%) had PSP pathology. The remainder had other neurodegenerative diseases. The overall sensitivity of the Movement Disorders Society criteria was 87.9% compared to 45.5% for National Institutes of Neurological Disease and Society for Progressive Supranuclear Palsy criteria, whereas the specificity of the Movement Disorders Society criteria probable PSP criteria was 85.7% and 90.5% for National Institutes of Neurological Disease criteria. Individual patients were noted to have features of multiple PSP phenotypes. Conclusion: The Movement Disorders Society criteria recognize several phenotypes of PSP and hence have a higher sensitivity than the previous criteria.

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Cerebellar ataxia in progressive supranuclear palsy: An autopsy study of PSP‐C

Cited by 62 publications

References 40 publications

Advances in progressive supranuclear palsy: new diagnostic criteria, biomarkers, and therapeutic approaches

Advances in progressive supranuclear palsy: new diagnostic criteria, biomarkers, and therapeutic approaches

Distribution and characteristics of transactive response DNA binding protein 43 kDa pathology in progressive supranuclear palsy

Sensitivity and Specificity of Diagnostic Criteria for Progressive Supranuclear Palsy

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