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    Progressive Supranuclear Palsy Medical Slides

    Generate publication-quality progressive supranuclear palsy lecture slides in 30 seconds. AI-powered content structured for clinical education.

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    Why teach Progressive Supranuclear Palsy?

    Progressive supranuclear palsy is the most common atypical parkinsonian disorder, with a prevalence of 5-7 per 100,000 and a median survival of 7 years from symptom onset. The 2017 MDS diagnostic criteria defined multiple clinical phenotypes beyond the classic Richardson syndrome. As a primary 4-repeat tauopathy, PSP is a key model for understanding tau-mediated neurodegeneration and a target for emerging anti-tau therapeutic trials.

    Sample Lecture Slides

    What AI generates for Progressive Supranuclear Palsy

    Enter “Progressive Supranuclear Palsy” and SlideCraft generates a complete lecture deck with slides like these.

    01PSP Phenotypes: Richardson Syndrome, PSP-Parkinsonism, PSP-CBS, PSP-FTD, and Others
    02Cardinal Features: Vertical Supranuclear Gaze Palsy and Postural Instability with Early Falls
    032017 MDS Diagnostic Criteria: Core Features, Supportive Features, and Exclusion Criteria
    04Neuropathology: 4-Repeat Tau, Tufted Astrocytes, and Brainstem/Basal Ganglia Predominance
    05MRI Features: Hummingbird Sign (Midbrain Atrophy) and Morning Glory Sign on Axial View
    06Management: Levodopa Trial, Falls Prevention, Dysphagia Management, and Anti-Tau Clinical Trials
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    Progressive Supranuclear Palsy Presentation FAQ

    How should PSP be differentiated from Parkinson disease in teaching?

    Present red flags for PSP over PD: early falls within the first year (backward), vertical supranuclear gaze palsy (initially slow downward saccades), symmetric onset (PD is asymmetric), axial-predominant rigidity (PD is appendicular), poor levodopa response (<30% improvement), frontal-executive cognitive changes early, and pseudobulbar affect. Emphasize that the PSP-Parkinsonism phenotype can initially mimic PD, making longitudinal follow-up and re-evaluation essential.

    What are the characteristic MRI findings and how should they be shown?

    Present two pathognomonic signs: (1) "Hummingbird" or "penguin" sign on midsagittal MRI — midbrain atrophy with preserved pons creating a bird-like silhouette, midbrain AP diameter <9.35 mm, midbrain-to-pons ratio <0.52; (2) "Morning glory" sign on axial view — concavity of the lateral midbrain margin. These have high specificity (>90%) but emerge in advanced disease. SWI sequences showing midbrain T2 hypointensity from iron deposition are an earlier finding.

    How should the multiple PSP phenotypes be organized in teaching?

    Organize by the 2017 MDS criteria phenotypic classification: Richardson syndrome (classic PSP with early vertical gaze palsy and falls), PSP-Parkinsonism (asymmetric, tremor, initial levodopa response — mimics PD), PSP-CBS (corticobasal syndrome with apraxia and cortical sensory loss), PSP-SL (speech/language predominant — progressive non-fluent aphasia), and PSP-FTD (behavioral variant frontotemporal dementia features). This taxonomy helps learners recognize that PSP is broader than the classic Richardson presentation.

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