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Progressive Supranuclear Palsy - Richardson Syndrome

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Progressive Supranuclear Palsy - Richardson Syndrome

Overview

Progressive supranuclear palsy - Richardson syndrome (PSP-RS), also known as classic PSP or Steele-Richardson-Olszewski syndrome, is the most common phenotypic variant of progressive supranuclear palsy, accounting for approximately 50-55% of all PSP cases. It is characterized by early postural instability, vertical supranuclear gaze palsy, and progressive akinesia[1]. [@williams2005]

Epidemiology

  • Prevalence: 5-6 per 100,000 population[2]
  • Incidence: 0.5-1.0 per 100,000 annually[2]
  • Age of onset: Typically 60-65 years[2]
  • Disease duration: Median 6-9 years[2]
  • No significant gender predominance

Genetics

Risk Factors

  • MAPT H1 haplotype: Strongest genetic risk factor[3]
  • C9orf72 expansions: Occasionally found in PSP-FTD spectrum[3]
  • Familial aggregation: Rare but reported in some families[3]
  • Most cases are sporadic

Associated Genes

| Gene | Variant | Effect | [@litvan1996]
|------|---------|--------| [@hglinger2017]
| MAPT | H1 haplotype | Increased risk | [@dickson2010]
| MAPT | p.P301T | Penetrant PSP | [@steele1964]
| STX6 | rs646776 | Modest risk | [@hglinger2017a]
| EIF2AK3 | rs7447 | Modest risk | [@niccolini2015]

Pathophysiology

Tau Pathology

PSP-RS is a 4-repeat (4R) tauopathy characterized by[4]: [@vale2016]

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