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Does SAPHO syndrome exist in dermatology? | LitMetric

Does SAPHO syndrome exist in dermatology?

J Eur Acad Dermatol Venereol

Department of Dermatology and Allergy, Ludwig-Maximilian-University of Munich, Munich, Germany.

Published: September 2022

AI Article Synopsis

  • * The term SAPHO syndrome was introduced in 1987 to describe a group of inflammatory diseases, including synovitis and pustulosis, but some experts suggest reclassifying it as Sasaki syndrome to better represent specific conditions like PPP without skin issues.
  • * Understanding the pathophysiology of these disorders remains incomplete; expert opinion now favors a more detailed approach using high-throughput sequencing to help dissect

Article Abstract

In the late 1960s, palmoplantar pustulosis (PPP) with sternocostoclavicular arthropathy was first described in Japan, predominantly affecting women in the perimenopausal age. In the 1970s, the chronic non-bacterial osteomyelitis and chronic recurrent multifocal osteomyelitis were initially observed in paediatric patients with approximately 70% girls. Acne fulminans accompanied by polyarthralgia have been observed since early 1970s, which almost exclusively occurs in adolescent boys. Report on spondyloarthropathy associated with hidradenitis suppurativa can be traced back to 1982. The SAPHO syndrome was coined in 1987 to lump together synovitis, acne, pustulosis, hyperostosis and osteitis to conceptualize a group of inflammatory osteocutaneous diseases of unclear etiopathogenesis and ill-defined associations spanning disparate age and gender groups. From historical view, Sasaki syndrome is proposed to replace SAPHO syndrome to represent PPP with sternocostoclavicular arthropathy in the absence of other skin manifestations. Hidradenitis suppurativa is folliculitis in pathogenesis and no longer classified as acne. PPP accompanied by psoriasis vulgaris is more likely psoriasis pustulosa palmoplantaris in dermatological aspect, and the associated arthritis is part of psoriatic arthropathy. Pathophysiology of these disorders is incompletely understood. To echo the advancement of high-throughput sequencing, splitting but not lumping of clinical findings would be a better strategy to decipher these multigenic complex inflammatory disorders.

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Source
http://dx.doi.org/10.1111/jdv.18172DOI Listing

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