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Ischemic fasciitis

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(Redirected from Ischaemic fasciitis)
Ischemic fasciitis
Other namesAtypical decubital fibroplasia, decubital ischemic fasciitis
Histopathology of ischemic fasciitis, with typical features
SpecialtyDermatology, Dermatopathology, General Surgery
CausesUnknown
TreatmentSurgical removal or long-term observation
PrognosisCompletely benign tumor
FrequencyRare
DeathsNone

Ischemic fasciities (IF), also termed atypical decubital fibroplasia[1] or decubital ischemic fasciitis,[2] is a rare pseudosarcomatous (i.e. easily mistaken for a sarcoma) tumor. It was first described by E. A. Montgomery et al. in 1992.[3] This tumor typically forms in the subcutaneous tissues (i.e. lower most tissue layer of the skin) that overlie bony protuberances such as a hip in individuals who are debilitated and bed-ridden.[1]

Microscopically, IF lesions consist of proliferating, atypical fibroblasts and/or myofibroblasts. The lesions were initially regarded as non-neoplastic proliferation responses of these cell types to long-term tissue pressure or trauma.[4] More recently, however, the World Health Organization, 2020, defined IF lesions as neoplasms, i.e. tissue growths which are uncoordinated with that of the normal surrounding tissue and persist in growing even if the original trigger for their development is removed. The Organization formally classified IF lesions as belonging to the category of benign fibroblastic and myofibroblastic tumors.[5]

The treatment of choice for these often disfiguring, uncomfortable, and/or painful IF tumors is generally conservative, local surgical excision.[6] It is critically important that these benign tumors be distinguished from other fasciitis tumors as well as certain sarcomas which can be highly invasive and/or malignant and therefor require far more aggressive treatment.[2]

Presentation

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In the original study of IF, individuals diagnosed with the disorder were women (16 cases) or men (12 cases) age 15 to 95 years;[3] In a more recent study, diagnosed individuals were women (15 cases) or men (29 cases) aged 23–96 years old.[4] Most individuals in these two studies were in their 8th or 9th decade when diagnosed with IF and, overall, had a relatively long history of being invalided, immobilized, and/or bed-ridden due to other disorders such as severe osteoarthritis, rheumatoid arthritis, chronic renal failure, chronic obstructive pulmonary disease, cancer,[3] or dementia.[2] In the study of 44 individuals, however, an appreciable number of patients did not have a history of debilitation.[4][7] Some individuals reported that they had prior trauma in the areas where their lesions developed.[4]

Individuals present with a painless[3] or painful[4] and sometimes disabling[1] slowly growing mass[1] that is ill-defined, located in deep subcutaneous tissues, and, rarely, has spread into an adjacent skeletal muscle or tendon. The masses vary from 1.3 to 10 cm in maximum diameter.[3] In the study of 44 cases, 76.7% of the tumors were located around the base of a hip (11 cases), shoulder (7 cases), or greater trochanter of the femur; 4 were in a hip joint, 4 in a thigh, 3 in the iliac crest, 2 in a buttock, and 1 each in the lumbar region, scapular region, or a deltoid muscle; in the remaining cases, ~11.2% of the tumors were on the chest wall away from the shoulders and ~11.2% were on the back.[3] Typically, the tumors reside over boney protuberances which, it is thought, provide the mechanical pressures that cause poor blood flow to nearby subcutaneous tissues, aberrant wound healing in these tissues, and thereby the development of IF.[4]

Pathology

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On gross examination, IF tumors are typically white-yellow masses with central necrosis (i.e. areas of dead or dying cells), and areas containing cysts and/or old, dried hemorrhages.[6] The tumors are often poorly circumscribed, have an infiltrative appearance, may be multinodular, and lie in subcutaneous tissue but may also involve the dermal layer of the skin[8] and/or the reticular dermis.[6] Microscopic histopathological studies of IF tissues report the characteristic presence of a distinct zonal appearance, i.e. the presence of central zones of fibrinoid necrosis and areas of cyst-laden necrosis in a hypocellular background surrounding by a zone of granulation tissue (i.e. connective tissue containing microscopic blood vessels) populated by atypical, swollen fibroblasts, myofibroblasts, and/or macrophages.[4]

Immunohistochemistry analyses of IF tumors often show the presence of fibroblasts, fibroblast-like cells, and or other types of cells that in a percentage of cases express smooth muscle actin proteins, CD68 protein,.[6] desmin protein,[4] vimentin protein, and collagen type IV protein, but not keratin, S100,[6] calponin, or CD34 proteins.[1] The finding that a tumor's cells have some of these patterns of protein expression can help support the diagnosis of IF.[6]

Gene and chromosome abnormalities

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A single case of IF was found to have tumor cells bearing chromosomal translocations between chromosomes 1 and 2 and/or chromosomes 7 and 19. While further studies are needed to confirm these finding and to conduct further gene and chromosome analyses, these results support the notion that IF tumors are neoplasms rather than purely reactive lesions.[8]

Diagnosis

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IF tumors have features which overlap other types of fasciitis disorders such as proliferative fasciitis and nodular fasciitis. However, the age, history of debilitation, tumor location over boney protuberances, and tumor histopathology of having two distinctly different zones tend to distinguish IF from these two as well as the following tumors. Decubitus ulcers, i.e. common bed sores, differ from IF in typically having extensive ulcerations of the skin and histopathological evidence of acute inflammation as determined by the presence of various types of white blood cells.[4] IF has also been mistaken for epithelioid sarcoma and elastofibroma dorsi. IF differs form epithelioid sarcoma by its clinical presentation, typical tumor cell morphology, i.e. round cells with atypical nuclei and eosinophilic cytoplasm,[1] and complete or relative lack of necrotic areas.[6] Elastofibroma dorsi is distinguished from IF by its abundant content of elastic fibers.[1]

Treatment

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IF tumors are commonly treated by surgical excision although in rare cases these tumors have recurred at the site of their removal. Recurrent tumors have been treated by repeated surgical excisions.[7] Since IF tumors have not been reported to metastasize and no deaths have been attributed to it,[1] long-term clinical observation without surgical intervention is a reasonable alternative to surgery, particularly for IF tumors that are neither uncomfortable, painful, or disfiguring.[7]

References

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  1. ^ a b c d e f g h Fukunaga M (September 2001). "Atypical decubital fibroplasia with unusual histology". APMIS. 109 (9): 631–5. doi:10.1034/j.1600-0463.2001.d01-185.x. PMID 11878717. S2CID 29499215.
  2. ^ a b c Kuyumcu G, Zhang Y, Ilaslan H (December 2019). "Case 272: Decubital Ischemic Fasciitis". Radiology. 293 (3): 721–724. doi:10.1148/radiol.2019171255. PMID 31751192.
  3. ^ a b c d e f Montgomery EA, Meis JM, Mitchell MS, Enzinger FM (July 1992). "Atypical decubital fibroplasia. A distinctive fibroblastic pseudotumor occurring in debilitated patients". The American Journal of Surgical Pathology. 16 (7): 708–15. doi:10.1097/00000478-199207000-00009. PMID 1530110. S2CID 21116139.
  4. ^ a b c d e f g h i Liegl B, Fletcher CD (October 2008). "Ischemic fasciitis: analysis of 44 cases indicating an inconsistent association with immobility or debilitation". The American Journal of Surgical Pathology. 32 (10): 1546–52. doi:10.1097/PAS.0b013e31816be8db. PMID 18724246. S2CID 24664236.
  5. ^ Sbaraglia M, Bellan E, Dei Tos AP (April 2021). "The 2020 WHO Classification of Soft Tissue Tumours: news and perspectives". Pathologica. 113 (2): 70–84. doi:10.32074/1591-951X-213. PMC 8167394. PMID 33179614.
  6. ^ a b c d e f g Saeed L; Bahrani E; Lauw MIS; Tabatabai ZL; Arron ST; Mauro TM (March 2020). "Ischemic Fasciitis Mimicking A Lipoma". Dermatologic Surgery. 46 (3): 427–430. doi:10.1097/DSS.0000000000001853. PMID 30789504. S2CID 73465332.
  7. ^ a b c Sakamoto A, Arai R, Okamoto T, Yamada Y, Yamakado H, Matsuda S (October 2018). "Ischemic Fasciitis of the Left Buttock in a 40-Year-Old Woman with Beta-Propeller Protein-Associated Neurodegeneration (BPAN)". The American Journal of Case Reports. 19: 1249–1252. doi:10.12659/AJCR.911300. PMC 6206622. PMID 30341275.
  8. ^ a b Sachak T, Heerema NA, Mayerson J, Payne JE, Parwani A, Iwenofu OH (March 2018). "Novel t(1;2)(p36.1;q23) and t(7;19)(q32;q13.3) chromosomal translocations in ischemic fasciitis: expanding the spectrum of pseudosarcomatous lesions with clonal pathogenetic link". Diagnostic Pathology. 13 (1): 18. doi:10.1186/s13000-018-0695-y. PMC 5834908. PMID 29499721.