Focal myositis: a clinicopathologic study of 115 cases of an intramuscular mass-like reactive process.

[focal myositis]

Focal myositis is an uncommon inflammatory pseudotumor of skeletal muscle that can be confused with a variety of neoplastic and inflammatory diseases . It is often misunderstood because it presents as a tumor -like mass , but histologically resembles a skeletal muscle myopathy or dystrophy . We wanted to discuss the detailed morphologic and immunophenotypic features of the largest reported group of focal myositis patients .Two hundred and six cases coded as "focal myositis " were culled from our files . Only 115 cases with adequate material , a solitary lesion , and correct diagnosis were included . A variety of immunohistochemical studies were performed , as were polymerase chain reaction for T cell receptor gene rearrangement and immunoglobulin heavy chain rearrangement .Age ranged from 7 to 94 years (mean 41 , median 36 y ). Most patients were otherwise healthy , and with the exception of 10 cases , lacked antecedent trauma . Masses that ranged in size from 1 .0 to 20 .0 cm (median 3 .0 cm , mean 3 .9 cm ) were reported in specific muscles of the lower extremities (including vastus lateralis , adductor muscle , and groin muscles , n =39 ; gastrocnemius , n =22 ), followed by the trunk , neck (mentalis , n =8 ; sternocleidomastoid muscle , n =8 ), and upper extremity . Histologically , these were solitary intramuscular processes composed of variable myopathic (93 %) and focal neurogenic (89 %) changes , fibrosis , and inflammation (97 %), occasionally accompanied by prominent eosinophils (n =20 ). By immunohistochemistry , most cases had CD 163 -positive macrophages that were negative for S 100 protein and CD 1 a . Lymphocytes were mostly CD 3 , CD 4 -positive lymphocytes that were negative for cytotoxic markers , TIA -1 and granzyme-B . Polymerase chain reaction did not show B cell or T cell rearrangement . In situ studies for Epstein-Barr -encoded receptor were negative , as was ALK -1 immunohistochemistry . Major histocompatibility complex -1 and weak IgG 4 were focally positive in skeletal muscle . Cases with severe inflammation had increased numbers of CD 2 0 -positive B cells and CD 123 -positive plasmacytic dendritic cells . S 100 was strongest in skeletal muscle fibers with vacuolar change . Clinical diagnostic considerations ranged from benign entities such as rhabdomyoma , intramuscular lipoma , fibromatosis , myositis ossificans , proliferative myositis , inflammatory myofibroblastic tumor , and inflammatory myopathy to malignant entities such as rhabdomyosarcoma , leiomyosarcoma , liposarcoma , and lymphoma . Available follow-up revealed spontaneous regression .Focal myositis occurs in specific muscle groups of young adults of both sexes without significant trauma . It is a largely unrecognized entity with specific histology including myopathic , focal neurogenic , fibrosis , and inflammatory features . It can be easily mistaken for an inflammatory myopathy , dystrophy , alternate reactive , or even neoplastic process . Focal myositis seems to be a macrophage and T -cell-rich lesion that changes to B cell and dendritic plasmacytoid cells when markedly inflamed , but does not seem to have a known viral or molecular etiology . IgG 4 presence may be linked to the fibrosis in these lesions ; a possible transient autoimmune etiology can not be excluded . Careful attention to reproducible clinicopathologic features can aid diagnosis and spare patients from excessive surgery or adverse therapy .