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IgG4 Overexpression Is Rare in Meningiomas with a Prominent Inflammatory Component: A Review of 16 Cases
Authors:Aseem Lal  Sonika Dahiya  Michael Gonzales  Annie Hiniker  Richard Prayson  Bette K Kleinschmidt‐DeMasters  Arie Perry
Institution:1. Department of Pathology, University of California San Francisco, , San Francisco, CA;2. Department of Pathology, Washington University School of Medicine, , St. Louis, MO;3. Anatomical Pathology Department, Royal Melbourne Hospital, , Melbourne, Australia;4. Department of Anatomic Pathology, Cleveland Clinic Foundation, , Cleveland, OH;5. Department of Pathology, University of Colorado Health Science Center, , Denver, CO;6. Neurological Surgery, University of California San Francisco, , San Francisco, CA
Abstract:Meningiomas with prominent inflammation are traditionally classified as “lymphoplasmacyte‐rich meningioma” (LPM). Both inflammatory and neoplastic meningeal proliferations have recently been linked to IgG4 disease, although a potential association with LPM has not been previously explored. Sixteen meningiomas with inflammatory cells outnumbering tumor cells were further characterized by CD3, CD20, CD68 and/or CD163, CD138, kappa, lambda, IgG and IgG4 immunostains. There were 11 female and 4 male patients, ranging from 22 to 78 (median 59) years of age. Tumors consisted of 10 World Health Organization (WHO) grade I, 5 grade II and 1 grade III LPMs. Immunohistochemically, the most numerous cell type was the macrophage in all cases followed by CD3‐positive T cells and fewer CD20‐positive B cells. Plasma cells ranged from moderate‐marked (N = 5) to rare (N = 7), or absent (N = 4). Maximal numbers of IgG4 plasma cells per high power field (HPF) ranged from 0 to 32, with only two cases having counts exceeding 10/HPF. The IgG4/IgG ratio was increased focally in only two cases (30% and 31%). Additionally, plasma cells represented only a minor component in most examples, whereas macrophages predominated, suggesting that “inflammation‐rich meningioma” may be a more accurate term. The inflammatory stimulus for most cases remains to be elucidated.
Keywords:IgG4  inflammation  lymphoplasmacyte rich  meningioma
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