首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >Myeloperoxidase Expression by Histiocytes in Kikuchi’s and Kikuchi-Like Lymphadenopathy
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Myeloperoxidase Expression by Histiocytes in Kikuchi’s and Kikuchi-Like Lymphadenopathy

机译:菊池和菊池样淋巴结病中组织细胞的髓过氧化物酶表达

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摘要

Forty-five examples of Kikuchi’s lymphadenitis (KL), 5 Kikuchi-like lupus erythematosus lymphadenopathies, 25 nonnecrotizing lymphadenitidies (5 toxoplasmic, 5 sarcoid-like, 6 dermatopathic, 4 suppurative, 3 tubercular, 2 with sinus histiocytosis), 4 examples of hyaline-vascular Castleman disease (CD), 2 plasmacytoid monocyte tumors (PM-Ts), and 61 accessory cell neoplasms were studied by a panel of antibodies, including the PG-M1 (against a macrophage-restricted CD68 epitope) and a polyclonal anti-myeloperoxidase (MPO). In KL and Kikuchi-like lupus erythematosus lymphadenopathies, 25 to 75% of CD68+ histiocytes co-expressed MPO. This did not occur in nonnecrotizing lymphadenitidies and accessory cell neoplasms. MPO+/CD68+ elements corresponded to nonphagocytosing mononuclear cells and some crescentic macrophages and phagocytosing histiocytes. Typical PMs were MPO/CD68+ in all cases, including CD and PM-T. Our observations suggest that in KL and KL-like lymphadenopathies: 1) MPO+/CD68+ blood monocytes might be attracted into tissues because of the lack or paucity of granulocytes and the need of MPO for oxidative processes; 2) PMs are more likely to be involved in the cytotoxic immune reaction than in phagocytic phenomena; 3) the peculiar phenotype of the histiocytic component can be usefully used for the differentiation from malignant lymphoma and PM-T.
机译:菊池淋巴结炎(KL)的45个例子,菊池样红斑狼疮淋巴腺病5个,非坏死性淋巴腺病25个(弓形虫5个,类结节状5个,皮肤病,4个化脓性,3个结核性,2个窦性血吸虫病的例子) -血管Castleman病(CD),2个浆细胞样单核细胞肿瘤(PM-Ts)和61个辅助细胞肿瘤由一组抗体研究,包括PG-M1(针对巨噬细胞限制性CD68表位)和多克隆抗髓过氧化物酶(MPO)。在KL和菊池样红斑狼疮淋巴腺病中,CD68 + 组织细胞中有25%至75%共同表达MPO。这在非坏死性淋巴结肿大和辅助细胞肿瘤中没有发生。 MPO + / CD68 + 元素对应于非吞噬单核细胞,某些月牙巨噬细胞和吞噬组织细胞。在所有情况下,包括CD和PM-T,典型的PM是MPO - / CD68 + 。我们的观察结果提示,在KL和KL样淋巴腺病中:1)MPO + / CD68 + 血液单核细胞可能由于缺乏或缺乏粒细胞而被吸引入组织。氧化过程需要MPO; 2)PMs比吞噬现象更可能参与细胞毒性免疫反应; 3)组织细胞成分的独特表型可用于区分恶性淋巴瘤和PM-T。

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