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大剂量甲基强的松龙治疗对系统性红斑狼疮患者吞噬细胞功能的影响。

Effect of high-dose methylprednisolone therapy on phagocyte function in systemic lupus erythematosus.

作者信息

Boghossian S H, Isenberg D A, Wright G, Snaith M L, Segal A W

出版信息

Ann Rheum Dis. 1984 Aug;43(4):541-50. doi: 10.1136/ard.43.4.541.

Abstract

Circulating phagocytes play a major role in the defence of the host against microbial infection. In an attempt to identify the reason for the unusual susceptibility to infection of patients with systemic lupus erythematosus (SLE) various parameters of phagocytic cell function were assessed kinetically in whole blood, and the accumulation of cells in areas of inflammation was studied in vivo with the skin window technique. The effect on these parameters of conventional therapy with glucocorticoids and pulse therapy with large doses of methylprednisolone were examined. Patients on conventional doses of steroids had no abnormality of phagocyte function that might have predisposed to infection, apart from a reduced accumulation of monocytes in areas of inflammation and decreased lactoferrin secretion. Pulse therapy with methylprednisolone considerably delayed the secretion of lactoferrin and the adherence of neutrophils in most of the patients, as well as impairing bacterial killing and digestion.

摘要

循环吞噬细胞在宿主抵御微生物感染的防御中起主要作用。为了确定系统性红斑狼疮(SLE)患者对感染异常易感的原因,对全血中吞噬细胞功能的各种参数进行了动力学评估,并采用皮肤窗技术在体内研究了炎症区域细胞的聚集情况。研究了糖皮质激素常规治疗和大剂量甲泼尼龙脉冲治疗对这些参数的影响。接受常规剂量类固醇治疗的患者,除了炎症区域单核细胞聚集减少和乳铁蛋白分泌减少外,没有可能易患感染的吞噬细胞功能异常。甲泼尼龙脉冲治疗在大多数患者中显著延迟了乳铁蛋白的分泌和中性粒细胞的黏附,同时损害了细菌的杀灭和消化。

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本文引用的文献

5
High-dose intravenous methylprednisolone pulse therapy in systemic lupus erythematosus.
Am J Med. 1981 Apr;70(4):817-24. doi: 10.1016/0002-9343(81)90538-6.
6
The kinetic measurement of phagocyte function in whole blood.
J Immunol Methods. 1983 May 27;60(1-2):125-40. doi: 10.1016/0022-1759(83)90341-1.
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A human skin window technique using micropore membranes.
J Immunol Methods. 1982 Oct 15;54(1):129-39. doi: 10.1016/0022-1759(82)90121-1.
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Budesonide and nasal mucosal histamine content and anti-IgE induced histamine release.
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