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氨苯砜对中性粒细胞与抗体黏附的抑制作用:氨苯砜治疗IgA皮肤病的一种可能治疗机制。

Inhibition of neutrophil adherence to antibody by dapsone: a possible therapeutic mechanism of dapsone in the treatment of IgA dermatoses.

作者信息

Thuong-Nguyen V, Kadunce D P, Hendrix J D, Gammon W R, Zone J J

机构信息

Dermatology Section, Veterans Affair Medical Center, Salt Lake City, Utah.

出版信息

J Invest Dermatol. 1993 Apr;100(4):349-55. doi: 10.1111/1523-1747.ep12471811.

Abstract

Dapsone is frequently effective in cutaneous diseases characterized by antibody deposition and accumulation of neutrophils. We hypothesized that this mechanism of action of dapsone may involve the inhibition of neutrophil adherence to antibody. The neutrophil adherence assay, which measures the binding of neutrophils to basement membrane zone-bound antibody on skin sections, was used to evaluate the effect of dapsone on neutrophil adherence to immunoglobulin A and immunoglobulin G. We evaluated the effect of dapsone on adherence of normal neutrophils to immunoglobulin A and immunoglobulin G from sera of linear immunoglobulin A bullous dermatosis and bullous pemphigoid patients, respectively. Linear immunoglobulin A bullous dermatosis or bullous pemphigoid antibody were bound to the basement membrane zone of normal skin sections as a substrate for the neutrophil adherence assay. Dapsone was added directly to the neutrophils or to the antibody source in concentrations of 0-50 micrograms/ml (pharmacologic range). Addition of dapsone to neutrophils produced an incremental inhibition of neutrophil adherence up to 75% at 50 micrograms/ml. Dapsone produced similar inhibition when added directly to the antibody itself, despite washing prior to usage in the neutrophil-adherence assay. Control specimens including irrelevant fractions of patient sera failed to demonstrate binding. Serum from a patient on dapsone therapy also showed inhibition of neutrophil adherence compared to the same patient on no therapy. We conclude that dapsone inhibits the adherence of neutrophils to basement membrane zone antibody in a dose-dependent manner. This may be related to an effect directly on antibody. This inhibition may contribute to the clinical efficacy of dapsone in antibody-mediated diseases.

摘要

氨苯砜对以抗体沉积和中性粒细胞聚集为特征的皮肤疾病常常有效。我们推测氨苯砜的这一作用机制可能涉及抑制中性粒细胞与抗体的黏附。中性粒细胞黏附试验用于评估氨苯砜对中性粒细胞与免疫球蛋白A和免疫球蛋白G黏附的影响,该试验可测量中性粒细胞与皮肤切片上基底膜带结合抗体的结合情况。我们分别评估了氨苯砜对正常中性粒细胞与线状免疫球蛋白A大疱性皮肤病和大疱性类天疱疮患者血清中免疫球蛋白A和免疫球蛋白G黏附的影响。将线状免疫球蛋白A大疱性皮肤病或大疱性类天疱疮抗体结合到正常皮肤切片的基底膜带,作为中性粒细胞黏附试验的底物。将氨苯砜以0 - 50微克/毫升(药理范围)的浓度直接添加到中性粒细胞或抗体来源中。向中性粒细胞中添加氨苯砜会使中性粒细胞黏附受到逐渐增强的抑制,在50微克/毫升时抑制率高达75%。尽管在用于中性粒细胞黏附试验之前进行了洗涤,但将氨苯砜直接添加到抗体本身时也产生了类似的抑制作用。包括患者血清无关组分的对照标本未显示出结合。与未接受治疗的同一患者相比,接受氨苯砜治疗患者的血清也显示出对中性粒细胞黏附的抑制作用。我们得出结论,氨苯砜以剂量依赖的方式抑制中性粒细胞与基底膜带抗体的黏附。这可能与对抗体的直接作用有关。这种抑制作用可能有助于氨苯砜在抗体介导疾病中的临床疗效。

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