首页> 美国卫生研究院文献>Clinical and Experimental Immunology >Soluble adhesion molecules in sera of patients with leprosy: levels of soluble intercellular adhesion molecule-1 (sICAM-1) rapidly decrease during multi-drug therapy
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Soluble adhesion molecules in sera of patients with leprosy: levels of soluble intercellular adhesion molecule-1 (sICAM-1) rapidly decrease during multi-drug therapy

机译:麻风患者血清中的可溶性粘附分子:在多种药物治疗期间可溶性细胞间粘附分子-1(sICAM-1)的水平迅速下降

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摘要

The clinicopathological spectrum of leprosy is associated with an altered immunological reaction. The expression of adhesion molecules on endothelial cells directs the cellular traffic to sites of local skin and nerve inflammation. Soluble forms of adhesion molecules, which are released upon cytokine activation, can be detected in the circulation and may reflect ongoing tissue inflammation. We determined the serum levels of sICAM-1, sE-selectin and sL-selectin in 74 patients with leprosy (tuberculoid form, n = 23; lepromatous form, n = 36; acute leprous reaction, n = 16) and 15 healthy age- and sex-matched control donors. Patients with lepromatous leprosy had significantly higher levels of sICAM-1 (564 ± 174 versus 450 ± 92 versus 334 ± 57 ng/ml) and E-selectin (90 ± 31 versus 74 ± 29 versus 50 ± 10 ng/ml) than patients with tuberculoid leprosy and normal donors (P<0.01). No differences between groups were detected for L-selectin. Patients with leprous reactions had similar high levels to lepromatous patients. Twenty lepromatous patients were re-examined after 4 weeks of therapy. A significant decrease in sICAM-1 serum levels was observed after 1 month of anti-mycobacterial treatment, which was accompanied by a reduction of mycobacteria in skin biopsies (P<0.01). Patients with leprous reactions (n = 13) also demonstrated a drop in sICAM-1 after anti-inflammatory therapy. sE-selectin and sL-selectin serum values decreased only in lepromatous patients after therapy. It can be concluded that soluble adhesion molecules like sICAM-1 and sE-selectin are promising activity markers in patients with leprosy, which may be useful for treatment monitoring.
机译:麻风的临床病理频谱与免疫反应改变有关。粘附分子在内皮细胞上的表达将细胞运输导向局部皮肤和神经发炎的部位。在细胞因子激活后释放的可溶性形式的粘附分子可以在循环中检测到,并可能反映正在进行的组织炎症。我们确定了74位麻风病患者(stubeloid型,n = 23;麻风型,n = 36;急性麻风反应,n = 16)和15岁健康年龄的患者的sICAM-1,sE-选择素和sL-选择素的血清水平和性别匹配的对照供体。麻风麻风病患者的sICAM-1(564±174对450±92对334±57 ng / ml)和E-选择素(90±31对74±29对50±10 ng / ml)的水平明显高于患者结核性麻风患者和正常供者(P <0.01)。 L-选择素在组之间未检测到差异。麻风反应患者的高水平与麻风患者相似。治疗4周后,对20名麻风病患者进行了重新检查。抗分枝杆菌治疗1个月后观察到sICAM-1血清水平显着下降,同时皮肤活检中分枝杆菌减少(P <0.01)。麻风反应患者(n = 13)也显示出抗炎治疗后sICAM-1下降。 sE-selectin和sL-selectin血清值仅在治疗后的麻风病患者中降低。可以得出结论,可溶性粘附分子如sICAM-1和sE-选择素是麻风病患者的有前途的活性标记物,可能对治疗监测有用。

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