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银屑病患者的外周血淋巴细胞对β-链球菌超抗原反应低下。

Peripheral blood lymphocytes from psoriatic patients are hyporesponsive to beta-streptococcal superantigens.

作者信息

Horiuchi N, Aiba S, Ozawa H, Sugawara S, Rikiishi H, Kumagai K, Tagami H

机构信息

Department of Dermatology, Tohoku University School of Medicine, Sendai, Japan.

出版信息

Br J Dermatol. 1998 Feb;138(2):229-35. doi: 10.1046/j.1365-2133.1998.02066.x.

Abstract

The strong association of acute guttate psoriasis and streptococcal throat infection, together with the preferential use of T cells expressing a particular T-cell receptor, has suggested a role for bacterial superantigens in the pathogenesis of psoriasis. We examined the proliferative responses of peripheral blood lymphocytes (PBLs), obtained from patients with psoriasis and from healthy controls, to streptococcal superantigens, cytoplasmic membrane-associated protein (CAP) and secretion-type CAP (SCAP), isolated from group A, beta-haemolytic streptococci. PBLs from patients with psoriasis showed significantly less response to SCAP and CAP than those from healthy controls. Because there was no difference between psoriatic patients and controls in the proliferative response of PBLs to staphylococcal enterotoxin A or E (SEA, SEE) or the mitogen phytohaemagglutinin (PHA), these findings strongly suggest that the reduced reactivity to the streptococcal superantigens seems to reflect anergy of a population of PBLs to the superantigens. As the CAP used in the present study stimulates V beta 8 T cells selectively, we further examined the proliferation of V beta 8 T cells after such stimulation using flow cytometry. V beta 8 T cells obtained from three of four psoriatic patients failed to proliferate in the presence of CAP, whereas they proliferated vigorously in the presence of SEE, which activates V beta 8 T cells, confirming the specific hyporesponsiveness of PBLs from psoriatic patients to streptococcal superantigens. We then determined the effects of serum factors on the suppressed response of PBLs to the streptococcal superantigens with SCAP or CAP. It was partially restored when PBLs were cultured with sera obtained from healthy subjects, although the responses were still significantly lower than those of the healthy controls. In contrast, psoriatic sera markedly suppressed the proliferative response of PBLs from healthy controls to CAP or SCAP, but showed no suppression of the proliferative response of PBLs to SEA. Because these findings suggest the presence of specific inhibitory factors in psoriatic sera, we examined whether the inhibitory effect was caused by antisuperantigen antibody. However, no significant increase was detected in antibody titre to CAP in psoriatic sera, as has been noted in sera from patients with poststreptococcal glomerulonephritis. The present results show for the first time the hyporesponsiveness of PBLs to streptococcal superantigens and the presence of serum inhibitors that specifically inhibit T-cell response to the superantigens in psoriatic patients. These findings suggest a pathological role for streptococcal infections in the pathogenesis of psoriasis.

摘要

点滴状银屑病与链球菌性咽炎感染之间的密切关联,以及表达特定T细胞受体的T细胞的优先使用,提示细菌超抗原在银屑病发病机制中发挥作用。我们检测了从银屑病患者和健康对照者获取的外周血淋巴细胞(PBLs)对从A组β溶血性链球菌分离出的链球菌超抗原、细胞质膜相关蛋白(CAP)和分泌型CAP(SCAP)的增殖反应。银屑病患者的PBLs对SCAP和CAP的反应明显低于健康对照者。由于银屑病患者和对照者的PBLs对葡萄球菌肠毒素A或E(SEA、SEE)或促有丝分裂原植物血凝素(PHA)的增殖反应没有差异,这些发现强烈表明对链球菌超抗原反应性降低似乎反映了一群PBLs对超抗原的无反应性。由于本研究中使用的CAP选择性刺激Vβ8 T细胞,我们使用流式细胞术进一步检测了此类刺激后Vβ8 T细胞的增殖情况。从四名银屑病患者中的三名获取的Vβ8 T细胞在有CAP存在时未能增殖,而在激活Vβ8 T细胞的SEE存在时它们则强烈增殖,证实了银屑病患者的PBLs对链球菌超抗原具有特异性低反应性。然后我们确定了血清因子对PBLs对带有SCAP或CAP的链球菌超抗原的抑制反应的影响。当PBLs与从健康受试者获取血清一起培养时,反应部分恢复,尽管仍明显低于健康对照者。相反,银屑病血清显著抑制健康对照者的PBLs对CAP或SCAP的增殖反应,但对PBLs对SEA的增殖反应无抑制作用。因为这些发现提示银屑病血清中存在特异性抑制因子,我们检测了这种抑制作用是否由抗超抗原抗体引起。然而,银屑病血清中对CAP的抗体滴度没有显著增加,这与链球菌感染后肾小球肾炎患者的血清情况一致。目前的结果首次显示了银屑病患者PBLs对链球菌超抗原的低反应性以及血清抑制剂的存在,这些抑制剂特异性抑制T细胞对超抗原的反应。这些发现提示链球菌感染在银屑病发病机制中具有病理作用。

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