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首页> 外文期刊>Archives of dermatological research. >Lipoteichoic acid-related molecule derived from the streptococcal preparation, OK-432, which suppresses atopic dermatitis-like lesions in NC/Nga mice.
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Lipoteichoic acid-related molecule derived from the streptococcal preparation, OK-432, which suppresses atopic dermatitis-like lesions in NC/Nga mice.

机译:源自链球菌制剂OK-432的脂蛋白酸相关分子可抑制NC / Nga小鼠的特应性皮炎样病变。

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Bacterial stimulation may serve to control atopic disorders such as atopic dermatitis (AD) through inducement of Th1 cell-mediated immune response. The lipoteichoic acid (LTA)-related molecule (okLTA) from streptococcal preparation, OK-432, has been shown to be a potent Th1 inducer through the action of IL-12. Examination was made of the therapeutic effects of this okLTA injected intra- and/or subcutaneously into AD-like lesions in NC/Nga mice, particularly in the vicinity of the suppressor of cytokine signaling (SOCS) regulatory pathways. Using immunohistochemical staining with IL-4/IL-12p40 and phosphorylated STAT6/p-STAT4 and RT-PCR for IL-4/IL-12p40, STAT6/STAT4 and mRNA expression and in situ hybridization of SOCS3 and 5, evaluation was made of the immunoregulatory effects of this okLTA in the treatment of spontaneous AD-like lesions in NC/Nga mice. Following the injection of okLTA, remarkable improvement in the lesions of NC/Nga mice was noted. In okLTA-treated skin, IL-12p40/p-STAT4 positive cellular infiltration was extensive while IL-4/p-STAT6 positive cell infiltration was seen to diminish considerably, compared to untreated NC mice. SOCS3 in situ expression in okLTA-treated mice was noted to be significantly less compared to untreated NC mice, in which the expression was prominent. SOCS5 in situ expression was rather, though not significantly, strong in okLTA-treated mice. okLTA treatment is clearly shown to induce Th1 cellular response and down-regulate immune response in the Th2 pathway through SOCS3 reduction in AD-like lesions of NC/Nga mice. The present results demonstrate that bacterial wall components such as okLTA should serve as an effective new therapeutic approach for treating AD.
机译:细菌刺激可通过诱导Th1细胞介导的免疫反应来控制特应性疾病,例如特应性皮炎(AD)。链球菌制剂OK-432中与脂蛋白酸(LTA)相关的分子(okLTA)已显示通过IL-12的作用是有效的Th1诱导剂。检查了将这种okLTA皮内和/或皮下注射到NC / Nga小鼠的AD样病变中的治疗效果,特别是在细胞因子信号转导(SOCS)调节通路的抑制剂附近。使用IL-4 / IL-12p40和磷酸化STAT6 / p-STAT4的免疫组织化学染色以及RT-PCR对IL-4 / IL-12p40,STAT6 / STAT4和mRNA表达以及SOCS3和5的原位杂交进行评估这种okLTA对NC / Nga小鼠自发性AD样病变的免疫调节作用。注射okLTA后,注意到NC / Nga小鼠的病变明显改善。与未经治疗的NC小鼠相比,在经okLTA处理的皮肤中,IL-12p40 / p-STAT4阳性细胞浸润广泛,而IL-4 / p-STAT6阳性细胞浸润明显减少。 okLTA处理的小鼠中SOCS3原位表达与未处理的NC小鼠相比明显减少,后者的表达很明显。在经okLTA处理的小鼠中,SOCS5原位表达相当强,尽管不明显。 okLTA治疗已明确显示可通过SOCS3减少NC / Nga小鼠AD样病变而诱导Th1细胞应答并通过Th2途径下调免疫应答。目前的结果表明,细菌壁成分如okLTA应该成为治疗AD的有效新治疗方法。

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