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Toxin Levels in Serum Correlate with the Development of Staphylococcal Scalded Skin Syndrome in a Murine Model

机译:在小鼠模型中血清中的毒素水平与葡萄球菌烫伤的皮肤综合症的发展相关

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Staphylococcal scalded skin syndrome (SSSS) is an exfoliative dermatitis that results from infection with exfoliative toxin-producingStaphylococcus aureus. SSSS is seen primarily in infants and children. Here we ask if there is a specific maturation process that protects healthy adults from this syndrome. For these studies, an active recombinant exfoliative toxin A (rETA) was used in a neonatal mouse model. A time course generated on the susceptibility to the toxin as a function of mouse age indicated that BALB/c mice developed the characteristic symptoms of SSSS until day 7 of life. Between day 7 and day 8 of life there was a dramatic decrease in susceptibility, such that mice at day 9 of life were resistant to the effects of the toxin. This time course corresponds approximately to the time needed for maturation of the adaptive immune response, and SSSS in adults is often identified with immunocompromised states. Therefore, mice deficient in this response were examined. Adult mice thymectomized at birth and adult SCID mice did not develop the symptoms of SSSS after injection with the toxin, indicating that the adaptive immune response is not responsible for the lack of susceptibility observed in the older mice. SSSS in adults is also associated with renal disorders, suggesting that levels of toxin in serum are important in the development of the disease. rETA was not cleared as efficiently from the serum of 1-day-old mice compared to clearance from 10-day-old mice. Ten-day-old mice were given repeated injections of toxin so that the maximal level of toxin was maintained for a sustained period of time, and exfoliation occurred in these mice. Thus, whereas the adaptive immune response is not needed for protection of adult mice from SSSS, efficient clearance of the toxin from the bloodstream is a critical factor.
机译:葡萄球菌烫伤皮肤综合症(SSSS)是一种由剥脱性毒素产生的金黄色葡萄球菌感染引起的剥脱性皮炎。 SSSS主要见于婴儿和儿童。在这里,我们问是否有特定的成熟过程可以保护健康的成年人免受这种综合征的困扰。对于这些研究,在新生小鼠模型中使用了活性重组脱落性毒素A(rETA)。关于毒素的敏感性随小鼠年龄变化的时间过程表明,BALB / c小鼠在生命的第7天出现SSSS的特征性症状。在生命的第7天至第8天之间,药敏性急剧下降,因此生命第9天的小鼠对毒素的作用具有抗性。该时间过程大致对应于适应性免疫反应成熟所需的时间,成人中的SSSS通常被识别为免疫功能低下状态。因此,检查了该反应不足的小鼠。注射毒素后,在出生时被胸腺切除的成年小鼠和成年的SCID小鼠没有出现SSSS的症状,这表明适应性免疫反应与在老年小鼠中缺乏药敏性无关。成人的SSSS也与肾脏疾病有关,这表明血清中的毒素水平在疾病的发展中很重要。与从10天大的小鼠中清除相比,从1天大的小鼠血清中不能有效清除rETA。给十天大的小鼠重复注射毒素,以使毒素的最大水平维持一段持续的时间,并且在这些小鼠中发生脱落。因此,尽管保护成年小鼠免于SSSS并不需要适应性免疫应答,但从血液中有效清除毒素却是一个关键因素。

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