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新生期给予辣椒素处理的大鼠中慢性复发性瘙痒性皮炎;人类特应性皮炎的潜在大鼠模型。

Chronically relapsing pruritic dermatitis in the rats treated as neonate with capsaicin; a potential rat model of human atopic dermatitis.

机构信息

Neuroscience Research Institute and Department of Physiology, Korea University College of Medicine, Seoul, Republic of Korea.

出版信息

J Dermatol Sci. 2012 Aug;67(2):111-9. doi: 10.1016/j.jdermsci.2012.05.006. Epub 2012 May 28.

Abstract

BACKGROUND

The pathophysiological mechanisms underlying chronic pruritic skin diseases, e.g. atopic dermatitis (AD), and effective therapies remain elusive due to the paucity of animal models. Recently, we rediscovered that injection of capsaicin into rat pups resulted in vigorous scratching behavior and chronically relapsing AD-like cutaneous lesions well into adulthood.

OBJECTIVES

To characterize the chronic pruritic dermatitis induced by neonatal capsaicin treatment.

METHODS

Capsaicin (50mg/kg) was given to rat pups subcutaneously within 48 h after birth, and then scratching behavior, dermatitis and pathophysiological changes of rat skin were investigated chronologically.

RESULTS

Neonatal capsaicin treatment led to not only severe scratching and cutaneous lesions but also a large number of pathophysiological changes in the skin, such as histopathological changes including the deficiency of epidermal filaggrin expression, increases in the number of mast cells, levels of tissue NGF and Th2 cytokine mRNA, impaired skin barrier function and colonization with S. aureus. In addition, we observed the hyperproduction of serum IgE, which is clinically similar to the pathophysiology seen in the patients with atopic dermatitis. During the follow-up observation, the rats showed the alternative periods of relapsing and remitting skin lesions.

CONCLUSION

Injection of capsaicin into rat pups results in chronically relapsing pruritic dermatitis, similar to human AD. Therefore, we think neonatal capsaicin treatment could be a useful model for studying human AD and for the development of novel therapeutic drugs.

摘要

背景

慢性瘙痒性皮肤病(如特应性皮炎[AD])的病理生理机制及其有效治疗方法仍难以捉摸,这是因为缺乏动物模型。最近,我们重新发现,向幼鼠皮内注射辣椒素会导致剧烈的搔抓行为,并在成年后长期反复出现类似 AD 的皮肤损伤。

目的

描述新生鼠接受辣椒素处理后诱发的慢性瘙痒性皮炎。

方法

在新生大鼠出生后 48 小时内,皮内给予辣椒素(50mg/kg),然后对搔抓行为、皮炎和大鼠皮肤的病理生理变化进行了系统的研究。

结果

新生鼠接受辣椒素处理不仅导致严重的搔抓和皮肤损伤,而且导致皮肤出现大量的病理生理变化,如组织学变化包括表皮丝聚合蛋白表达缺失、肥大细胞数量增加、组织神经生长因子和 Th2 细胞因子 mRNA 水平升高、皮肤屏障功能受损以及金黄色葡萄球菌定植。此外,我们观察到血清 IgE 的过度产生,这在临床上类似于特应性皮炎患者的病理生理学变化。在随访观察中,这些大鼠出现了反复发作和缓解的皮肤损伤交替期。

结论

向幼鼠皮内注射辣椒素会导致慢性反复发作的瘙痒性皮炎,类似于人类 AD。因此,我们认为新生鼠接受辣椒素处理可能是研究人类 AD 及开发新型治疗药物的有用模型。

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