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锂与银屑病:锂对培养淋巴细胞和银屑病角质形成细胞的细胞因子调节作用

Lithium and psoriasis: cytokine modulation of cultured lymphocytes and psoriatic keratinocytes by lithium.

作者信息

Ockenfels H M, Wagner S N, Keim-Maas C, Funk R, Nussbaum G, Goos M

机构信息

Department of Dermatology, University of Essen, Germany.

出版信息

Arch Dermatol Res. 1996 Apr;288(4):173-8. doi: 10.1007/BF02505220.

Abstract

The predominant cutaneous side effect of lithium is the exacerbation or aggravation of psoriasis, but the pathogenesis is still unclear. The hyperproliferation of keratinocytes and a dense lesional infiltrate of mononuclear cells are the hallmarks of psoriatic skin lesions. Interactions between keratinocytes and T cells are thought to be one reason for an increased secretion of proinflammatory cytokines and growth factors. To investigate whether lithium influences cytokines of the "psoriatic cytokine network', we established a coculture model with keratinocytes from psoriatic patients and from healthy controls cultured with HUT 78 lymphocytes and measured the cytokine levels of Il-2, Il-6, Il-8, IFN gamma and TGF alpha in the culture supernatants after treatment with lithium. Il-6 levels were slightly elevated in the supernatants obtained from psoriatic and control keratinocyte cultures after lithium treatment, but IFN gamma and Il-2 levels were elevated only in the lithium-treated cocultures with psoriatic keratinocytes. In contrast, these two cytokines were not affected by lithium in HUT 78 monocultures or in cocultures with normal epidermal cells. We also found slightly elevated TGF alpha levels in lithium-treated psoriatic cocultures but not in control cultures. We therefore demonstrated that lithium influences the cell communication of psoriatic keratinocytes with HUT 78 lymphocytes by triggering the secretion of TGF alpha, Il-2 and, massively, IFN gamma. It seems possible that lithium also influences similar parts of the psoriatic cytokine network in vivo.

摘要

锂的主要皮肤副作用是银屑病的加重,但发病机制仍不清楚。角质形成细胞的过度增殖和单核细胞密集的损伤浸润是银屑病皮肤病变的标志。角质形成细胞与T细胞之间的相互作用被认为是促炎细胞因子和生长因子分泌增加的一个原因。为了研究锂是否影响“银屑病细胞因子网络”中的细胞因子,我们建立了一个共培养模型,将银屑病患者和健康对照者的角质形成细胞与HUT 78淋巴细胞一起培养,并在锂处理后测量培养上清液中Il-2、Il-6、Il-8、IFNγ和TGFα的细胞因子水平。锂处理后,银屑病和对照角质形成细胞培养物获得的上清液中Il-6水平略有升高,但IFNγ和Il-2水平仅在锂处理的银屑病角质形成细胞共培养物中升高。相比之下,这两种细胞因子在HUT 78单培养物或与正常表皮细胞的共培养物中不受锂的影响。我们还发现锂处理的银屑病共培养物中TGFα水平略有升高,但对照培养物中没有。因此,我们证明锂通过触发TGFα、Il-2和大量IFNγ的分泌来影响银屑病角质形成细胞与HUT 78淋巴细胞的细胞通讯。锂似乎也可能在体内影响银屑病细胞因子网络的类似部分。

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