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银屑病中的一种环磷酸腺苷结合异常。

A cAMP binding abnormality in psoriasis.

作者信息

Raynaud F, Gerbaud P, Enjolras O, Gorin I, Donnadieu M, Anderson W B, Evain-Brion D

机构信息

Laboratoire de Physiopathologie du Développement, CNRS-Ecole Normale Supérieure, Bethesda, Maryland.

出版信息

Lancet. 1989 May 27;1(8648):1153-6. doi: 10.1016/s0140-6736(89)92748-7.

Abstract

In 34 psoriatic patients with various cutaneous manifestations (psoriasis vulgaris, erythroderma psoriaticum, guttate psoriasis), the ability of the RI regulatory subunit of cAMP-dependent protein kinase (PKA) to bind a cAMP analogue (8-azido [32P] cAMP) in erythrocyte membranes was significantly lower than that in 19 normal subjects (mean [SEM] 565 [35] vs 930 [35] fmol/mg protein). This enzyme defect was not found in patients with other forms of dermatitis that can be confused with psoriasis or with other inflammatory diseases. There was a significant negative correlation between the severity of the disease as expressed by the psoriatic area and severity index score and the binding of the cAMP analogue to PKA. A long-term study showed that oral retinoid treatment of psoriatic patients resulted in a correction of the binding defect. Unaffected members of psoriatic families had significantly lower than normal binding of cAMP to PKA (773 [60] fmol/mg protein). This study shows for the first time that in psoriasis a biochemical defect expressed in erythrocytes correlates with the severity of the disease as well as its clinical evolution. These results will be useful in clinical management of psoriatic disease for the choice and follow-up of retinoid therapy.

摘要

在34例有各种皮肤表现(寻常型银屑病、红皮病型银屑病、点滴状银屑病)的银屑病患者中,红细胞膜中依赖环磷酸腺苷(cAMP)的蛋白激酶(PKA)的RI调节亚基与cAMP类似物(8-叠氮基[32P]cAMP)结合的能力显著低于19名正常受试者(平均值[标准误]565[35]对930[35]fmol/mg蛋白)。在其他可与银屑病混淆的皮炎形式患者或其他炎症性疾病患者中未发现这种酶缺陷。银屑病面积和严重程度指数评分所表示的疾病严重程度与cAMP类似物与PKA的结合之间存在显著负相关。一项长期研究表明,对银屑病患者进行口服维甲酸治疗可纠正结合缺陷。银屑病家族中未受影响的成员cAMP与PKA的结合显著低于正常水平(773[60]fmol/mg蛋白)。这项研究首次表明,银屑病中红细胞中表现出的生化缺陷与疾病严重程度及其临床演变相关。这些结果将有助于银屑病疾病的临床管理中维甲酸治疗的选择和随访。

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