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首页> 外文期刊>Arthritis research & therapy. >A set of serum markers detecting systemic inflammation in psoriatic skin, entheseal, and joint disease in the absence of C-reactive protein and its link to clinical disease manifestations
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A set of serum markers detecting systemic inflammation in psoriatic skin, entheseal, and joint disease in the absence of C-reactive protein and its link to clinical disease manifestations

机译:在没有C-反应蛋白质的情况下检测银屑病皮肤,肠杆菌和联合疾病中的全身炎症的一套血清标志物及其与临床疾病表现的联系

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C-reactive protein (CRP) is often normal in patients with psoriatic disease. Herein, we aimed to define markers of systemic inflammation in patients with monomorphic and polymorphic psoriatic skin, entheseal, and joint disease. Three-step approach: (i) selection of serum markers elevated in psoriatic arthritis compared healthy controls from a panel of 10 different markers reflecting the pathophysiology of psoriatic disease; (ii) testing of these selected markers as well as C-reactive protein (CRP) in a larger cohort of 210 individuals- 105 healthy controls and 105 patients with psoriatic disease with either monomorphic skin (S), entheseal (E) or joint (A) involvement or polymorphic disease with various combinations of skin, entheseal and joint disease (SE, SA, EA, SEA); (iii) testing whether tumor necrosis factor (TNF) and interleukin (IL)-17 inhibitor therapy normalizes these markers. CRP was not elevated or was rarely elevated in the subgroups (S 0%, E 0%, A 20%, SE 7%, SA 33%, EA 27%, SEA 33%) despite active psoriatic disease. In sharp contrast, beta-defensin 2 and lipocalin-2 levels were elevated in the majority of patients with monomorphic skin (93% and 73%) and entheseal (both 53%), but not joint disease (27% and 20%). Conversely, elevations of calprotectin and IL-8 were found in the majority of patients with monomorphic joint disease (both 73%). IL-22 was elevated in all three monomorphic disease manifestations (S 60%, E 46%; A 60%). Furthermore, the vast majority of patients with polymorphic psoriatic disease (SE, SA, EA, SEA) showed widespread marker elevation. IL-17- and TNF inhibitor treatment significantly lowered all 5 markers of inflammation in PsA patients. Systemic inflammation is detectable in the majority of patients with psoriatic disease, even if CRP is normal. The respective marker pattern depends on the manifestation of psoriatic disease with respect to skin, entheseal, and joint involvement.
机译:在银屑病患者中,C反应蛋白(CRP)通常是正常的。在此,我们旨在确定单数和多晶型银屑病皮肤,患者和关节疾病患者的全身炎症的标志物。三步方法:(i)在银屑病关节炎中升高的血清标记的选择与反映银屑病病理生理学的10个不同标记的面板比较了健康对照; (ii)在较大的210个体 - 105个健康对照组和105例患有单组织皮肤,entheseal(E)或关节(e),entheseal(e)或关节( a)具有各种皮肤,肠杆菌和联合疾病组合的参与或多态疾病(SE,SA,EA,Sea); (iii)测试肿瘤坏死因子(TNF)和白细胞介素(IL)-17抑制剂治疗是否标准化这些标志物。尽管有活跃的银屑病疾病,CRP在亚组中未升高或很少升高或在亚组中较少升高,亚群,0%,20%,SE,23%,SEA 33%)。在鲜明的对比度下,β-防御素2和脂蛋白-2水平在大多数患有单数皮肤(93%和73%)和肠杆菌(53%)的患者中升高,但不是关节疾病(27%和20%)。相反,在大多数单数关节疾病(73%)的大多数患者中发现了CalProtectin和IL-8的升高。 IL-22在所有三种单组态疾病表现中升高(60%,E 46%; 60%)。此外,绝大多数具有多态性银屑病疾病(SE,SA,EA,海)的患者显示出广泛的标记升高。 IL-17-和TNF抑制剂治疗显着降低了PSA患者中的所有5种炎症标记。即使CRP是正常的,大多数患者的大多数患者都可以检测到全身炎症。相应的标记模式取决于对皮肤,肠道和关节参与的银屑病疾病的表现。

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