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血小板 P-选择素反映皮肤炎症状态:可能应用于监测银屑病的治疗效果。

Platelet P-selectin reflects a state of cutaneous inflammation: possible application to monitor treatment efficacy in psoriasis.

机构信息

Department of Dermatology, Clinic of the Goethe-University, Theodor-Stern-Kai 7, Frankfurt, Germany.

出版信息

Exp Dermatol. 2010 Aug;19(8):736-41. doi: 10.1111/j.1600-0625.2010.01095.x.

Abstract

Haemostasis-maintaining platelets are also recognized as important modulators in the regulation of immune response. Activated platelets expressing P-selectin (CD62P) are involved in the extravasation of leucocytes. This study evaluated platelet P-selectin expression as a biomarker for cutaneous inflammation. P-selectin expression was assessed by flow cytometry in 147 successive patients suffering from an inflammatory or infectious skin condition at the day of admission for in-patient treatment as well as a day prior to demission. Forty-one patients admitted for allergy testing served as controls. A commercially available ELISA was used in 17 patients to determine soluble P-selectin in the plasma. In patients with psoriasis, the Psoriasis Area and Severity Index (PASI) was documented as a measure for disease severity. We observed a significant increase in platelet P-selectin expression in patients with inflammatory or infectious disorders, when compared to the control group (3,01% vs. 1,46%; P < 0.000001). Successful treatment resulted in a significant decrease in P-selectin expression to the level of the control group. In the case of psoriasis (n = 47), we found highly significant correlation between P-selectin and PASI (r = 0.51; P < 0.000001), as well as between the change in the PASI and the change in P-selectin expression (r = 0.4; P = 0.006). Platelet P-selectin expression as determined by flow cytometry correlated well with the results of soluble P-selectin, determined by ELISA (r = 0.63; P < 0.01). Thus, platelet P-selectin expression may be used as an efficacy biomarker to monitor treatment success in psoriasis. As platelet P-selectin correlates with soluble P-selectin in patient plasma, which can be measured by ELISA, the latter is feasible also for routine use.

摘要

维持止血的血小板也被认为是调节免疫反应的重要调节剂。表达 P-选择素(CD62P)的活化血小板参与白细胞的渗出。本研究评估了血小板 P-选择素表达作为皮肤炎症的生物标志物。在入院接受住院治疗的 147 例炎症或感染性皮肤病患者以及出院前一天,通过流式细胞术评估血小板 P-选择素表达。41 例接受过敏测试的患者作为对照。在 17 例患者中使用商业上可获得的 ELISA 来确定血浆中可溶性 P-选择素。在银屑病患者中,记录银屑病面积和严重程度指数 (PASI) 作为疾病严重程度的指标。与对照组相比,我们观察到炎症或感染性疾病患者的血小板 P-选择素表达显著增加(3.01%比 1.46%;P<0.000001)。成功治疗导致 P-选择素表达显著降低至对照组水平。在银屑病(n=47)的情况下,我们发现 P-选择素与 PASI 之间存在高度显著相关性(r=0.51;P<0.000001),以及 PASI 的变化与 P-选择素表达的变化之间存在相关性(r=0.4;P=0.006)。流式细胞术测定的血小板 P-选择素表达与通过 ELISA 测定的可溶性 P-选择素结果高度相关(r=0.63;P<0.01)。因此,血小板 P-选择素表达可用作监测银屑病治疗成功的疗效生物标志物。由于血小板 P-选择素与患者血浆中的可溶性 P-选择素相关,而后者可通过 ELISA 测量,因此后者也可用于常规用途。

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