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多发性硬化症中的凝血因子 XII 水平与内源性凝血酶生成

Coagulation Factor XII Levels and Intrinsic Thrombin Generation in Multiple Sclerosis.

作者信息

Ziliotto Nicole, Baroni Marcello, Straudi Sofia, Manfredini Fabio, Mari Rosella, Menegatti Erica, Voltan Rebecca, Secchiero Paola, Zamboni Paolo, Basaglia Nino, Marchetti Giovanna, Bernardi Francesco

机构信息

Department of Life Sciences and Biotechnology, University of Ferrara, Ferrara, Italy.

Neuroscience and Rehabilitation Department, Ferrara University Hospital, Ferrara, Italy.

出版信息

Front Neurol. 2018 Apr 20;9:245. doi: 10.3389/fneur.2018.00245. eCollection 2018.

Abstract

BACKGROUND

Factor XII (FXII) activation initiates the intrinsic (contact) coagulation pathway. It has been recently suggested that FXII could act as an autoimmunity mediator in multiple sclerosis (MS). FXII depositions nearby dentritic cells were detected in the central nervous system of MS patients and increased FXII activity has been reported in plasma of relapsing remitting and secondary progressive MS patients. FXII inhibition has been proposed to treat MS.

OBJECTIVE

To investigate in MS patients multiple FXII-related variables, including the circulating amount of protein, its pro-coagulant function, and their variation over time. To explore kinetic activation features of FXII in thrombin generation (TG).

METHODS

In plasma from 74 MS patients and 49 healthy subjects (HS), FXII procoagulant activity (FXII:c) and FXII protein (FXII:Ag) levels were assessed. Their ratio (FXII:ratio) values were derived. Intrinsic TG was evaluated by different triggers.

RESULTS

Higher FXII:Ag levels ( = 0.003) and lower FXII:ratio ( < 0.001) were detected in MS patients compared with HS. FXII variables were highly correlated over four time points, which supports investigation of FXII contribution to disease phenotype and progression. A significant difference over time was detected for FXII:c ( = 0.031). In patients selected for the lowest FXII:ratio, TG triggered by ellagic acid showed a trend in lower endogenous thrombin potential (ETP) in MS patients compared with HS ( = 0.042). Intrinsic triggering of TG by nucleic acid addition produced longer time parameters in patients than in HS and substantially increased ETP in MS patients ( = 0.004) and TG peak height in HS ( = 0.008). Coherently, lower FXII:ratio and longer lag time ( = 0.02) and time to peak ( = 0.007) point out a reduced response of FXII to activation in part of MS patients.

CONCLUSION

In MS patients, factor-specific and modified global assays suggest the presence of increased FXII protein level and reduced function within the intrinsic coagulation pathway. These novel findings support further investigation by multiple approaches of FXII contribution to disease phenotype and progression.

摘要

背景

凝血因子 XII(FXII)的激活启动了内源性(接触)凝血途径。最近有研究表明,FXII 可能在多发性硬化症(MS)中作为自身免疫介质发挥作用。在 MS 患者的中枢神经系统中检测到树突状细胞附近有 FXII 沉积,并且在复发缓解型和继发进展型 MS 患者的血浆中报告了 FXII 活性增加。有人提出抑制 FXII 来治疗 MS。

目的

研究 MS 患者中多个与 FXII 相关的变量,包括蛋白质的循环量、其促凝血功能以及它们随时间的变化。探讨 FXII 在凝血酶生成(TG)中的动力学激活特征。

方法

评估了 74 例 MS 患者和 49 例健康受试者(HS)血浆中的 FXII 促凝血活性(FXII:c)和 FXII 蛋白(FXII:Ag)水平。得出它们的比值(FXII:比值)。通过不同的触发因素评估内源性 TG。

结果

与 HS 相比,MS 患者中检测到更高的 FXII:Ag 水平(=0.003)和更低的 FXII:比值(<0.001)。FXII 变量在四个时间点高度相关,这支持研究 FXII 对疾病表型和进展的贡献。检测到 FXII:c 随时间有显著差异(=0.031)。在选择 FXII:比值最低的患者中,与 HS 相比,由鞣花酸触发的 TG 在 MS 患者中显示出较低的内源性凝血酶潜力(ETP)趋势(=0.042)。通过添加核酸对 TG 进行内源性触发在患者中产生的时间参数比在 HS 中更长,并且在 MS 患者中显著增加了 ETP(=0.004),在 HS 中增加了 TG 峰值高度(=0.008)。一致地,较低的 FXII:比值以及较长的滞后时间(=0.02)和达到峰值的时间(=0.007)表明部分 MS 患者中 FXII 对激活的反应降低。

结论

在 MS 患者中,因子特异性和改良的整体检测表明内源性凝血途径中存在 FXII 蛋白水平升高和功能降低的情况。这些新发现支持通过多种方法进一步研究 FXII 对疾病表型和进展的贡献。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8f87/5919941/525688f92917/fneur-09-00245-g001.jpg

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