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首页> 外文期刊>Journal of molecular medicine: Official organ of the "Gesellschaft Deutscher Naturforscher und Arzte." >Early central vs. peripheral immunological and neurobiological effects of fingolimod-a longitudinal study
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Early central vs. peripheral immunological and neurobiological effects of fingolimod-a longitudinal study

机译:中部中部与外周免疫和神经生物学作用Fingolimod-A纵向研究

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Fingolimod (FTY) is known to have multiple effects on the immune system and the central nervous system (CNS) in patients with multiple sclerosis (MS). In this study, we evaluated the immunological and neurobiological effects of FTY in MS. Blood and cerebrospinal fluid (CSF) samples were collected from 15 MS patients before first FTY administration and after 4 months of FTY therapy. Immunophenotyping and evaluation of sphingosine-1-phosphate (S1P), neurofilament light chain (NFL), S-100 and neuron-specific enolase (NSE) levels were conducted. After 4 months of FTY therapy, absolute cell count in CSF was decreased from 6.33 to 2.43 MPt/l, accompanied by decreases of CD3+ (2.22 to 0.65 MPt/l) and of CD4+ counts (1.60 to 0.39 MPt/l). In blood, CD3+ (1.05 to 0.09 GPt/l), CD4+ (0.80 to 0.02 GPt/l), CD8+ (0.23 to 0.04 GPt/l) and CD19+ (0.21 to 0.01GPt/l) cell counts were as well reduced. CD14+ cell count remained stable over the same period (0.24 to 0.26GPt/l). NFL and S1P levels in CSF and blood were reduced over time (NFL: CSF 1759 to 1359 pg/l, blood 8.42 to 7.36 pg/l; S1P: CSF 2.12 to 0.71 nmol/l, blood 392.1 to 312.9 nmol/l). Strong correlations between CSF and blood NFL levels were observed. Neuronal damage markers such as S-100 (1.86 to 1.69 mu g/l) and NSE (9.53 to 8.67 mu g/l) were reduced to a lesser degree than other markers. FTY exerted significant effects on immunological and neurobiological markers in the central and peripheral compartment. Decreases in levels of neuroinflammatory and neurodegenerative markers were already evident after 4 months of treatment. Four-month serum NFL level appears to be a useful marker for FTY efficacy that correlates well with changes in the CNS compartment. Key messages
机译:众所周知,Fingolimod(FTY)对多发性硬化症(MS)的患者对免疫系统和中枢神经系统(CNS)具有多种影响。在这项研究中,我们评估了MS中FTY的免疫学和神经生物学作用。在第一次FTY给药前和4个月后从15毫秒患者中收集血液和脑脊髓液(CSF)样品。对鞘氨醇-1-磷酸(S1P),神经膜轻链(NFL),S-100和神经元特异性烯醇酶(NSE)水平进行免疫蛋白酶型和评价。在4个月的FTY疗法后,CSF中的绝对细胞计数从6.33降至2.43mpt / L,伴随着CD3 +(2.22至0.65mpt / L)和CD4 +计数(1.60至0.39mpt / L)。在血液中,CD3 +(1.05至0.09 GPT / L),CD4 +(0.80至0.02 GPT / L),CD8 +(0.23至0.04 GPT / L)和CD19 +(0.21至0.01GPT / L)细胞计数也降低。 CD14 +细胞计数在同一时期保持稳定(0.24至0.26gpt / l)。随着时间的推移,CSF和血液中的NFL和S1P水平(NFL:CSF 1759至1359 pg / L,血液8.42至7.36 pg / L; S1P:CSF 2.12至0.71 nmol / L,血液392.1至312.9 nmol / L)。观察到CSF和血液NFL水平之间的强相关性。诸如S-100(1.86至1.69μg)和NSE(9.53至8.67μg/ L)的神经元损伤标记减少到比其他标志物的较小程度。对于中央和周边隔室中的免疫和神经生物学标志物产生显着影响。在治疗4个月后,神经炎性和神经变性标记的水平降低已经明显。四个月的血清NFL水平似乎是有用的标记,用于与CNS隔间的变化相比好相关的效能。关键信息

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