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在静脉注射甲基强的松龙治疗多发性硬化症期间,CD4亚群(CD45RA/RO)在增殖反应、白细胞介素-2和γ-干扰素产生方面存在差异。

CD4 subsets (CD45RA/RO) exhibit differences in proliferative responses, IL-2 and gamma-interferon production during intravenous methylprednisolone treatment of multiple sclerosis.

作者信息

Crockard A D, Treacy M T, Droogan A G, Hawkins S A

机构信息

Regional Immunology Laboratory, Royal Victoria Hospital, Queen's University of Belfast, Northern Ireland.

出版信息

J Neurol. 1996 Jun;243(6):475-81. doi: 10.1007/BF00900503.

Abstract

Phytohaemagglutinin (PHA)-induced proliferative responses, interleukin 2 (IL-2) and gamma-interferon production were determined in purified CD4CD45RA and CD4CD45RO lymphocytes isolated by immunomagnetic bead separations from normal subjects and multiple sclerosis (MS) patients. Significantly higher proliferative activities were observed for CD4CD45RA cells compared with the corresponding CD4CD45RO cell population in normal subjects and MS patients. CD4CD45RA lymphocyte proliferative responses declined by 50% 3 h following a single dose (500 mg) of intravenous methylprednisolone (IVMP). At 24 h, levels were similar to those determined pre-therapy, as were the levels observed 24 h after a 5-day course (500 mg daily) of IVMP. In contrast, CD4CD45RO cells were unaffected by IVMP. In vitro incorporation of methylprednisolone (10(-6) M) to cell cultures resulted in a modest reduction in proliferative activities of both CD4 subsets. In MS patients subnormal levels of IL-2 and gamma-interferon were observed in PHA-stimulated cultures of CD4CD45RA and CD4CD45RO cells. Following 5 days of IVMP therapy, IL-2 and gamma-interferon production was similar to that observed in CD4CD45RA and CD4CD45RO cells from normal subjects. IVMP therapy causes selective, but transient, inhibition of CD4CD45RA lymphocyte proliferative responses and enhancement of PHA-induced IL-2 and gamma-interferon production by both CD4CD45RA and CD4CD45RO cells.

摘要

采用免疫磁珠分离法从正常人和多发性硬化症(MS)患者中分离出纯化的CD4CD45RA和CD4CD45RO淋巴细胞,测定其对植物血凝素(PHA)诱导的增殖反应、白细胞介素2(IL-2)和γ干扰素的产生。与正常人和MS患者相应的CD4CD45RO细胞群体相比,观察到CD4CD45RA细胞具有显著更高的增殖活性。单次静脉注射甲基强的松龙(IVMP,500 mg)后3小时,CD4CD45RA淋巴细胞的增殖反应下降了50%。在24小时时,其水平与治疗前测定的水平相似,5天疗程(每日500 mg)的IVMP治疗后24小时观察到的水平也是如此。相比之下,CD4CD45RO细胞不受IVMP影响。将甲基强的松龙(10(-6) M)加入细胞培养物中,导致两个CD4亚群的增殖活性适度降低。在MS患者中,在PHA刺激的CD4CD45RA和CD4CD45RO细胞培养物中观察到IL-2和γ干扰素水平低于正常。IVMP治疗5天后,IL-2和γ干扰素的产生与正常受试者的CD4CD45RA和CD4CD45RO细胞中观察到的情况相似。IVMP治疗可选择性但短暂地抑制CD4CD45RA淋巴细胞的增殖反应,并增强PHA诱导的CD4CD45RA和CD4CD45RO细胞产生IL-2和γ干扰素。

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