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接受慢性甲基强的松龙治疗的肾移植受者CD4+和CD8+淋巴细胞的24小时免疫学评估。

24-hour immunologic assessment of CD4+ and CD8+ lymphocytes in renal transplant recipients receiving chronic methylprednisolone.

作者信息

Tornatore K M, Reed K, Venuto R

机构信息

Department of Pharmacy Practice, School of Pharmacy, State University of New York at Buffalo, Erie County Medical Center 14260, USA.

出版信息

Clin Nephrol. 1995 Nov;44(5):290-8.

PMID:8605708
Abstract

Glucocorticoids are commonly prescribed in the post transplant period as a component of combination immunosuppressive regimens. However, the daily 24-hour pattern of helper lymphocytes (CD4+) and suppressor cells (CD8+) during chronic methylprednisolone therapy has not been examined in renal transplant recipients in relation to glucocorticoid exposure and time post-transplant. The response of total lymphocytes, CD4+ and CD8+ lymphocytes was examined in 23 stable renal transplant recipients who received methylprednisolone for at least 8 months post-transplant. The patient's prescribed oral methylprednisolone dose (mean daily dose = 9.7 +/- 2.6 mg) was given intravenously and whole blood was sampled periodically over 24 h for lymphocyte counts and methylprednisolone concentrations. A complete blood count with differential was determined via an automated hemocytometer with CD4+ and CD8+ lymphocytes determined using flow cytometry. Methylprednisolone area under the concentration versus time curve (AUC) was determined and normalized for each patient's respective dose. A general lymphopenia resulted in all patients with a mean decrease of 61 +/- 15% and an average nadir time occurring at 6 h. The decline from baseline was 76 +/- 17% for absolute number of CD4+ and 59 +/- 18% for CD8+ lymphocytes with an average nadir time at 6 h. Twelve patients exhibited a baseline CD4+ count to be less than 688 cells/mm3 (the low end of the reference range) and the lymphocyte count of all the patients fell below this value at the nadir. Six patients had a CD8+ lymphocyte count below 380 cells/mm3 (low end of the reference range) at baseline with 21 of the 23 patients exhibiting less than 380 cells/mm3 at the nadir time. At the time of nadir, the mean CD4+ and CD8+ counts were 156 +/- 105 cells/mm3 and 256 +/- 270 cells/mm3, respectively. In 17 of the 23 patients, the CD4+ count was below 200 cells/mm3 at the time of nadir. The dose-normalized AUC of methylprednisolone ranged from 22.6 to 113.5 ng.h/ml with 48% of patients exhibiting morning cortisol concentrations greater than 60 ng/ml. No correlation was noted between daily methylprednisolone exposure and the extent of lymphocyte decline. Lymphocyte response patterns are not clinically recognized in renal transplant recipients, as a means of monitoring immunosuppression. The absolute CD4+ and CD8+ lymphocyte count and the timing of these sample collections post-steroid administration, may have clinical relevance when serially assessed as is done in other immunologic diseases. Prospective evaluation of lymphocyte subset patterns and correlation with susceptibility to overimmunosuppressive (i.e. opportunistic infections) is necessary to help determine if these complications can be minimized by more individualized steroid dose modification.

摘要

糖皮质激素在移植后阶段通常作为联合免疫抑制方案的一部分被处方使用。然而,在肾移植受者中,慢性甲泼尼龙治疗期间辅助淋巴细胞(CD4+)和抑制细胞(CD8+)的每日24小时模式,尚未就糖皮质激素暴露情况和移植后时间进行研究。对23名稳定的肾移植受者进行了研究,这些受者在移植后接受甲泼尼龙治疗至少8个月,检测了总淋巴细胞、CD4+和CD8+淋巴细胞的反应。将患者规定的口服甲泼尼龙剂量(平均每日剂量 = 9.7 +/- 2.6毫克)静脉注射,在24小时内定期采集全血,用于淋巴细胞计数和甲泼尼龙浓度检测。通过自动血细胞计数器进行全血细胞计数及分类,使用流式细胞术测定CD4+和CD8+淋巴细胞。测定甲泼尼龙浓度-时间曲线下面积(AUC),并针对每位患者的各自剂量进行标准化。所有患者均出现一般性淋巴细胞减少,平均减少61 +/- 15%,平均最低点时间出现在6小时。CD4+绝对数量从基线下降76 +/- 17%,CD8+淋巴细胞下降59 +/- 18%,平均最低点时间为6小时。12名患者基线CD4+计数低于688个细胞/mm3(参考范围下限),所有患者的淋巴细胞计数在最低点时均低于该值。6名患者基线时CD8+淋巴细胞计数低于380个细胞/mm3(参考范围下限),23名患者中有21名在最低点时低于380个细胞/mm3。在最低点时,平均CD4+和CD8+计数分别为156 +/- 105个细胞/mm3和256 +/- 270个细胞/mm3。在23名患者中的17名,最低点时CD4+计数低于200个细胞/mm3。甲泼尼龙的剂量标准化AUC范围为22.6至113.5 ng.h/ml,48%的患者早晨皮质醇浓度大于60 ng/ml。未发现每日甲泼尼龙暴露与淋巴细胞下降程度之间存在相关性。在肾移植受者中,淋巴细胞反应模式未被临床认可为监测免疫抑制的一种手段。当像在其他免疫疾病中那样进行连续评估时,类固醇给药后绝对CD4+和CD8+淋巴细胞计数以及这些样本采集的时间,可能具有临床相关性。有必要对淋巴细胞亚群模式进行前瞻性评估,并与过度免疫抑制(即机会性感染)易感性进行相关性分析,以帮助确定是否可以通过更个体化的类固醇剂量调整将这些并发症降至最低。

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