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外周血祖细胞动员期间粒细胞集落刺激因子的血清药代动力学:根据中性粒细胞计数调整剂量可能会潜在地改善动员效果并更具成本效益。

G-CSF serum pharmacokinetics during peripheral blood progenitor cell mobilization: neutrophil count-adjusted dosage might potentially improve mobilization and be more cost-effective.

作者信息

Faulkner L B, Tucci F, Tamburini A, Tintori V, Lippi A A, Bambi F, Malentacca F, Azzari C, Gelli A M, Genovese F, Bernini G

机构信息

Department of Pediatrics, University of Florence, Ospedale Pediatrico A Meyer, Italy.

出版信息

Bone Marrow Transplant. 1998 Jun;21(11):1091-5. doi: 10.1038/sj.bmt.1701241.

DOI:10.1038/sj.bmt.1701241
PMID:9645570
Abstract

The optimal dosing schedule of G-CSF for peripheral blood progenitor cell (PBPC) mobilization is still under investigation although many centers use 10 microg/kg/day in a single subcutaneous dose. However, G-CSF clearance increases with increasing absolute neutrophil count (ANC). Hence a G-CSF dosage adjusted to ANC might be a reasonable approach. We measured G-CSF trough serum levels by sandwich ELISA assay at different ANCs in eight patients undergoing treatment with filgrastim at 10 microg/kg/day in a single subcutaneous dose. A total of 26 samples were analyzed, and a strong correlation between increasing ANC and decreasing G-CSF levels was found by linear regression analysis (P < 0.0003, r2 = 0.4199). For ANC values above 5000/microl the trough serum levels, ie 24 h after administration, were consistently below the level that provides maximal clonogenic precursor stimulation in vitro (10 ng/ml). Serial serum G-CSF measurements performed in three patients at 0, 3, 6, 9 and 24 h after G-CSF administration, showed a reduction of the area under the curve (AUC) with increasing ANC. For an ANC of 20000/microl or greater, the G-CSF serum level fell under the maximal in vitro stimulation threshold of 10 ng/ml within 12 h. This preliminary pharmacokinetic data seems to suggest that an ANC-adjusted G-CSF dosing schedule might improve the design of PBPC mobilization regimens.

摘要

尽管许多中心采用10微克/千克/天的单次皮下注射剂量来动员外周血祖细胞(PBPC),但粒细胞集落刺激因子(G-CSF)的最佳给药方案仍在研究中。然而,G-CSF的清除率会随着绝对中性粒细胞计数(ANC)的增加而升高。因此,根据ANC调整G-CSF剂量可能是一种合理的方法。我们采用夹心酶联免疫吸附测定法,对8例接受非格司亭10微克/千克/天单次皮下注射治疗的患者,在不同ANC水平下测量了G-CSF的谷血清水平。共分析了26个样本,通过线性回归分析发现ANC升高与G-CSF水平降低之间存在强相关性(P<0.0003,r2=0.4199)。对于ANC值高于5000/微升的情况,给药后24小时的谷血清水平始终低于体外提供最大克隆形成前体刺激的水平(10纳克/毫升)。对3例患者在G-CSF给药后0、3、6、9和24小时进行的连续血清G-CSF测量显示,随着ANC升高,曲线下面积(AUC)减小。对于ANC为20000/微升或更高的情况,G-CSF血清水平在12小时内降至体外最大刺激阈值10纳克/毫升以下。这些初步的药代动力学数据似乎表明,根据ANC调整G-CSF给药方案可能会改善PBPC动员方案的设计。

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