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首页> 外文期刊>Anticancer Research: International Journal of Cancer Research and Treatment >In vivo biological effects of pegfilgrastim after myelosuppressive chemotherapy in breast cancer.
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In vivo biological effects of pegfilgrastim after myelosuppressive chemotherapy in breast cancer.

机译:乳腺癌骨髓抑制化疗后使用培格非司亭的体内生物学效应。

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摘要

BACKGROUND: No exhaustive data are available on the in vivo biological effects of pegfilgrastim utilized in dose-dense chemotherapy (CT). The cytokinetic effects exerted in a multicyclic CT program by this cytokine on CD34+/38+ peripheral blood (PB) progenitor cells was the focus of this study. PATIENTS AND METHODS: PB samples from 19 breast cancer patients treated with 4 courses of docetaxel and epirubicin followed by pegfilgrastim were studied. The absolute number of CD34+/38+ circulating progenitor cells (CPCs) along with the percentage undergoing GO/G1, S and G2-M phases of the cell cycle or showing apoptotic features, were evaluated at baseline, after the first and before the fourth CT course using a dedicated flow cytometric technique. RESULTS AND CONCLUSION: Pegfilgrastim, after CT, exerted stimulatory effects on the cell cycle status of PB CD34+/38+ CPCs, at the same time protecting them from apoptosis. This was particularly evident 7 days after administration and tended to decrease one week later, without additional cytokinetic changes during the subsequent CT courses.
机译:背景:关于剂量密集型化疗(CT)中使用的pegfilgrastim的体内生物学作用,尚无详尽的数据。该细胞因子在多环CT程序中对CD34 + / 38 +外周血(PB)祖细胞产生的细胞动力学效应是本研究的重点。患者与方法:研究了19例乳腺癌患者的PB样品,这些患者接受了4个疗程的多西他赛和表柔比星治疗,随后接受了聚乙二醇非格司亭治疗。在基线,第一次和第四次之后,第四次之前评估CD34 + / 38 +循环祖细胞(CPC)的绝对数量,以及经历细胞周期GO / G1,S和G2-M阶段或显示凋亡特征的百分比使用专用的流式细胞仪技术进行CT扫描。结果与结论:吡格雷非司亭在CT后对PB CD34 + / 38 + CPCs的细胞周期状态具有刺激作用,同时保护其免于凋亡。给药后7天尤为明显,并在一周后趋于下降,在随后的CT疗程中没有其他细胞动力学变化。

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