Bugelski Peter J, Nesspor Thomas, Volk Amy, O'Brien Joanne, Makropoulos Dorie, Shamberger Kim, Fisher Paul W, James Ian, Graden Danielle, Capocasale Renold J
Discovery Research, Centocor Research & Development, Inc., Radnor, SP 19087, USA.
Pharm Res. 2008 Feb;25(2):369-78. doi: 10.1007/s11095-007-9372-7. Epub 2007 Jul 4.
Originally approved for three times/week dosing, recombinant human erythropoietin (rhEPO) is now often used at weekly intervals. We have studied rhEPO in mice to better understand why the extended dosing interval retains efficacy.
C57Bl/6 mice received a single sc. dose of rhEPO (3,000 IU/kg). Bone marrow and blood were collected at 8 h and 1, 2, 5 and 7 days. Staining for TER-119 and CD71, pulse labeling with bromodeoxyuridine, annexin-V binding and vital staining with 7-aminoactinomycin D: were used cell cycle and apoptosis in erythroblasts by four color flow cytometry.
A wave of proliferation and/or maturation progressed through all erythroblasts, resulting in the emigration of immature reticulocytes into the periphery. An increase in the fraction of erythroblasts in S and G2M was found, but suppression of apoptosis was not.
Most of the effects of rhEPO occurred 48 h after dosing, when the concentration of rhEPO was less than 1% of Cmax, suggesting that the processes set in motion by rhEPO can continue after rhEPO concentrations fall. Our observation of apoptosis in erythroblasts even when rhEPO concentrations were high suggests that regulatory mechanisms which down-regulate erythropoiesis are also engaged.
重组人促红细胞生成素(rhEPO)最初获批的给药方案为每周3次,现在常按每周一次的间隔给药。我们在小鼠中研究了rhEPO,以更好地理解延长给药间隔仍能保持疗效的原因。
C57Bl/6小鼠单次皮下注射rhEPO(3000 IU/kg)。在8小时以及1、2、5和7天时采集骨髓和血液。使用TER-119和CD71染色、溴脱氧尿苷脉冲标记、膜联蛋白-V结合以及7-氨基放线菌素D活体染色,通过四色流式细胞术分析成红细胞的细胞周期和凋亡情况。
一波增殖和/或成熟过程贯穿所有成红细胞,导致未成熟网织红细胞向外周迁移。发现S期和G2M期成红细胞的比例增加,但凋亡未受抑制。
rhEPO的大多数作用在给药后48小时出现,此时rhEPO的浓度低于Cmax的1%,这表明rhEPO引发的过程在rhEPO浓度下降后仍可继续。即使rhEPO浓度较高时我们仍观察到成红细胞凋亡,这表明下调红细胞生成的调节机制也在发挥作用。
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