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Human neutrophil kinetics: modeling of stable isotope labeling data supports short blood neutrophil half-lives

机译:人类嗜中性粒细胞动力学:稳定同位素标记数据的建模支持短血嗜中性粒细胞半衰期

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摘要

Human neutrophils have traditionally been thought to have a short half-life in blood; estimates vary from 4 to 18 hours. This dogma was recently challenged by stable isotope labeling studies with heavy water, which yielded estimates in excess of 3 days. To investigate this disparity, we generated new stable isotope labeling data in healthy adult subjects using both heavy water (n = 4) and deuterium-labeled glucose (n = 9), a compound with more rapid labeling kinetics. To interpret results, we developed a novel mechanistic model and applied it to previously published (n = 5) and newly generated data. We initially constrained the ratio of the blood neutrophil pool to the marrow precursor pool (ratio = 0.26; from published values). Analysis of heavy water data sets yielded turnover rates consistent with a short blood half-life, but parameters, particularly marrow transit time, were poorly defined. Analysis of glucose-labeling data yielded more precise estimates of half-life (0.79 ± 0.25 days; 19 hours) and marrow transit time (5.80 ± 0.42 days). Substitution of this marrow transit time in the heavy water analysis gave a better-defined blood half-life of 0.77 ± 0.14 days (18.5 hours), close to glucose-derived values. Allowing the ratio of blood neutrophils to mitotic neutrophil precursors (R) to vary yielded a best-fit value of 0.19. Reanalysis of the previously published model and data also revealed the origin of their long estimates for neutrophil half-life: an implicit assumption that R is very large, which is physiologically untenable. We conclude that stable isotope labeling in healthy humans is consistent with a blood neutrophil half-life of less than 1 day.
机译:传统上认为人类嗜中性粒细胞在血液中的半衰期很短。估计从4到18小时不等。这种教条最近受到重水稳定同位素标记研究的挑战,该研究得出的估计超过3天。为了研究这种差异,我们使用重水(n = 4)和氘标记的葡萄糖(n = 9)(一种具有更快标记动力学的化合物)在健康成人受试者中产生了新的稳定同位素标记数据。为了解释结果,我们开发了一种新颖的机械模型并将其应用于先前发布的数据(n = 5)和新生成的数据。我们最初限制了血液中性粒细胞池与骨髓前体池的比率(比率= 0.26;根据已公布的值)。对重水数据集的分析得出的周转率与血液半衰期短相符,但参数(尤其是骨髓通过时间)定义不明确。对葡萄糖标记数据的分析得出了更精确的半衰期(0.79±0.25天; 19小时)和骨髓转运时间(5.80±0.42天)的估计值。在重水分析中取代该骨髓转运时间可得到更精确的血液半衰期,为0.77±0.14天(18.5小时),接近于葡萄糖衍生的值。允许血液中性粒细胞与有丝分裂中性粒细胞前体(R)的比率发生变化时,最佳拟合值为0.19。对先前发表的模型和数据的重新分析也揭示了他们对嗜中性粒细胞半衰期的长期估计的起源:一个隐含的假设,即R很大,这在生理上是站不住脚的。我们得出的结论是,健康人体内稳定的同位素标记与血液中性粒细胞的半衰期少于1天一致。

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