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缩小稳定同位素标记研究中来自小鼠和人类的 T 细胞寿命估计值之间的差距。

Closing the gap between T-cell life span estimates from stable isotope-labeling studies in mice and humans.

机构信息

Laboratory for Translational Immunology, University Medical Center Utrecht, Utrecht, The Netherlands;

出版信息

Blood. 2013 Sep 26;122(13):2205-12. doi: 10.1182/blood-2013-03-488411. Epub 2013 Aug 14.

Abstract

Quantitative knowledge of the turnover of different leukocyte populations is a key to our understanding of immune function in health and disease. Much progress has been made thanks to the introduction of stable isotope labeling, the state-of-the-art technique for in vivo quantification of cellular life spans. Yet, even leukocyte life span estimates on the basis of stable isotope labeling can vary up to 10-fold among laboratories. We investigated whether these differences could be the result of variances in the length of the labeling period among studies. To this end, we performed deuterated water-labeling experiments in mice, in which only the length of label administration was varied. The resulting life span estimates were indeed dependent on the length of the labeling period when the data were analyzed using a commonly used single-exponential model. We show that multiexponential models provide the necessary tool to obtain life span estimates that are independent of the length of the labeling period. Use of a multiexponential model enabled us to reduce the gap between human T-cell life span estimates from 2 previously published labeling studies. This provides an important step toward unambiguous understanding of leukocyte turnover in health and disease.

摘要

定量了解不同白细胞群体的周转率是理解健康和疾病中免疫功能的关键。由于引入了稳定同位素标记这一先进技术,我们得以在体内定量评估细胞寿命,因此在这方面取得了很大的进展。然而,即使基于稳定同位素标记的白细胞寿命估计值在不同实验室之间也可能相差 10 倍。我们研究了这些差异是否可能是由于研究之间标记期长度的差异造成的。为此,我们在小鼠中进行了氘水标记实验,其中仅改变了标记物的给予时间。当使用常用的单指数模型分析数据时,结果表明,当使用常用的单指数模型分析时,寿命估计值确实取决于标记期的长度。我们表明,多指数模型提供了获得与标记期长度无关的寿命估计值的必要工具。使用多指数模型使我们能够减少之前发表的两项标记研究中人类 T 细胞寿命估计值之间的差距。这朝着明确理解健康和疾病中的白细胞周转率迈出了重要的一步。

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