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红细胞内稳态的发育可塑性。

Developmental plasticity of red blood cell homeostasis.

机构信息

Department of Environmental Toxicology, University of California Davis, Davis, California; California National Primate Research Center, University of California Davis, Davis, California.

出版信息

Am J Hematol. 2014 May;89(5):459-66. doi: 10.1002/ajh.23666. Epub 2014 Mar 3.

Abstract

Most human physiologic set points like body temperature are tightly regulated and show little variation between healthy individuals. Red blood cell (RBC) characteristics such as hematocrit and mean cell volume are stable within individuals but can vary by 20% from one healthy person to the next. The mechanisms for the majority of this inter-individual variation are unknown and do not appear to involve common genetic variation. Here, we show that environmental conditions present during development, namely in utero iron availability, can exert long-term influence on a set point related to the RBC life cycle. In a controlled study of rhesus monkeys and a retrospective study of humans, we use a mathematical model of in vivo RBC population dynamics to show that in utero iron deficiency is associated with a lowered threshold for RBC clearance and turnover. This in utero effect is plastic, persisting at least 2 years after birth and after the cessation of iron deficiency. Our study reports a rare instance of developmental plasticity in the human hematologic system and also shows how mathematical modeling can be used to identify cellular mechanisms involved in the adaptive control of homeostatic set points.

摘要

大多数人体生理平衡点,如体温,都受到严格的调节,在健康个体之间几乎没有差异。红细胞(RBC)的特征,如血细胞比容和平均细胞体积,在个体内部是稳定的,但在个体之间可能会有 20%的差异。大多数这种个体间差异的机制尚不清楚,似乎不涉及常见的遗传变异。在这里,我们表明,发育过程中存在的环境条件,即宫内铁的可用性,可以对与 RBC 生命周期相关的设定点产生长期影响。在恒河猴的对照研究和人类的回顾性研究中,我们使用体内 RBC 群体动力学的数学模型表明,宫内铁缺乏与 RBC 清除和周转率的降低阈值有关。这种宫内作用是可塑的,至少在出生后 2 年,以及缺铁停止后仍然存在。我们的研究报告了人类血液系统中罕见的发育可塑性实例,也展示了数学建模如何用于识别参与稳态设定点自适应控制的细胞机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8c1e/4086753/823cc2e13824/nihms600781f1.jpg

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Developmental plasticity of red blood cell homeostasis.红细胞内稳态的发育可塑性。
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