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In Vivo Volume and Hemoglobin Dynamics of Human Red Blood Cells

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2014

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Public Library of Science
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Malka, Roy, Francisco Feijó Delgado, Scott R. Manalis, and John M. Higgins. 2014. “In Vivo Volume and Hemoglobin Dynamics of Human Red Blood Cells.” PLoS Computational Biology 10 (10): e1003839. doi:10.1371/journal.pcbi.1003839. http://dx.doi.org/10.1371/journal.pcbi.1003839.

Abstract

Human red blood cells (RBCs) lose ∼30% of their volume and ∼20% of their hemoglobin (Hb) content during their ∼100-day lifespan in the bloodstream. These observations are well-documented, but the mechanisms for these volume and hemoglobin loss events are not clear. RBCs shed hemoglobin-containing vesicles during their life in the circulation, and this process is thought to dominate the changes in the RBC physical characteristics occurring during maturation. We combine theory with single-cell measurements to investigate the impact of vesiculation on the reduction in volume, Hb mass, and membrane. We show that vesicle shedding alone is sufficient to explain membrane losses but not volume or Hb losses. We use dry mass measurements of human RBCs to validate the models and to propose that additional unknown mechanisms control volume and Hb reduction and are responsible for ∼90% of the observed reduction. RBC population characteristics are used in the clinic to monitor and diagnose a wide range of conditions including malnutrition, inflammation, and cancer. Quantitative characterization of cellular maturation processes may help in the early detection of clinical conditions where maturation patterns are altered.

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Biology and Life Sciences, Anatomy, Body Fluids, Blood, Blood Counts, Hematocrit, Blood Volume, Biophysics, Computational Biology, Population Modeling, Physiology, Hematopoietic System, Population Biology, Population Dynamics, Systems Biology, Integrative Physiology, Theoretical Biology, Medicine and Health Sciences, Hematology, Physical Sciences, Mathematics, Probability Theory, Markov Processes, Stochastic Processes

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