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Red blood cell lingering modulates hematocrit distribution in the microcirculation

View ORCID ProfileYazdan Rashidi, View ORCID ProfileGreta Simionato, View ORCID ProfileQi Zhou, View ORCID ProfileThomas John, View ORCID ProfileAlexander Kihm, Mohammed Bendaoud, Timm Krüger, View ORCID ProfileMiguel O. Bernabeu, View ORCID ProfileLars Kaestner, View ORCID ProfileMatthias W. Laschke, View ORCID ProfileMichael D. Menger, View ORCID ProfileChristian Wagner, View ORCID ProfileAlexis Darras
doi: https://doi.org/10.1101/2022.08.16.504126
Yazdan Rashidi
1Experimental Physics, Saarland University, 66123 Saarbruecken, Germany
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  • For correspondence: yazdan.rashidi@uni-saarland.de alexis.darras@uni-saarland.de
Greta Simionato
1Experimental Physics, Saarland University, 66123 Saarbruecken, Germany
2Institute for Clinical and Experimental Surgery, Saarland University, 66421 Homburg, Germany
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Qi Zhou
3School of Engineering, Institute for Multiscale Thermofluids, University of Edinburgh, Edinburgh EH9 3FD, United Kingdom
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Thomas John
1Experimental Physics, Saarland University, 66123 Saarbruecken, Germany
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Alexander Kihm
1Experimental Physics, Saarland University, 66123 Saarbruecken, Germany
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  • ORCID record for Alexander Kihm
Mohammed Bendaoud
1Experimental Physics, Saarland University, 66123 Saarbruecken, Germany
4Université Grenoble Alpes, CNRS, LIPhy, F-38000 Grenoble, France
5LaMCScI, Faculty of Sciences, Mohammed V University of Rabat, Rabat 1014, Morocco
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Timm Krüger
3School of Engineering, Institute for Multiscale Thermofluids, University of Edinburgh, Edinburgh EH9 3FD, United Kingdom
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Miguel O. Bernabeu
6Centre for Medical Informatics, Usher Institute, University of Edinburgh, Edinburgh EH16 4UX, United Kingdom
7The Bayes Centre, The University of Edinburgh, Edinburgh EH8 9BT, United Kingdom
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Lars Kaestner
1Experimental Physics, Saarland University, 66123 Saarbruecken, Germany
8Theoretical Medicine and Biosciences, Saarland University, 66421 Homburg, Germany
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Matthias W. Laschke
2Institute for Clinical and Experimental Surgery, Saarland University, 66421 Homburg, Germany
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Michael D. Menger
2Institute for Clinical and Experimental Surgery, Saarland University, 66421 Homburg, Germany
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Christian Wagner
1Experimental Physics, Saarland University, 66123 Saarbruecken, Germany
9Physics and Materials Science Research Unit, University of Luxembourg, L-1511 Luxembourg, Luxembourg
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Alexis Darras
1Experimental Physics, Saarland University, 66123 Saarbruecken, Germany
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  • For correspondence: yazdan.rashidi@uni-saarland.de alexis.darras@uni-saarland.de
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Abstract

The distribution of red blood cells (RBCs) in the microcirculation determines the oxygen delivery and solute transport to tissues. This process relies on the partitioning of RBCs at successive bifurcations throughout the microvascular network and it is known since the last century that RBCs partition disproportionately to the fractional blood flow rate, therefore leading to heterogeneity of the hematocrit (i.e. volume fraction of RBCs in blood) in microvessels. Usually, downstream of a microvascular bifurcation, the vessel branch with a higher fraction of blood flow receives an even higher fraction of RBC flux. However, both temporal and time-average deviations from this phaseseparation law have been observed in recent works. Here, we quantify how the microscopic behavior of RBCs lingering (i.e. RBCs temporarily residing near the bifurcation apex with diminished velocity) influences their partitioning, through combined in vivo experiments and in silico simulations. We developed an approach to quantify the cell lingering at highly-confined capillary-level bifurcations and demonstrate that it correlates with deviations of the phase-separation process from established empirical predictions by Pries et al. Furthermore, we shed light on how the bifurcation geometry and cell membrane rigidity can affect the lingering behavior of RBCs, e.g. rigid cells tend to linger less than softer ones. Taken together, RBC lingering is an important mechanism that should be considered when studying how abnormal RBC rigidity in diseases such as malaria and sickle-cell disease could hinder the microcirculatory blood flow or how the vascular networks are altered under pathological conditions (e.g. thrombosis, aneurysm).

Competing Interest Statement

The authors have declared no competing interest.

Footnotes

  • Minor update in figures and spellchecking.

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The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. All rights reserved. No reuse allowed without permission.
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Posted August 31, 2022.
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Red blood cell lingering modulates hematocrit distribution in the microcirculation
Yazdan Rashidi, Greta Simionato, Qi Zhou, Thomas John, Alexander Kihm, Mohammed Bendaoud, Timm Krüger, Miguel O. Bernabeu, Lars Kaestner, Matthias W. Laschke, Michael D. Menger, Christian Wagner, Alexis Darras
bioRxiv 2022.08.16.504126; doi: https://doi.org/10.1101/2022.08.16.504126
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Red blood cell lingering modulates hematocrit distribution in the microcirculation
Yazdan Rashidi, Greta Simionato, Qi Zhou, Thomas John, Alexander Kihm, Mohammed Bendaoud, Timm Krüger, Miguel O. Bernabeu, Lars Kaestner, Matthias W. Laschke, Michael D. Menger, Christian Wagner, Alexis Darras
bioRxiv 2022.08.16.504126; doi: https://doi.org/10.1101/2022.08.16.504126

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