Patients with sickle cell anemia (SCD) and pulmonary hypertension (PH) have a significantly increased risk of sudden death compared to patients with SCD alone. Sickled red blood cells (RBCs) are stiffer, more dense, more frequently undergo hemolysis, and have a sixfold shorter lifespan compared to normal RBCs. Here, we sought to investigate the impact of increased RBC stiffness, independent of other SCD-related biological and mechanical RBC abnormalities, on the hemodynamic changes that ultimately cause PH and increase mortality in SCD. To do so, pulmonary vascular impedance (PVZ) measures were recorded in control C57BL6 mice before and after ∼50 μl of blood (Hct = 45%) was extracted and replaced with an equal volume of blood containing either untreated RBCs or RBCs chemically stiffened with glutaraldehyde (Hct = 45%). Chemically stiffened RBCs increased mean pulmonary artery pressure (mPAP) (13.5 ± 0.6 mmHg at baseline to 23.2 ± 0.7 mmHg after the third injection), pulmonary vascular resistance (PVR) (1.23 ± 0.11 mmHg*min/ml at baseline to 2.24 ± 0.14 mmHg*min/ml after the third injection), and wave reflections (0.31 ± 0.02 at baseline to 0.43 ± 0.03 after the third injection). Chemically stiffened RBCs also decreased cardiac output, but did not change hematocrit, blood viscosity, pulmonary arterial compliance, or heart rate. The main finding of this study is that increased RBC stiffness alone affects pulmonary pulsatile hemodynamics, which suggests that RBC stiffness plays an important role in the development of PH in patients with SCD.
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February 2016
Research-Article
Increased Red Blood Cell Stiffness Increases Pulmonary Vascular Resistance and Pulmonary Arterial Pressure
David A. Schreier,
David A. Schreier
Department of Biomedical Engineering,
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706
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Omid Forouzan,
Omid Forouzan
Department of Biomedical Engineering,
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706
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Timothy A. Hacker,
Timothy A. Hacker
Department of Medicine,
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
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John Sheehan,
John Sheehan
Department of Medicine,
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
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Naomi Chesler
Naomi Chesler
Department of Biomedical Engineering,
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706;
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706;
Department of Medicine,
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
e-mail: chesler@engr.wisc.edu
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
e-mail: chesler@engr.wisc.edu
Search for other works by this author on:
David A. Schreier
Department of Biomedical Engineering,
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706
Omid Forouzan
Department of Biomedical Engineering,
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706
Timothy A. Hacker
Department of Medicine,
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
John Sheehan
Department of Medicine,
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
Naomi Chesler
Department of Biomedical Engineering,
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706;
University of Wisconsin,
2146 ECB, 1550 Engineering Drive,
Madison, WI 53706;
Department of Medicine,
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
e-mail: chesler@engr.wisc.edu
1685 Highland Avenue,
5158 Medical Foundation Centennial Building,
Madison, WI 53705-2281
e-mail: chesler@engr.wisc.edu
1Corresponding author.
Manuscript received August 3, 2015; final manuscript received November 30, 2015; published online January 27, 2016. Editor: Victor H. Barocas.
J Biomech Eng. Feb 2016, 138(2): 021012 (7 pages)
Published Online: January 27, 2016
Article history
Received:
August 3, 2015
Revised:
November 30, 2015
Citation
Schreier, D. A., Forouzan, O., Hacker, T. A., Sheehan, J., and Chesler, N. (January 27, 2016). "Increased Red Blood Cell Stiffness Increases Pulmonary Vascular Resistance and Pulmonary Arterial Pressure." ASME. J Biomech Eng. February 2016; 138(2): 021012. https://doi.org/10.1115/1.4032187
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