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Article type: Research Article
Authors: Reinhart, Walter H.
Affiliations: Department of Internal Medicine, Kantonsspital, Chur, Switzerland
Note: [] Address for correspondence: Walter H. Reinhart, MD, Department of Internal Medicine, Kantonsspital, CH‐7000 Chur, Switzerland. Tel.: +41 81 256 6305; Fax: +41 81 256 6381; E‐mail: walter.reinhart@ksc.gr.ch.
Abstract: Blood viscosity is determined by plasma viscosity, hematocrit, erythrocyte deformability and aggregation. Plasma viscosity and hematocrit are directly regulated by the organism. The molecular biology of the principal determinants of plasma viscosity, i.e., fibrinogen, immunoglobulins, albumin, and lipoproteins is outlined in this work. Hematocrit is regulated by erythropoietin, which is primarily induced by tissue hypoxia. Evidence begins to emerge that autoregulatory mechanisms may be involved in blood viscosity. Viscosity modulates gene transcription for albumin and apolipoproteins in cultured hepatocytes and the erythropoietin response to anemia in rats. Further investigations into these self‐regulatory mechanisms in biorheology are, however, needed for a better understanding of blood viscosity regulation in health and disease.
Keywords: Albumin, erythropoietin, fibrinogen, gammaglobulin, lipoprotein, molecular biology, viscosity
Journal: Biorheology, vol. 38, no. 2-3, pp. 203-212, 2001
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