RESISTANCE TO BLOOD-FLOW IN MICROVESSELS IN-VIVO

Resistance to blood flow through peripheral vascular beds strongly influences cardiovascular function and transport to tissue. For a given Vascular architecture, flow resistance is determined by the rheological behavior of blood flowing through microvessels. A new approach for calculating the contribution of blood theology to microvascular flow resistance is presented. Morphology (diameter and length), flow velocity, hematocrit, and topological position were determined for all vessel segments (up to 913) of terminal microcirculatory networks in the rat mesentery by intravital microscopy. Flow velocity and hematocrit were also predicted from mathematical dow simulations, in which the assumed dependence of how resistance on diameter, hematocrit, and shear rate was optimized to minimize the deviation between measured and predicted values. For microvessels with diameters below approximate to 40 mu m, the resulting flow resistances are markedly higher and show a stronger dependence on hematocrit than previously estimated from measurements of blood flow in narrow glass tubes. For example, flow resistance in 10-mu m microvessels at normal hematocrit is found to exceed that of a corresponding glass tube by a factor of approximate to 4. In separate experiments, flow resistance of microvascular networks was estimated from direct measurements of total pressure drop and volume flow, at systemic hematocrits intentionally Varied from 0.08 to 0.68. The results agree closely with predictions based on the above-optimized resistance but not with predictions based on grass-tube data. The unexpectedly high flow resistance in small microvessels may be related to interactions between blood components and the inner vessel surface that do not occur in smooth-walled tubes.