Abstract

In striated muscle, the number of capillaries containing moving red blood cells increases with increasing metabolic demand. This phenomenon, termed capillary recruitment, has long been recognized, but its mechanism has been unclear. Here, a theoretical model for metabolic blood flow regulation in a heterogeneous network is used to test the hypothesis that capillary recruitment occurs as a result of active control of arteriolar diameters, combined with unequal partition of hematocrit at diverging microvascular bifurcations. The network structure is derived from published observations of hamster cremaster muscle in control and dilated states. The model for modulation of arteriolar diameters includes length-tension characteristics of vascular smooth muscle and responses of smooth muscle tone to myogenic, shear-dependent, and metabolic stimuli. Blood flow is simulated including nonuniform hematocrit distribution. Convective and diffusive oxygen transport in the network is simulated. Oxygen-dependent metabolic signals are assumed to be conducted upstream from distal vessels to arterioles. With increasing oxygen demand, arterioles dilate, blood flow increases, and the numbers of flowing arterioles and capillaries, as defined by red blood cell flux above a small threshold value, increase. Unequal hematocrit partition at diverging bifurcations contributes to recruitment and enhances tissue oxygenation. The results imply that capillary recruitment, as observed in the hamster cremaster preparations, can occur as a consequence of local control of arteriolar tone and the resulting nonuniform changes in red blood cell fluxes, and provide an explanation for observations of sequential recruitment of individual capillaries in response to modulation of terminal arteriolar diameter.

Highlights

  • Proper distribution of blood flow within organs is essential for the matching of oxygen and nutrient supply to tissue demand

  • The objective of this study is to test the hypothesis that capillary recruitment occurs in heterogeneous microvascular networks as a consequence of local blood flow regulation by changes in arteriolar vascular smooth muscle (VSM) tone, in combination with unequal hematocrit partition at diverging microvessel bifurcations

  • The network structure is derived from observations of the hamster cremaster muscle (Berg 1995; Berg et al 1997), in which the microvasculature was imaged and mapped in a control state and in a pharmacologically induced maximally dilated state, and red blood cells (RBCs) fluxes were measured in the arterioles and capillaries

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Summary

Introduction

Proper distribution of blood flow within organs is essential for the matching of oxygen and nutrient supply to tissue demand. Changes in VSM tone are elicited in response to changes in several factors, including levels of oxygen and other metabolites, intraluminal pressure, and luminal wall shear stress (Duling et al 1987). These vasoactive stimuli act locally and induce responses that are propagated upstream, causing vessels feeding the site of the stimulus to constrict or dilate. The resulting coordinated control of VSM tone in vessels proximal to the affected site contributes to blood flow regulation in response to changes in the metabolic demand of the tissue (Segal et al 1989; Berg et al 1997; Cohen et al 2000). Starting with the work of Krogh (1919a,b), it has been proposed that one of the contributing mechanisms is capillary recruitment,

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