Microvascular blood flow and oxygenation during hemorrhagic hypotension
Understanding microvascular oxygen transport requires the knowledge of microvessel topology and geometry, blood flow and oxygen levels. Microvascular hemodynamic responses to hemorrhagic hypotension (HH) such as size-dependent vasoconstriction and blood flow reduction could lead to increased longitu...
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Veröffentlicht in: | Microvascular research 2008-03, Vol.75 (2), p.217-226 |
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Sprache: | eng |
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Zusammenfassung: | Understanding microvascular oxygen transport requires the knowledge of microvessel topology and geometry, blood flow and oxygen levels. Microvascular hemodynamic responses to hemorrhagic hypotension (HH) such as size-dependent vasoconstriction and blood flow reduction could lead to increased longitudinal oxygen partial pressure (
PO
2) gradients. However, the mesenteric microvascular
PO
2 has never been evaluated during HH. Therefore, we studied hemodynamic variables and
PO
2 distribution in 165 mesenteric microvessels from 39 anesthetized rats to investigate whether HH-induced vasoconstriction and blood flow reduction were associated with changes in longitudinal
PO
2 gradients. Vessels were analyzed according to their position in the network, as well as a few interstitial
PO
2 areas. We found that during baseline a small
PO
2 gradient exists, but HH is accompanied by more pronounced microvascular longitudinal
PO
2 gradients. Decreased blood flow did not seem to completely explain these findings, since blood flow was uniformly diminished in arterioles and venules, independent of diameter and position in the network. During HH, some microvessels presented higher
PO
2 than during baseline despite blood flow reduction, possibly due to a combination of systemic hyperoxia and low oxygen consumption of mesentery. The data suggest that blood flow measurements may be a poor indicator of the oxygenation status in some regions of the mesentery. The enhanced mesenteric longitudinal
PO
2 gradient may lead to regions with different levels of other physiologically active compounds. |
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ISSN: | 0026-2862 1095-9319 |
DOI: | 10.1016/j.mvr.2007.07.003 |