Continuous, noninvasive, and localized microvascular tissue oximetry using visible light spectroscopy

被引:79
作者
Benaron, DA [1 ]
Parachikov, IH [1 ]
Friedland, S [1 ]
Soetikno, R [1 ]
Brock-Utne, J [1 ]
van der Starre, PJA [1 ]
Nezhat, C [1 ]
Terris, MK [1 ]
Maxim, PG [1 ]
Carson, JJL [1 ]
Razavi, MK [1 ]
Gladstone, HB [1 ]
Fincher, EF [1 ]
Hsu, CP [1 ]
Clark, FL [1 ]
Cheong, WF [1 ]
Duckworth, JL [1 ]
Stevenson, DK [1 ]
机构
[1] Stanford Univ, Sch Med, Dept Pediat, Div Neonatal & Dev Med, Palo Alto, CA 94304 USA
关键词
D O I
10.1097/00000542-200406000-00019
中图分类号
R614 [麻醉学];
学科分类号
100217 ;
摘要
Background The authors evaluated the ability of visible tight spectroscopy (VLS) oximetry to detect hypoxemia and ischemia in human and animal subjects. Unlike near-infrared spectroscopy or pulse oximetry (Spo(2)), VLS tissue oximetry uses shallow-penetrating visible light to measure microvascular hemoglobin oxygen saturation (Sto(2)) in small, thin tissue volumes. Methods: In pigs, Sto(2) was measured in muscle and enteric mucosa during normoxia, hypoxemia (Spo(2) = 40-96%), and ischemia (occlusion, arrest). In patients, Sto(2) was measured in skin, muscle, and oral/enteric mucosa during normoxia, hypoxemia (SPo2 = 60-99%), and ischemia (occlusion, compression, ventricular fibrillation). Results: In pigs, normoxic Sto(2) was 71 +/- 4% (mean +/- SD), without differences between sites, and decreased during hypoxemia (muscle, 11 +/- 6%; P < 0.001) and ischemia (colon, 31 +/- 11%; P < 0.001). In patients, mean normoxic Sto(2) ranged from 68 to 77% at different sites (733 measures, 111 subjects); for each noninvasive site except skin, variance between subjects was low (e.g., colon, 69% +/- 4%, 40 subjects; buccal, 77% +/- 3%, 21 subjects). During hypoxemia, Sto(2) correlated with Spo(2) (animals, r(2) = 0.98; humans, r(2) = 0.87). During ischemia, Sto(2) initially decreased at -1.3 +/- 0.2%/s and decreased to zero in 3-9 min (r(2) = 0.94). Ischemia was distinguished from normoxia and hypoxemia by a widened pulse/VLS saturation difference (Delta < 30% during normoxia or hypoxemia vs. Delta > 35% during ischemia). Conclusions: VLS oximetry provides a continuous, noninvasive, and localized measurement of the Sto(2), sensitive to hypoxemia, regional, and global ischemia. The reproducible and narrow Sto(2) normal range for oral/enteric mucosa supports use of this site as an accessible and reliable reference point for the VLS monitoring of systemic flow.
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页码:1469 / 1475
页数:7
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