A test of the interaction between central and peripheral respiratory chemoreflexes in humans.

The Journal of physiology(2023)

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摘要
How central and peripheral chemoreceptor drives to breathe interact in humans remains contentious. We measured the peripheral chemoreflex sensitivity to hypoxia (PChS) at various isocapnic CO tensions ( ) to determine the form of the relationship between PChS and central . Twenty participants (10F) completed three repetitions of modified rebreathing tests with end-tidal ( ) clamped at 150, 70, 60 and 45 mmHg. End-tidal ( ), , ventilation ( ) and calculated oxygen saturation (S O ) were measured breath-by-breath by gas-analyser and pneumotach. The - relationship of repeat-trials were linear-interpolated, combined, averaged into 1 mmHg bins, and fitted with a double-linear function ( S, L min mmHg ). PChS was computed at intervals of 1 mmHg of as follows: the difference in between the three hypoxic profiles and the hyperoxic profile (∆ ) was calculated; three ∆ values were plotted against corresponding S O ; and linear regression determined PChS (Lmin mmHg %S O ). These processing steps were repeated at each to produce the PChS vs. isocapnic relationship. These were fitted with linear and polynomial functions, and Akaike information criterion identified the best-fit model. One-way repeated measures analysis of variance assessed between-condition differences. S increased (P < 0.0001) with isoxic from 3.7 ± 1.5 L min mmHg at 150 mmHg to 4.4 ± 1.8, 5.0 ± 1.6 and 6.0 ± 2.2 Lmin mmHg at 70, 60 and 45 mmHg, respectively. Mean S O fell progressively (99.3 ± 0%, 93.7 ± 0.1%, 90.4 ± 0.1% and 80.5 ± 0.1%; P < 0.0001). In all individuals, PChS increased with , and this relationship was best described by a linear model in 75%. Despite increasing central chemoreflex activation, PChS increased linearly with indicative of an additive central-peripheral chemoreflex response. KEY POINTS: How central and peripheral chemoreceptor drives to breathe interact in humans remains contentious. We measured peripheral chemoreflex sensitivity to hypoxia (PChS) at various isocapnic carbon dioxide tensions ( ) to determine the form of the relationship between PChS and central . Participants performed three repetitions of modified rebreathing with end-tidal fixed at 150, 70, 60 and 45 mmHg. PChS was computed at intervals of 1 mmHg of end-tidal ( ) as follows: the difference in between the three hypoxic profiles and the hyperoxic profile (∆ ) was calculated; three ∆ values were plotted against corresponding calculated oxygen saturation (S O ); and linear regression determined PChS (Lmin mmHg %S O ). In all individuals, PChS increased with , and this relationship was best described by a linear (rather than polynomial) model in 15 of 20. Most participants did not exhibit a hypo- or hyper-additive effect of central chemoreceptors on the peripheral chemoreflex indicating that the interaction was additive.
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关键词
carbon dioxide, control of breathing, hypercapnia, hyperoxia, hypoxic ventilatory response, rebreathing
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