M. Erin Moir scite author profile

²

,

³

et al. 2018

Pulsatile blood flow is generally mediated by the compliance of blood vessels whereby they distend locally and momentarily to accommodate the passage of the pressure wave. This freedom of the blood vessels to exercise their compliance may be suppressed within the confines of the rigid skull. The effect of this on the mechanics of pulsatile blood flow within the cerebral circulation is not known, and the situation is compounded by experimental access difficulties. We present an approach which we have developed to overcome these difficulties in a study of the mechanics of pulsatile cerebral blood flow. The main finding is that while the innate compliance of cerebral vessels is indeed suppressed within the confines of the skull, this is compensated somewhat by compliance provided by other “extravascular” elements within the skull. The net result is what we have termed “intracranial compliance,” which we argue is more pertinent to the mechanics of pulsatile cerebral blood flow than is intracranial pressure.

Heterogeneous baroreflex control of sympathetic action potential subpopulations in humans

¹

,

The Journal of Physiology

²

,

Usselman

³

et al. 2020

Emission patterns in muscle sympathetic nerve activity stem from differently sized action potential (AP) subpopulations that express varying discharge probabilities. The mechanisms governing these firing behaviours are unclear. This study investigated the hypothesis that the arterial baroreflex exerts varying control over the different AP subpopulations. r During baseline, medium APs expressed the greatest baroreflex slopes, while small and large APs exhibited weaker slopes. On going from baseline to lower body negative pressure (LBNP; simulated orthostatic stress), baroreflex slopes for some clusters of medium APs expressed the greatest increase, while slopes for large APs also increased but to a lesser degree. A subpopulation of previously silent larger APs was recruited with LBNP but these APs expressed weak baroreflex slopes. r The arterial baroreflex heterogeneously regulates sympathetic AP subpopulations, exerting its strongest effect over medium APs. Weak baroreflex mechanisms govern the recruitment of latent larger AP subpopulations during orthostatic stress.

Rapid changes in vascular compliance contribute to cerebrovascular adjustments during transient reductions in blood pressure in young, healthy adults

¹

,

Journal of Applied Physiology

²

,

Zamir

³

et al. 2020

Historically, dynamic cerebral autoregulation has been characterized by adjustments in cerebrovascular resistance following systematic changes in blood pressure. However, with the use of Windkessel modeling approaches, this study revealed rapid and large increases in cerebrovascular compliance that preceded reductions in cerebrovascular resistance following standing-induced blood pressure reductions. Importantly, the rapid cerebrovascular compliance response contributed to preservation of systolic blood velocity during the transient hypotensive phase. These results broaden our understanding of dynamic cerebral autoregulation.

Asynchronous Action Potential Discharge in Human Muscle Sympathetic Nerve Activity

¹

,

²

,

Shoemaker

³

2019

Pulse‐rhythmic bursts formed by synchronous action potential (AP) discharge characterises the firing behaviour of muscle sympathetic nerve activity (MSNA). However, complex AP discharge patterns related to multiple sites of control warrant an investigation of synchronicity in the human sympathetic system. Therefore, this study quantified the synchronicity of muscle sympathetic AP discharge in eight healthy individuals (4 females, 23 – 31 years, 170 ± 7 cm, 69 ± 13 kg, 60 ± 7 bpm, 89 ± 6 mmHg). MSNA (microneurography) was measured during baseline (BSL), −10 mmHg lower body negative pressure (LBNP), −40 mmHg LBNP, and an end‐expiratory apnea (APN; 30 ± 7 s). MSNA APs were detected from the filtered raw signal using a wavelet deconstruction approach and binned in clusters based on peak‐to‐peak amplitude (normalized within‐participant). An AP was considered to fire synchronously: 1) if its occurrence corresponded with a burst in the integrated MSNA signal (i.e., within ± 0.4 s of the burst peak), or 2) if it was one of ≥ 2 visible APs in the filtered microneurographic signal firing within ± 0.4 s of an ECG R‐wave, after adjusting for the conduction delay. All other APs were considered to fire asynchronously. At BSL, 33 ± 12 % of total AP activity was asynchronous (99 ± 48 asynchronous APs/100beats) and a pattern emerged whereby the probability of asynchronous AP firing decreased logarithmically (R2 = 0.80, P < 0.01) as AP cluster size increased. Compared to BSL (20 ± 6 bursts/min, 42 ± 7 AU), MSNA burst frequency increased on going to −10 mmHg LBNP (24 ± 6 bursts/min), −40 mmHg LBNP (35 ± 8 bursts/min), and APN (35 ± 9 bursts/min), while burst amplitude increased only with −40 mmHg LBNP (57 ± 8 AU) and APN (64 ± 14 AU) (both repeated measures analysis of variance [RM ANOVA]: P < 0.05, all Ppost‐hoc < 0.05). Compared with BSL, within‐burst AP discharge increased across all conditions (BSL: 144 ± 69 AP/min, 7 ± 2 AP/burst; −10 mmHg LBNP: 211 ± 87 AP/min, 8 ± 3 AP/burst; −40 mmHg LBNP: 410 ± 207 AP/min, 11 ± 4 AP/burst; APN: 397 ± 160 AP/min, 11 ± 3 AP/burst) (both RM ANOVA: P < 0.05, all Ppost‐hoc < 0.05). Compared to BSL, increased burst amplitude with −40 mmHg LBNP and APN was attributed to an increase in the within‐burst firing of previously active APs (BSL: 4 ± 1 clusters/burst, −40 mmHg LBNP: 5 ± 2 clusters/burst, APN: 5 ± 1 clusters/burst; RM ANOVA: P < 0.05, both Ppost‐hoc < 0.05) more so than the recruitment of new AP clusters (BSL: 14 ± 4 total clusters; −40 mmHg LBNP: 18 ± 7 total clusters; APN: 16 ± 6 total clusters; RM ANOVA: P > 0.05). However, compared to BSL (33 ± 12 %), the probability of asynchronous AP firing was reduced with −10 mmHg LBNP (26 ± 10 %), −40 mmHg LBNP (16 ± 7 %), and APN (14 ± 7 %; RM ANOVA: P < 0.05, all Ppost‐hoc < 0.05). The probability of asynchronous AP discharge was inversely and linearly related to burst frequency (β = −0.98, r2 = 0.67) and amplitude (β = −0.41, r2 = 0.20; both P < 0.01). This study suggests that: 1) integrated bursts of MSNA formed by synchronous AP firing are not separated by ‘neural silence’ but rather, by asynchronous AP discharge, and 2) smaller sympathetic APs are more likely to exhibit asynchronous discharge.Support or Funding InformationThis work was funded by a Natural Sciences and Engineering Research Council of Canada Discovery Grant.This abstract is from the Experimental Biology 2019 Meeting. There is no full text article associated with this abstract published in The FASEB Journal.

Asynchronous action potential discharge in human muscle sympathetic nerve activity

¹

,

American Journal of Physiology-Heart and Circulatory Physiology

²

,

Limberg

³

et al. 2019

Pulse‐rhythmic bursts formed by synchronous action potential (AP) discharge characterises the firing behaviour of muscle sympathetic nerve activity (MSNA). However, complex AP discharge patterns related to multiple sites of control warrant an investigation of synchronicity in the human sympathetic system. Therefore, this study quantified the synchronicity of muscle sympathetic AP discharge in eight healthy individuals (4 females, 23 – 31 years, 170 ± 7 cm, 69 ± 13 kg, 60 ± 7 bpm, 89 ± 6 mmHg). MSNA (microneurography) was measured during baseline (BSL), −10 mmHg lower body negative pressure (LBNP), −40 mmHg LBNP, and an end‐expiratory apnea (APN; 30 ± 7 s). MSNA APs were detected from the filtered raw signal using a wavelet deconstruction approach and binned in clusters based on peak‐to‐peak amplitude (normalized within‐participant). An AP was considered to fire synchronously: 1) if its occurrence corresponded with a burst in the integrated MSNA signal (i.e., within ± 0.4 s of the burst peak), or 2) if it was one of ≥ 2 visible APs in the filtered microneurographic signal firing within ± 0.4 s of an ECG R‐wave, after adjusting for the conduction delay. All other APs were considered to fire asynchronously. At BSL, 33 ± 12 % of total AP activity was asynchronous (99 ± 48 asynchronous APs/100beats) and a pattern emerged whereby the probability of asynchronous AP firing decreased logarithmically (R2 = 0.80, P < 0.01) as AP cluster size increased. Compared to BSL (20 ± 6 bursts/min, 42 ± 7 AU), MSNA burst frequency increased on going to −10 mmHg LBNP (24 ± 6 bursts/min), −40 mmHg LBNP (35 ± 8 bursts/min), and APN (35 ± 9 bursts/min), while burst amplitude increased only with −40 mmHg LBNP (57 ± 8 AU) and APN (64 ± 14 AU) (both repeated measures analysis of variance [RM ANOVA]: P < 0.05, all Ppost‐hoc < 0.05). Compared with BSL, within‐burst AP discharge increased across all conditions (BSL: 144 ± 69 AP/min, 7 ± 2 AP/burst; −10 mmHg LBNP: 211 ± 87 AP/min, 8 ± 3 AP/burst; −40 mmHg LBNP: 410 ± 207 AP/min, 11 ± 4 AP/burst; APN: 397 ± 160 AP/min, 11 ± 3 AP/burst) (both RM ANOVA: P < 0.05, all Ppost‐hoc < 0.05). Compared to BSL, increased burst amplitude with −40 mmHg LBNP and APN was attributed to an increase in the within‐burst firing of previously active APs (BSL: 4 ± 1 clusters/burst, −40 mmHg LBNP: 5 ± 2 clusters/burst, APN: 5 ± 1 clusters/burst; RM ANOVA: P < 0.05, both Ppost‐hoc < 0.05) more so than the recruitment of new AP clusters (BSL: 14 ± 4 total clusters; −40 mmHg LBNP: 18 ± 7 total clusters; APN: 16 ± 6 total clusters; RM ANOVA: P > 0.05). However, compared to BSL (33 ± 12 %), the probability of asynchronous AP firing was reduced with −10 mmHg LBNP (26 ± 10 %), −40 mmHg LBNP (16 ± 7 %), and APN (14 ± 7 %; RM ANOVA: P < 0.05, all Ppost‐hoc < 0.05). The probability of asynchronous AP discharge was inversely and linearly related to burst frequency (β = −0.98, r2 = 0.67) and amplitude (β = −0.41, r2 = 0.20; both P < 0.01). This study suggests that: 1) integrated bursts of MSNA formed by synchronous AP firing are n...