Effects of losartan and allopurinol on cardiorespiratory regulation in obstructive sleep apnoea

Morgan, Barbara J.; Teodorescu, Mihaela; Pegelow, David F.; Jackson, Emily R.; Schneider, Devin L.; Plante, David T.; Gapinski, James P.; Hetzel, Scott; Dopp, John M.

doi:10.1113/ep087006

Cited by 13 publications

(15 citation statements)

References 75 publications

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“…The present analysis is based on data collected during a previously reported randomized clinical trial (NCT01637623) of the effects of allopurinol, losartan and placebo on chemoreflex sensitivity in hypertensive patients with OSA (Morgan et al . 2018). The majority of data reported herein were obtained at the initial (pre‐randomization, prior to drug treatment) visit to the laboratory.…”

Section: Methodsmentioning

confidence: 99%

“…Assessment of carotid chemoreflex sensitivity has received recent attention in clinical conditions such as hypertension (Tafil-Klawe et al 1985), heart failure (Schultz et al 2007) and obstructive sleep apnoea (OSA) (Narkiewicz et al 1999a), and also in the context of acclimatization to high altitude hypoxia (Dempsey et al 2014). A variety of transient and steady-state stimulatory and inhibitory interventions (Narkiewicz et al 1999a;Leuenberger et al 2001;Steinback et al 2009;Sinski et al 2014;Morgan et al 2018;Phillips et al 2018;Keir et al 2019) have been employed to provoke measurable increases and decreases in ventilation and sympathetic outflow; however, limited information is available on whether ventilatory and neurocirculatory responses to carotid chemoreceptor stimulation and inhibition are associated in human subjects.…”

Section: Introductionmentioning

confidence: 99%

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The need for specificity in quantifying neurocirculatory vs. respiratory effects of eucapnic hypoxia and transient hyperoxia

Prasad

Morgan

Gupta

et al. 2020

The Journal of Physiology

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Key points The carotid chemoreceptor mediates the ventilatory and muscle sympathetic nerve activity (MSNA) responses to hypoxia and contributes to tonic sympathetic and respiratory drives. It is often presumed that both excitatory and inhibitory tests of chemoreflex function show congruence in the end‐organ responses. Ventilatory and neurocirculatory (MSNA, blood pressure and heart rate) responses to chemoreflex inhibition elicited by transient hyperoxia and to chemoreflex excitation produced by steady‐state eucapnic hypoxia were measured in a cohort of 82 middle‐aged individuals. Ventilatory and MSNA responsiveness to hyperoxia and hypoxia were not significantly correlated within individuals. It was concluded that ventilatory responses to hypoxia and hyperoxia do not predict MSNA responses and it is recommended that tests using the specific outcome of interest, i.e. MSNA or ventilation, are required. Transient hyperoxia is recommended as a sensitive and reliable means of quantifying tonic chemoreceptor‐driven levels of sympathetic nervous system activity and respiratory drive. Abstract Hypersensitivity of the carotid chemoreceptor leading to sympathetic nervous system activation and ventilatory instability has been implicated in the pathogenesis and consequences of several common clinical conditions. A variety of treatment approaches aimed at lessening chemoreceptor‐driven sympathetic overactivity are now under investigation; thus, the ability to quantify this outcome variable with specificity and precision is crucial. Accordingly, we measured ventilatory and neurocirculatory responses to chemoreflex inhibition elicited by transient hyperoxia and chemoreflex excitation produced by exposure to graded, steady‐state eucapnic hypoxia in middle‐aged men and women (n = 82) with continuous positive airway pressure‐treated obstructive sleep apnoea. Progressive, eucapnic hypoxia produced robust and highly variable increases in ventilation (+83 ± 59%) and muscle sympathetic nerve activity (MSNA) burst frequency (+55 ± 31%), whereas transient hyperoxia caused marked reductions in these variables (−35 ± 14% and −42 ± 16%, respectively). Coefficients of variation for ventilatory and MSNA burst frequency responses, indicating test–retest reproducibility, were respectively 9% and 24% for hyperoxia and 35% and 28% for hypoxia. Based on statistical measures of rank correlation or even comparisons across quartiles of corresponding ventilatory and MSNA responses, we found that the magnitudes of ventilatory inhibition with hyperoxia or excitation with eucapnic hypoxia were not correlated with corresponding MSNA responses within individuals. We conclude that, in conscious, behaving humans, ventilatory sensitivities to progressive, steady‐state, eucapnic hypoxia and transient hyperoxia do not predict MSNA responsiveness. Our findings also support the use of transient hyperoxia as a reliable, sensitive, measure of the carotid chemoreceptor contribution to tonic sympathetic nervous system activity and respiratory drive.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

The need for specificity in quantifying neurocirculatory vs. respiratory effects of eucapnic hypoxia and transient hyperoxia

Prasad

Morgan

Gupta

et al. 2020

The Journal of Physiology

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“…The exaggerated lumbar sympathetic and MAP responses to breath hold following chronic intermittent hypoxia were attenuated by losartan, an effect likely mediated by blunted upregulation of AT 1 R expression on the carotid body (Marcus et al, 2010). In contrast, losartan does not influence the ventilatory response to step changes in normocapnic hypoxia in patients with OSA (Morgan et al, 2018). In agreement with our findings, this indicates an alternative mechanism involved in chemoreceptor sensitization that is independent of the AT 1 R. For example, heart failure models suggest a reduction in carotid body blood flow is necessary to reduce neural nitric oxide synthase expression while elevating carotid body AT 1 R expression and ANG-II concentration (Li and Schultz, 2006).…”

Section: Influence Of At 1 R Blockade On the Hypercapnic And Voluntarmentioning

confidence: 86%

Angiotensin II-Type I Receptor Antagonism Does Not Influence the Chemoreceptor Reflex or Hypoxia-Induced Central Sleep Apnea in Men

et al. 2020

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Components of the renin-angiotensin system (RAS) situated within the carotid body or central nervous system may promote hypoxia-induced chemoreceptor reflex sensitization or central sleep apnea (CSA). We determined if losartan, an angiotensin-II type-I receptor (AT 1 R) antagonist, would attenuate chemoreceptor reflex sensitivity before or after 8 h of nocturnal hypoxia, and consequently CSA severity. In a doubleblind, randomized, placebo-controlled, crossover protocol, 14 men (age: 25 ± 2 years; BMI: 24.6 ± 1.1 kg/m 2 ; means ± SEM) ingested 3 doses of either losartan (50 mg) or placebo every 8 h. Chemoreceptor reflex sensitivity was assessed during hypoxic and hyperoxic hypercapnic ventilatory response (HCVR) tests and during six-20s hypoxic apneas before and after 8 h of sleep in normobaric hypoxia (F I O 2 = 0.135). Loop gain was assessed from a ventilatory control model fitted to the ventilatory pattern of CSA recorded during polysomnography. Prior to nocturnal hypoxia, losartan had no effect on either the hyperoxic (losartan: 3.6 ± 1.1, placebo: 4.0 ± 0.6 l/min/mmHg; P = 0.9) or hypoxic HCVR (losartan: 5.3 ± 1.4, placebo: 5.7 ± 0.68 l/min/mmHg; P = 1.0). Likewise, losartan did not influence either the hyperoxic (losartan: 4.2 ± 1.3, placebo: 3.8 ± 1.1 l/min/mmHg; P = 0.5) or hypoxic HCVR (losartan: 6.6 ± 1.8, placebo: 6.3 ± 1.5 l/min/mmHg; P = 0.9) after nocturnal hypoxia. Cardiorespiratory responses to apnea and participants' apnea hypopnea indexes during placebo and losartan were similar (73 ± 15 vs. 75 ± 14 events/h; P = 0.9). Loop gain, which correlated with CSA severity (r = 0.94, P < 0.001), was similar between treatments. In summary, in young healthy men, hypoxia-induced CSA severity is strongly associated with loop gain, but the AT 1 R does not modulate chemoreceptor reflex sensitivity before or after 8 h of nocturnal hypoxia.

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“…Translational findings in humans are currently limited. However, in a recent clinical trial, it was observed that losartan reduced systolic and diastolic blood pressure in OSA patients without modifying muscle-sympathetic outflow or ventilation during hypoxia [ 102 ]. OSA was fairly well established in these patients and as such, there may have been irreversible epigenetic remodeling of CB function [ 103 ], accounting for the apparent lack of impact of losartan on CB function.…”

Section: G αQ -Protein-coupled Receptor Signalimentioning

confidence: 99%

G-Protein-Coupled Receptor (GPCR) Signaling in the Carotid Body: Roles in Hypoxia and Cardiovascular and Respiratory Disease

Aldossary

Alzahrani

Nathanael

et al. 2020

IJMS

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The carotid body (CB) is an important organ located at the carotid bifurcation that constantly monitors the blood supplying the brain. During hypoxia, the CB immediately triggers an alarm in the form of nerve impulses sent to the brain. This activates protective reflexes including hyperventilation, tachycardia and vasoconstriction, to ensure blood and oxygen delivery to the brain and vital organs. However, in certain conditions, including obstructive sleep apnea, heart failure and essential/spontaneous hypertension, the CB becomes hyperactive, promoting neurogenic hypertension and arrhythmia. G-protein-coupled receptors (GPCRs) are very highly expressed in the CB and have key roles in mediating baseline CB activity and hypoxic sensitivity. Here, we provide a brief overview of the numerous GPCRs that are expressed in the CB, their mechanism of action and downstream effects. Furthermore, we will address how these GPCRs and signaling pathways may contribute to CB hyperactivity and cardiovascular and respiratory disease. GPCRs are a major target for drug discovery development. This information highlights specific GPCRs that could be targeted by novel or existing drugs to enable more personalized treatment of CB-mediated cardiovascular and respiratory disease.

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Effects of losartan and allopurinol on cardiorespiratory regulation in obstructive sleep apnoea

Cited by 13 publications

References 75 publications

The need for specificity in quantifying neurocirculatory vs. respiratory effects of eucapnic hypoxia and transient hyperoxia

The need for specificity in quantifying neurocirculatory vs. respiratory effects of eucapnic hypoxia and transient hyperoxia

Angiotensin II-Type I Receptor Antagonism Does Not Influence the Chemoreceptor Reflex or Hypoxia-Induced Central Sleep Apnea in Men

G-Protein-Coupled Receptor (GPCR) Signaling in the Carotid Body: Roles in Hypoxia and Cardiovascular and Respiratory Disease

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