TY - JOUR
T1 - Safety, hemodynamic effects and detection of acute xenon inhalation
T2 - Rationale for banning xenon from sport
AU - Lawley, Justin Stevan
AU - Gatterer, Hannes
AU - Dias, Katrin A
AU - Howden, Erin J
AU - Sarma, Satyam
AU - Cornwell, William K
AU - Hearon, Christopher M
AU - Samels, Mitchel
AU - Everding, Braden
AU - Hendrix, Max
AU - Piper, Thomas
AU - Thevis, Mario
AU - Levine, Benjamin D
N1 - Online: 15.08.2019
PY - 2019/12/1
Y1 - 2019/12/1
N2 - This study aimed to quantify the sedative effects, detection rates, and cardiovascular responses to xenon. On 3 occasions, participants breathed xenon (FiXe 30% for 20 min; FiXe 50% for 5 min; FiXe 70% for 2 min) in a nonblinded design. Sedation was monitored by a board-certified anesthesiologist. During 70% xenon, participants were also verbally instructed to operate a manual value with time-to-task failure being recorded. Beat-by-beat hemodynamics were measured continuously by ECG, photoplethysmography, and transcranial Doppler. Over 48 h postadministration, xenon was measured in blood and urine by gas chromatography-mass spectrometry. Xenon caused variable levels of sedation and restlessness. Task failure of the selfoperating value occurred at 60-90 s in most individuals. Over the first minute, 50% and 70% xenon caused a substantial reduction in total peripheral resistance (P <0.05). All dosages caused an increase in cardiac output (P <0.05). By the end of xenon inhalation, slight hypertension was observed after all three doses (P <0.05), with an increase in middle cerebral artery velocity (P <0.05). Xenon was consistently detected, albeit in trace amounts, up to 3 h after all three doses of xenon inhalation in blood and urine with variable results thereafter. Xenon inhalation caused sedation incompatible with selfoperation of a breathing apparatus, thus causing a potential lifethreatening condition in the absence of an anesthesiologist. Yet, xenon can only be reliably detected in blood and urine up to 3 h postacute dosing. NEW & NOTEWORTHY Breathing xenon in dosages conceivable for doping purposes (FiXe 30% for 20 min; FiXe 50% for 5 min; FiXe 70% for 2 min) causes an initial rapid fall in total peripheral resistance with tachycardia and thereafter a mild hypertension with elevated middle cerebral artery velocity. These dose duration intervals cause sedation that is incompatible with operating a breathing apparatus and can only be detected in blood and urine samples with a high probability for up to ~3 h.
AB - This study aimed to quantify the sedative effects, detection rates, and cardiovascular responses to xenon. On 3 occasions, participants breathed xenon (FiXe 30% for 20 min; FiXe 50% for 5 min; FiXe 70% for 2 min) in a nonblinded design. Sedation was monitored by a board-certified anesthesiologist. During 70% xenon, participants were also verbally instructed to operate a manual value with time-to-task failure being recorded. Beat-by-beat hemodynamics were measured continuously by ECG, photoplethysmography, and transcranial Doppler. Over 48 h postadministration, xenon was measured in blood and urine by gas chromatography-mass spectrometry. Xenon caused variable levels of sedation and restlessness. Task failure of the selfoperating value occurred at 60-90 s in most individuals. Over the first minute, 50% and 70% xenon caused a substantial reduction in total peripheral resistance (P <0.05). All dosages caused an increase in cardiac output (P <0.05). By the end of xenon inhalation, slight hypertension was observed after all three doses (P <0.05), with an increase in middle cerebral artery velocity (P <0.05). Xenon was consistently detected, albeit in trace amounts, up to 3 h after all three doses of xenon inhalation in blood and urine with variable results thereafter. Xenon inhalation caused sedation incompatible with selfoperation of a breathing apparatus, thus causing a potential lifethreatening condition in the absence of an anesthesiologist. Yet, xenon can only be reliably detected in blood and urine up to 3 h postacute dosing. NEW & NOTEWORTHY Breathing xenon in dosages conceivable for doping purposes (FiXe 30% for 20 min; FiXe 50% for 5 min; FiXe 70% for 2 min) causes an initial rapid fall in total peripheral resistance with tachycardia and thereafter a mild hypertension with elevated middle cerebral artery velocity. These dose duration intervals cause sedation that is incompatible with operating a breathing apparatus and can only be detected in blood and urine samples with a high probability for up to ~3 h.
KW - Anesthesia
KW - Blood pressure
KW - Brain blood flow
KW - Doping
UR - https://www.mendeley.com/catalogue/244b9617-af9c-3807-9843-cf887e608c51/
U2 - 10.1152/japplphysiol.00290.2019
DO - 10.1152/japplphysiol.00290.2019
M3 - Journal articles
C2 - 31414955
SN - 8750-7587
VL - 127
SP - 1511
EP - 1518
JO - Journal of applied physiology (Bethesda, Md. : 1985)
JF - Journal of applied physiology (Bethesda, Md. : 1985)
IS - 6
ER -