Perfluorocarbon-associated gas exchange in gastric aspiration

F. D. Nesti; B. P. Fuhrman; D. M. Steinhorn; M. C. Papo; L. J. Hernan; L. C. Duffy; J. E. Fisher; C. L. Leach; P. R. Paczan; B. A. Burak

doi:10.1097/00003246-199409000-00015

Perfluorocarbon-associated gas exchange in gastric aspiration

F. D. Nesti
, B. P. Fuhrman
, D. M. Steinhorn
, M. C. Papo
, L. J. Hernan
, L. C. Duffy
, J. E. Fisher
, C. L. Leach
, P. R. Paczan
, B. A. Burak

Pediatrics

University at Buffalo

SUNY Buffalo

Research output: Contribution to journal › Article › peer-review

118 Scopus citations

Abstract

Objectives: To test whether perfluorocarbon-associated gas exchange (gas ventilation of the perfluorocarbon-liquid filled lung) could support oxygenation better than conventional positive pressure breathing in a piglet model of gastric aspiration-induced adult respiratory distress syndrome (ARDS). Design: Prospective, randomized, blinded, controlled study. Setting: A critical care research laboratory in a university medical school. Subjects: Fourteen healthy piglets. Interventions: Under α-chloralose anesthesia and metocurine iodide neuromuscular blockade, 14 piglets underwent tracheostomy; central venous, systemic and pulmonary arterial catheterizations; and volume- regulated continuous positive-pressure breathing. Homogenized gastric aspirate (1 mL/kg) titrated to pH of 1.0 was instilled into the tracheostomy tube of each subject at 0 min to induce ARDS. Hemodynamics, lung mechanics, and gas exchange were evaluated every 30 mins for 6 hrs. Seven piglets were treated at 60 mins by tracheal instillation of perflubron, a volume selected to approximate normal functional residual capacity, and were supported by perfluorocarbon-associated gas exchange without modifying ventilatory settings. Perflubron was added to the trachea every hour to replace evaporative losses. Measurements and Main Results: There was a significant difference in oxygenation over time when tested by repeated-measures analysis of variance (F test = 8.78, p < .01). On further analysis, the differences were not significant from baseline to 2.5 hrs but became increasingly significant from 2.5 to 6 hrs after injury (p < .05) in the inflammatory phase of gastric aspiration-induced ARDS. Histologic evidence for ARDS in the treated group 6 hrs after injury was lacking. Conclusions: In the piglet model, perfluorocarbon-associated gas exchange with perflubron facilitates oxygenation in the acute phase of gastric aspiration-induced inflammatory ARDS when compared with conventional positive-pressure breathing. Histologic and physiologic data suggest that perfluorocarbon-associated gas exchange with perflubron might prevent ARDS if instituted after aspiration in the time window before the acute inflammatory process is manifest.

Original language	English
Pages (from-to)	1445-1452
Number of pages	8
Journal	Critical Care Medicine
Volume	22
Issue number	9
DOIs	https://doi.org/10.1097/00003246-199409000-00015
State	Published - 1994

Keywords

critical care
disease models, animal
lung
oxygen
perfluorocarbons
pneumonia, aspiration
positive-pressure ventilation
pulmonary emergencies
respiratory distress syndrome, adult
respiratory mechanics
ventilation

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10.1097/00003246-199409000-00015

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@article{88b2934b9d6e411d891f0acba3e51f9f,

title = "Perfluorocarbon-associated gas exchange in gastric aspiration",

abstract = "Objectives: To test whether perfluorocarbon-associated gas exchange (gas ventilation of the perfluorocarbon-liquid filled lung) could support oxygenation better than conventional positive pressure breathing in a piglet model of gastric aspiration-induced adult respiratory distress syndrome (ARDS). Design: Prospective, randomized, blinded, controlled study. Setting: A critical care research laboratory in a university medical school. Subjects: Fourteen healthy piglets. Interventions: Under α-chloralose anesthesia and metocurine iodide neuromuscular blockade, 14 piglets underwent tracheostomy; central venous, systemic and pulmonary arterial catheterizations; and volume- regulated continuous positive-pressure breathing. Homogenized gastric aspirate (1 mL/kg) titrated to pH of 1.0 was instilled into the tracheostomy tube of each subject at 0 min to induce ARDS. Hemodynamics, lung mechanics, and gas exchange were evaluated every 30 mins for 6 hrs. Seven piglets were treated at 60 mins by tracheal instillation of perflubron, a volume selected to approximate normal functional residual capacity, and were supported by perfluorocarbon-associated gas exchange without modifying ventilatory settings. Perflubron was added to the trachea every hour to replace evaporative losses. Measurements and Main Results: There was a significant difference in oxygenation over time when tested by repeated-measures analysis of variance (F test = 8.78, p < .01). On further analysis, the differences were not significant from baseline to 2.5 hrs but became increasingly significant from 2.5 to 6 hrs after injury (p < .05) in the inflammatory phase of gastric aspiration-induced ARDS. Histologic evidence for ARDS in the treated group 6 hrs after injury was lacking. Conclusions: In the piglet model, perfluorocarbon-associated gas exchange with perflubron facilitates oxygenation in the acute phase of gastric aspiration-induced inflammatory ARDS when compared with conventional positive-pressure breathing. Histologic and physiologic data suggest that perfluorocarbon-associated gas exchange with perflubron might prevent ARDS if instituted after aspiration in the time window before the acute inflammatory process is manifest.",

keywords = "critical care, disease models, animal, lung, oxygen, perfluorocarbons, pneumonia, aspiration, positive-pressure ventilation, pulmonary emergencies, respiratory distress syndrome, adult, respiratory mechanics, ventilation",

author = "Nesti, \{F. D.\} and Fuhrman, \{B. P.\} and Steinhorn, \{D. M.\} and Papo, \{M. C.\} and Hernan, \{L. J.\} and Duffy, \{L. C.\} and Fisher, \{J. E.\} and Leach, \{C. L.\} and Paczan, \{P. R.\} and Burak, \{B. A.\}",

year = "1994",

doi = "10.1097/00003246-199409000-00015",

language = "English",

volume = "22",

pages = "1445--1452",

journal = "Critical Care Medicine",

issn = "0090-3493",

publisher = "Lippincott Williams and Wilkins",

number = "9",

}

TY - JOUR

T1 - Perfluorocarbon-associated gas exchange in gastric aspiration

AU - Nesti, F. D.

AU - Fuhrman, B. P.

AU - Steinhorn, D. M.

AU - Papo, M. C.

AU - Hernan, L. J.

AU - Duffy, L. C.

AU - Fisher, J. E.

AU - Leach, C. L.

AU - Paczan, P. R.

AU - Burak, B. A.

PY - 1994

Y1 - 1994

N2 - Objectives: To test whether perfluorocarbon-associated gas exchange (gas ventilation of the perfluorocarbon-liquid filled lung) could support oxygenation better than conventional positive pressure breathing in a piglet model of gastric aspiration-induced adult respiratory distress syndrome (ARDS). Design: Prospective, randomized, blinded, controlled study. Setting: A critical care research laboratory in a university medical school. Subjects: Fourteen healthy piglets. Interventions: Under α-chloralose anesthesia and metocurine iodide neuromuscular blockade, 14 piglets underwent tracheostomy; central venous, systemic and pulmonary arterial catheterizations; and volume- regulated continuous positive-pressure breathing. Homogenized gastric aspirate (1 mL/kg) titrated to pH of 1.0 was instilled into the tracheostomy tube of each subject at 0 min to induce ARDS. Hemodynamics, lung mechanics, and gas exchange were evaluated every 30 mins for 6 hrs. Seven piglets were treated at 60 mins by tracheal instillation of perflubron, a volume selected to approximate normal functional residual capacity, and were supported by perfluorocarbon-associated gas exchange without modifying ventilatory settings. Perflubron was added to the trachea every hour to replace evaporative losses. Measurements and Main Results: There was a significant difference in oxygenation over time when tested by repeated-measures analysis of variance (F test = 8.78, p < .01). On further analysis, the differences were not significant from baseline to 2.5 hrs but became increasingly significant from 2.5 to 6 hrs after injury (p < .05) in the inflammatory phase of gastric aspiration-induced ARDS. Histologic evidence for ARDS in the treated group 6 hrs after injury was lacking. Conclusions: In the piglet model, perfluorocarbon-associated gas exchange with perflubron facilitates oxygenation in the acute phase of gastric aspiration-induced inflammatory ARDS when compared with conventional positive-pressure breathing. Histologic and physiologic data suggest that perfluorocarbon-associated gas exchange with perflubron might prevent ARDS if instituted after aspiration in the time window before the acute inflammatory process is manifest.

AB - Objectives: To test whether perfluorocarbon-associated gas exchange (gas ventilation of the perfluorocarbon-liquid filled lung) could support oxygenation better than conventional positive pressure breathing in a piglet model of gastric aspiration-induced adult respiratory distress syndrome (ARDS). Design: Prospective, randomized, blinded, controlled study. Setting: A critical care research laboratory in a university medical school. Subjects: Fourteen healthy piglets. Interventions: Under α-chloralose anesthesia and metocurine iodide neuromuscular blockade, 14 piglets underwent tracheostomy; central venous, systemic and pulmonary arterial catheterizations; and volume- regulated continuous positive-pressure breathing. Homogenized gastric aspirate (1 mL/kg) titrated to pH of 1.0 was instilled into the tracheostomy tube of each subject at 0 min to induce ARDS. Hemodynamics, lung mechanics, and gas exchange were evaluated every 30 mins for 6 hrs. Seven piglets were treated at 60 mins by tracheal instillation of perflubron, a volume selected to approximate normal functional residual capacity, and were supported by perfluorocarbon-associated gas exchange without modifying ventilatory settings. Perflubron was added to the trachea every hour to replace evaporative losses. Measurements and Main Results: There was a significant difference in oxygenation over time when tested by repeated-measures analysis of variance (F test = 8.78, p < .01). On further analysis, the differences were not significant from baseline to 2.5 hrs but became increasingly significant from 2.5 to 6 hrs after injury (p < .05) in the inflammatory phase of gastric aspiration-induced ARDS. Histologic evidence for ARDS in the treated group 6 hrs after injury was lacking. Conclusions: In the piglet model, perfluorocarbon-associated gas exchange with perflubron facilitates oxygenation in the acute phase of gastric aspiration-induced inflammatory ARDS when compared with conventional positive-pressure breathing. Histologic and physiologic data suggest that perfluorocarbon-associated gas exchange with perflubron might prevent ARDS if instituted after aspiration in the time window before the acute inflammatory process is manifest.

KW - critical care

KW - disease models, animal

KW - lung

KW - oxygen

KW - perfluorocarbons

KW - pneumonia, aspiration

KW - positive-pressure ventilation

KW - pulmonary emergencies

KW - respiratory distress syndrome, adult

KW - respiratory mechanics

KW - ventilation

UR - https://www.scopus.com/pages/publications/0027981269

U2 - 10.1097/00003246-199409000-00015

DO - 10.1097/00003246-199409000-00015

M3 - Article

C2 - 8062568

SN - 0090-3493

VL - 22

SP - 1445

EP - 1452

JO - Critical Care Medicine

JF - Critical Care Medicine

IS - 9

ER -

Perfluorocarbon-associated gas exchange in gastric aspiration

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Keywords

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