In vitro validation and characterization of pulsed inhaled nitric oxide administration during early inspiration

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In vitro validation and characterization of pulsed inhaled nitric oxide administration during early inspiration

Metadaten

dc.​contributor.​author
Pickerodt, Philipp A.
dc.​contributor.​author
Hofferberth, Moritz B. T.
dc.​contributor.​author
Busch, Thilo
dc.​contributor.​author
Russ, Martin
dc.​contributor.​author
Taher, Mahdi
dc.​contributor.​author
Boemke, Willehad
dc.​contributor.​author
Weber-Carstens, Steffen
dc.​contributor.​author
Köbrich, Rainer
dc.​contributor.​author
Swenson, Erik
dc.​contributor.​author
Deja, Maria
dc.​contributor.​author
Francis, Roland C. E.
dc.​date.​accessioned
2023-07-24T12:49:34Z
dc.​date.​available
2023-07-24T12:49:34Z
dc.​date.​issued
2021
dc.​identifier.​uri
https://refubium.fu-berlin.de/handle/fub188/40219
dc.​identifier.​uri
http://dx.doi.org/10.17169/refubium-39939
dc.​description.​abstract
Purpose: Admixture of nitric oxide (NO) to the gas inspired with mechanical ventilation can be achieved through continuous, timed, or pulsed injection of NO into the inspiratory limb. The dose and timing of NO injection govern the inspired and intrapulmonary effect site concentrations achieved with different administration modes. Here we test the effectiveness and target reliability of a new mode injecting pulsed NO boluses exclusively during early inspiration. Methods: An in vitro lung model was operated under various ventilator settings. Admixture of NO through injection into the inspiratory limb was timed either (i) selectively during early inspiration ("pulsed delivery"), or as customary, (ii) during inspiratory time or (iii) the entire respiratory cycle. Set NO target concentrations of 5-40 parts per million (ppm) were tested for agreement with the yield NO concentrations measured at various sites in the inspiratory limb, to assess the effectiveness of these NO administration modes. Results: Pulsed delivery produced inspiratory NO concentrations comparable with those of customary modes of NO administration. At low (450 ml) and ultra-low (230 ml) tidal volumes, pulsed delivery yielded better agreement of the set target (up to 40 ppm) and inspiratory NO concentrations as compared to customary modes. Pulsed delivery with NO injection close to the artificial lung yielded higher intrapulmonary NO concentrations than with NO injection close to the ventilator. The maximum inspiratory NO concentration observed in the trachea (68 +/- 30 ppm) occurred with pulsed delivery at a set target of 40 ppm. Conclusion: Pulsed early inspiratory phase NO injection is as effective as continuous or non-selective admixture of NO to inspired gas and may confer improved target reliability, especially at low, lung protective tidal volumes.
en
dc.​language
eng
dc.​rights.​uri
https://creativecommons.org/licenses/by/4.0/
dc.​subject
Nitric oxide
en
dc.​subject
Inhalation
en
dc.​subject
PiNO
en
dc.​subject
Mechanical ventilation
en
dc.​subject
Artificial lung
en
dc.​subject
ARDS
en
dc.​subject.​ddc
600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::610 Medizin und Gesundheit
dc.​title
In vitro validation and characterization of pulsed inhaled nitric oxide administration during early inspiration
dc.​type
Wissenschaftlicher Artikel
dcterms.​bibliographicCitation.​doi
10.1007/s10877-021-00689-x
dcterms.​bibliographicCitation.​journaltitle
Journal of Clinical Monitoring and Computing
dcterms.​bibliographicCitation.​number
3
dcterms.​bibliographicCitation.​originalpublishername
Springer Nature
dcterms.​bibliographicCitation.​pagestart
637
dcterms.​bibliographicCitation.​pageend
648
dcterms.​bibliographicCitation.​volume
36
refubium.​affiliation
Charité - Universitätsmedizin Berlin
refubium.​funding
Springer Nature DEAL
refubium.​resourceType.​isindependentpub
no
dcterms.​accessRights.​openaire
open access
dcterms.​bibliographicCitation.​pmid
33735405
dcterms.​isPartOf.​issn
1387-1307
dcterms.​isPartOf.​eissn
1573-2614
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