Dead space ventilation promotes alveolar hypocapnia reducing surfactant secretion by altering mitochondrial function

Martina Kiefmann; Sascha Tank; Marc-Oliver Tritt; Paula Keller; Kai Heckel; Leonie Schulte-Uentrop; Cynthia Olotu; Sonja Schrepfer; Alwin E Goetz; Rainer Kiefmann

doi:10.1136/thoraxjnl-2018-211864

Dead space ventilation promotes alveolar hypocapnia reducing surfactant secretion by altering mitochondrial function

Standard

Dead space ventilation promotes alveolar hypocapnia reducing surfactant secretion by altering mitochondrial function. / Kiefmann, Martina; Tank, Sascha; Tritt, Marc-Oliver; Keller, Paula; Heckel, Kai; Schulte-Uentrop, Leonie ; Olotu, Cynthia; Schrepfer, Sonja; Goetz, Alwin E; Kiefmann, Rainer.

In: THORAX, Vol. 74, No. 3, 03.2019, p. 219-228.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Kiefmann, M, Tank, S, Tritt, M-O, Keller, P, Heckel, K, Schulte-Uentrop, L , Olotu, C, Schrepfer, S, Goetz, AE & Kiefmann, R 2019, 'Dead space ventilation promotes alveolar hypocapnia reducing surfactant secretion by altering mitochondrial function', THORAX, vol. 74, no. 3, pp. 219-228. https://doi.org/10.1136/thoraxjnl-2018-211864

APA

Kiefmann, M., Tank, S., Tritt, M-O., Keller, P., Heckel, K., Schulte-Uentrop, L., Olotu, C., Schrepfer, S., Goetz, A. E., & Kiefmann, R. (2019). Dead space ventilation promotes alveolar hypocapnia reducing surfactant secretion by altering mitochondrial function. THORAX, 74(3), 219-228. https://doi.org/10.1136/thoraxjnl-2018-211864

Vancouver

Kiefmann M, Tank S, Tritt M-O, Keller P, Heckel K, Schulte-Uentrop L et al. Dead space ventilation promotes alveolar hypocapnia reducing surfactant secretion by altering mitochondrial function. THORAX. 2019 Mar;74(3):219-228. https://doi.org/10.1136/thoraxjnl-2018-211864

Bibtex

@article{bbdce040dc8d4855a636afd791d6715f,

title = "Dead space ventilation promotes alveolar hypocapnia reducing surfactant secretion by altering mitochondrial function",

abstract = "BACKGROUND: In acute respiratory distress syndrome (ARDS), pulmonary perfusion failure increases physiologic dead space ventilation (VD/VT), leading to a decline of the alveolar CO2 concentration [CO2]iA. Although it has been shown that alveolar hypocapnia contributes to formation of atelectasis and surfactant depletion, a typical complication in ARDS, the underlying mechanism has not been elucidated so far.METHODS: In isolated perfused rat lungs, cytosolic or mitochondrial Ca2+ concentrations ([Ca2+]cyt or [Ca2+]mito, respectively) of alveolar epithelial cells (AECs), surfactant secretion and the projected area of alveoli were quantified by real-time fluorescence or bright-field imaging (n=3-7 per group). In ventilated White New Zealand rabbits, the left pulmonary artery was ligated and the size of subpleural alveoli was measured by intravital microscopy (n=4 per group). Surfactant secretion was determined in the bronchoalveolar lavage (BAL) by western blot.RESULTS: Low [CO2]iA decreased [Ca2+]cyt and increased [Ca2+]mito in AECs, leading to reduction of Ca2+-dependent surfactant secretion, and alveolar ventilation in situ. Mitochondrial inhibition by ruthenium red or rotenone blocked these responses indicating that mitochondria are key players in CO2 sensing. Furthermore, ligature of the pulmonary artery of rabbits decreased alveolar ventilation, surfactant secretion and lung compliance in vivo. Addition of 5% CO2 to the inspiratory gas inhibited these responses.CONCLUSIONS: Accordingly, we provide evidence that alveolar hypocapnia leads to a Ca2+ shift from the cytosol into mitochondria. The subsequent decline of [Ca2+]cyt reduces surfactant secretion and thus regional ventilation in lung regions with high VD/VT. Additionally, the regional hypoventilation provoked by perfusion failure can be inhibited by inspiratory CO2 application.",

keywords = "Journal Article",

author = "Martina Kiefmann and Sascha Tank and Marc-Oliver Tritt and Paula Keller and Kai Heckel and Leonie Schulte-Uentrop and Cynthia Olotu and Sonja Schrepfer and Goetz, {Alwin E} and Rainer Kiefmann",

note = "{\textcopyright} Author(s) (or their employer(s)) 2019. No commercial re-use. See rights and permissions. Published by BMJ.",

year = "2019",

month = mar,

doi = "10.1136/thoraxjnl-2018-211864",

language = "English",

volume = "74",

pages = "219--228",

journal = "THORAX",

issn = "0040-6376",

publisher = "BMJ PUBLISHING GROUP",

number = "3",

}

RIS

TY - JOUR

T1 - Dead space ventilation promotes alveolar hypocapnia reducing surfactant secretion by altering mitochondrial function

AU - Kiefmann, Martina

AU - Tank, Sascha

AU - Tritt, Marc-Oliver

AU - Keller, Paula

AU - Heckel, Kai

AU - Schulte-Uentrop, Leonie

AU - Olotu, Cynthia

AU - Schrepfer, Sonja

AU - Goetz, Alwin E

AU - Kiefmann, Rainer

PY - 2019/3

Y1 - 2019/3

N2 - BACKGROUND: In acute respiratory distress syndrome (ARDS), pulmonary perfusion failure increases physiologic dead space ventilation (VD/VT), leading to a decline of the alveolar CO2 concentration [CO2]iA. Although it has been shown that alveolar hypocapnia contributes to formation of atelectasis and surfactant depletion, a typical complication in ARDS, the underlying mechanism has not been elucidated so far.METHODS: In isolated perfused rat lungs, cytosolic or mitochondrial Ca2+ concentrations ([Ca2+]cyt or [Ca2+]mito, respectively) of alveolar epithelial cells (AECs), surfactant secretion and the projected area of alveoli were quantified by real-time fluorescence or bright-field imaging (n=3-7 per group). In ventilated White New Zealand rabbits, the left pulmonary artery was ligated and the size of subpleural alveoli was measured by intravital microscopy (n=4 per group). Surfactant secretion was determined in the bronchoalveolar lavage (BAL) by western blot.RESULTS: Low [CO2]iA decreased [Ca2+]cyt and increased [Ca2+]mito in AECs, leading to reduction of Ca2+-dependent surfactant secretion, and alveolar ventilation in situ. Mitochondrial inhibition by ruthenium red or rotenone blocked these responses indicating that mitochondria are key players in CO2 sensing. Furthermore, ligature of the pulmonary artery of rabbits decreased alveolar ventilation, surfactant secretion and lung compliance in vivo. Addition of 5% CO2 to the inspiratory gas inhibited these responses.CONCLUSIONS: Accordingly, we provide evidence that alveolar hypocapnia leads to a Ca2+ shift from the cytosol into mitochondria. The subsequent decline of [Ca2+]cyt reduces surfactant secretion and thus regional ventilation in lung regions with high VD/VT. Additionally, the regional hypoventilation provoked by perfusion failure can be inhibited by inspiratory CO2 application.

AB - BACKGROUND: In acute respiratory distress syndrome (ARDS), pulmonary perfusion failure increases physiologic dead space ventilation (VD/VT), leading to a decline of the alveolar CO2 concentration [CO2]iA. Although it has been shown that alveolar hypocapnia contributes to formation of atelectasis and surfactant depletion, a typical complication in ARDS, the underlying mechanism has not been elucidated so far.METHODS: In isolated perfused rat lungs, cytosolic or mitochondrial Ca2+ concentrations ([Ca2+]cyt or [Ca2+]mito, respectively) of alveolar epithelial cells (AECs), surfactant secretion and the projected area of alveoli were quantified by real-time fluorescence or bright-field imaging (n=3-7 per group). In ventilated White New Zealand rabbits, the left pulmonary artery was ligated and the size of subpleural alveoli was measured by intravital microscopy (n=4 per group). Surfactant secretion was determined in the bronchoalveolar lavage (BAL) by western blot.RESULTS: Low [CO2]iA decreased [Ca2+]cyt and increased [Ca2+]mito in AECs, leading to reduction of Ca2+-dependent surfactant secretion, and alveolar ventilation in situ. Mitochondrial inhibition by ruthenium red or rotenone blocked these responses indicating that mitochondria are key players in CO2 sensing. Furthermore, ligature of the pulmonary artery of rabbits decreased alveolar ventilation, surfactant secretion and lung compliance in vivo. Addition of 5% CO2 to the inspiratory gas inhibited these responses.CONCLUSIONS: Accordingly, we provide evidence that alveolar hypocapnia leads to a Ca2+ shift from the cytosol into mitochondria. The subsequent decline of [Ca2+]cyt reduces surfactant secretion and thus regional ventilation in lung regions with high VD/VT. Additionally, the regional hypoventilation provoked by perfusion failure can be inhibited by inspiratory CO2 application.

KW - Journal Article

U2 - 10.1136/thoraxjnl-2018-211864

DO - 10.1136/thoraxjnl-2018-211864

M3 - SCORING: Journal article

C2 - 30636196

VL - 74

SP - 219

EP - 228

JO - THORAX

JF - THORAX

SN - 0040-6376

IS - 3

ER -