Issue |
J Extra Corpor Technol
Volume 46, Number 3, September 2014
|
|
---|---|---|
Page(s) | 217 - 223 | |
DOI | https://doi.org/10.1051/ject/201446217 | |
Published online | 15 September 2014 |
Original Articles
Hemolysis-Associated Nitric Oxide Dysregulation during Extracorporeal Membrane Oxygenation
* Center for Surgical Outcomes Research, The Research Institute at Nationwide Children’s Hospital, Columbus, Ohio
† Department of Neonatology, Children’s Hospital of Philadelphia, Philadelphia, Pennsylvania
‡ Department of Critical Care Medicine, Children’s Hospital of Philadelphia, Philadelphia, Pennsylvania
Address correspondence to: Peter C. Minneci, MD, MHSc, Co-Director, Center for Surgical Outcomes Research, Assistant Professor, Department of Surgery, Center for Innovation in Pediatric Practice, The Research Institute at Nationwide Children’s Hospital, 700 Children’s Drive, JW4914, Columbus, OH 43205. E-mail: peter.minneci@nationwidechildrens.org
Received:
9
June
2014
Accepted:
13
August
2014
Acute intravascular hemolysis during extracorporeal membrane oxygenation (ECMO) leads to increased levels of cell-free hemoglobin (FHb). Our aim was to investigate whether FHb levels are associated with nitric oxide (NO) consumption and clinical outcomes. A prospective observational study was performed involving pediatric patients on ECMO. Blood samples were collected before, during, and after the ECMO run, and plasma was evaluated for FHb, oxyhemoglobin, and NO consumption. Clinical data were collected including baseline patient characteristics, indications for ECMO, circuit changes, and mortality. Correlations between laboratory measures and associations between laboratory measures and clinical observations were evaluated. Twenty-three patients (11 male, 17 neonates) were enrolled with a median weight of 3.1 kg (interquartile range, 2.8–14.0 kg) and median ECMO run of 12 days (interquartile range, 5–19 day). There was a significant increase in FHb over time on ECMO (p = .007), and significant correlations were present between NO consumption and both FHb (r = .41, p = .01) and oxyhemoglobin levels (r = .98, p < .0001). Patients on ECMO for sepsis (n = 6) had lower average levels of oxyhemoglobin (mean [standard deviation {SD}] 14.5 [4.4] versus 19.0 [5.0] μM, p = .07) and NO consumption (mean [SD] 15.8 [4.1] versus 19.8 [3.7] μM, p = .04) during ECMO than patients with other indications. In the 3 days leading up to a circuit change, there were increases in mean total cell-free hemoglobin levels (24%/day, p = .08), oxyhemoglobin (37%/day, p = .005), and NO consumption (40%/day, p = .006) (n = 5). There were no significant associations identified between peak or average plasma measures of hemolysis and type of ECMO (venovenous versus venoarterial) or mortality. For children on ECMO, we observed a strong correlation between increased levels of plasma FHb and elevations in oxyhemoglobin and NO consumption; however, these changes were not associated with increased mortality. Increased hemolysis before circuit changes may be both a marker and a contributor to circuit failure.
Key words: extracorporeal membrane oxygenation / ECMO / nitric oxide / consumption / hemolysis
Results from this manuscript were presented separately at the 2013 and 2014 Children’s National Medical Center Symposium on ECMO and Advanced Therapies for Respiratory Failure, Keystone, Colorado.
This project is supported by the University of Pennsylvania/Children’s Hospital of Philadelphia Clinical and Translational Science Award UL1 RR024134 (Dr. Minneci), National Institutes of Health 5T32HL098039-03 (Dr. Sulkowski), and intramural funding from the Research Institute at Nationwide Children’s Hospital.
© 2014 AMSECT
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