Red Blood Cell Transfusion After Stage I Palliation Is Associated With Worse Clinical Outcomes

Felina K Mille; Aditya Badheka; Priscilla Yu; Xuemei Zhang; David F Friedman; John Kheir; Sarah van den Bosch; Antonio G Cabrera; Javier J Lasa; Hannah Katcoff; Paula Hu; Santiago Borasino; Krissie Hock; Jordan Huskey; Jamie Weller; Harsh Kothari; Joshua Blinder

doi:10.1161/JAHA.119.015304

Red Blood Cell Transfusion After Stage I Palliation Is Associated With Worse Clinical Outcomes

J Am Heart Assoc. 2020 May 18;9(10):e015304. doi: 10.1161/JAHA.119.015304. Epub 2020 May 11.

Authors

Felina K Mille¹, Aditya Badheka², Priscilla Yu³, Xuemei Zhang¹, David F Friedman¹, John Kheir⁴, Sarah van den Bosch⁴, Antonio G Cabrera⁵, Javier J Lasa⁵, Hannah Katcoff¹, Paula Hu¹, Santiago Borasino⁶, Krissie Hock⁶, Jordan Huskey⁶, Jamie Weller³, Harsh Kothari², Joshua Blinder¹

Affiliations

¹ The Children's Hospital of Philadelphia Philadelphia PA.
² University of Iowa Stead Family Children's Hospital Iowa City IA.
³ University of Texas Southwestern Medical Center Dallas TX.
⁴ Boston Children's Hospital Boston MA.
⁵ Texas Children's Hospital Houston TX.
⁶ University of Alabama at Birmingham AL.

Abstract

Background Packed red blood cell transfusion may improve oxygen content in single-ventricle neonates, but its effect on clinical outcomes after Stage 1 palliation is unknown. Methods and Results Retrospective multicenter analysis of packed red blood cell transfusion exposures in neonates after Stage 1 palliation, excluding those with intraoperative mortality or need for extracorporeal membrane oxygenation. Transfusion practice variability was assessed, and multivariable regression used to identify transfusion risk factors. After propensity score adjustment for severity of illness, clinical outcomes were compared between transfused and nontransfused subjects. Of 396 subjects, 323 (82%) received 930 postoperative red blood cell transfusions. Packed red blood cell volume (median 9-42 mL/kg [P<0.0001]), donor exposures (1-2 [P<0.0001]), transfusion number (1-3 [P<0.0001]), and pretransfusion hemoglobin (12.1-13 g/dL, P=0.0049) varied between sites. Cyanosis (P=0.02), chest tube output (P=0.0003), and delayed sternal closure (P=0.0033) increased transfusion risk. Transfusion was associated with prolonged mechanical ventilation (6 [interquartile range 4, 12] versus 3 [1, 5] days, P=0.02) and intensive care unit stay (19 [12, 33] versus 9 [6, 19] days, P=0.016). When stratified by number of transfusions (0, 1, or >1), duration of mechanical ventilation (3 [1, 5] versus 4 [3, 6] versus 9 [5, 16] days [P<0.0001]) and intensive care unit stay (9 [6, 19] versus 13 [8, 25] versus 21 [13, 38] days [P<0.0001]) increased for those transfused more than once. Most subjects who died were transfused, though the association with mortality was not significant. Conclusions Packed red blood cell transfusion after Stage 1 palliation is common, and transfusion practice is variable. Transfusion is a significant predictor of longer intensive care unit stay and mechanical ventilation. Further studies to define evidence-based transfusion thresholds are warranted.

Keywords: Norwood operation; congenital heart disease; neonates; red blood cell transfusion; single ventricle; stage I palliation.

Publication types

Multicenter Study
Research Support, Non-U.S. Gov't

MeSH terms

Blalock-Taussig Procedure / adverse effects*
Blalock-Taussig Procedure / mortality
Erythrocyte Transfusion / adverse effects*
Erythrocyte Transfusion / mortality
Hospital Mortality
Humans
Infant, Newborn
Intensive Care Units
Length of Stay
Norwood Procedures / adverse effects*
Norwood Procedures / mortality
Palliative Care*
Respiration, Artificial
Retrospective Studies
Risk Assessment
Risk Factors
Time Factors
Treatment Outcome
United States
Univentricular Heart / mortality
Univentricular Heart / physiopathology
Univentricular Heart / surgery*