Vasopressor selection during critical care management of brain dead organ donors and the effects on kidney graft function
EA Swanson, MS Patel, T Groat… - Journal of Trauma …, 2020 - journals.lww.com
EA Swanson, MS Patel, T Groat, NE Jameson, MKM Ellis, MP Hutchens, CU Niemann…
Journal of Trauma and Acute Care Surgery, 2020•journals.lww.comBACKGROUND Delayed graft function (DGF), the need for dialysis in the first week following
kidney transplant, affects approximately one quarter of deceased-donor kidney transplant
recipients. Donor demographics, donor serum creatinine, and graft cold ischemia time are
associated with DGF. However, there is no consensus on the optimal management of
hemodynamic instability in organ donors after brain death (DBDs). Our objective was to
determine the relationship between vasopressor selection during donor management and …
kidney transplant, affects approximately one quarter of deceased-donor kidney transplant
recipients. Donor demographics, donor serum creatinine, and graft cold ischemia time are
associated with DGF. However, there is no consensus on the optimal management of
hemodynamic instability in organ donors after brain death (DBDs). Our objective was to
determine the relationship between vasopressor selection during donor management and …
Abstract
BACKGROUND
Delayed graft function (DGF), the need for dialysis in the first week following kidney transplant, affects approximately one quarter of deceased-donor kidney transplant recipients. Donor demographics, donor serum creatinine, and graft cold ischemia time are associated with DGF. However, there is no consensus on the optimal management of hemodynamic instability in organ donors after brain death (DBDs). Our objective was to determine the relationship between vasopressor selection during donor management and the development of DGF.
METHODS
Prospective observational data, including demographic and critical care parameters, were collected for all DBDs managed by 17 organ procurement organizations from nine Organ Procurement and Transplantation Network Regions between 2012 and 2018. Recipient outcome data were linked with donor data through donor identification numbers. Donor critical care parameters, including type of vasopressor and doses, were recorded at three standardized time points during donor management. The analysis included only donors who received at least one vasopressor at all three time points. Vasopressor doses were converted to norepinephrine equivalent doses and analyzed as continuous variables. Univariate analyses were conducted to determine the association between donor variables and DGF. Results were adjusted for known predictors of DGF using binary logistic regression.
RESULTS
Complete data were available for 5,554 kidney transplant recipients and 2,985 DBDs. On univariate analysis, donor serum creatinine, donor age, donor subtype, kidney donor profile index, graft cold ischemia time, phenylephrine dose, and dopamine dose were associated with DGF. After multivariable analysis, increased donor serum creatinine, donor age, kidney donor profile index, graft cold ischemia time, and phenylephrine dose remained independent predictors of DGF.
CONCLUSION
Higher doses of phenylephrine were an independent predictor of DGF. With the exception of phenylephrine, the selection and dose of vasopressor during donor management did not predict the development of DGF.
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