ASSOCIATION OF URINARY PROTEOMICS WITH THE KIDNEY ALLOGRAFT FAILURE RISK AND LEFT VENTRICULAR DYSFUNCTION AT 48 MONTHS AFTER TRANSPLANTATION

E-Poster

https://storage.unitedwebnetwork.com/files/1099/ae0c08896e9cc9ebf76b445044a5c0ee.pdf

Abstract Title

First Name *

Irena

Last Name *

Rambabova Bushljetikj

Co-author 1

Lada Trajceska lada.trajceska@gmail.com University Clinic for Nephrology Nephrology Skopje

Co-author 2

Oliver Bushljetikj oliverbuhljetik@yahoo.com University Clinic for Cardiology Cardiology Skopje

Co-author 3

Harald Mischak mischak@mosaiques.dn Mosaiques Diagnostics Mosaiques Diagnostic Hanover

Co-author 4

Goce Spasovski gspas@gmail.com University Clinic for Nephrology Nephrology Skopje

Co-author 5

Co-author 6

Co-author 7

Co-author 8

Co-author 9

Co-author 10

Co-author 11

Co-author 12

Co-author 13

Co-author 14

Co-author 15

Introduction

Kidney transplantation is best treatment option for end stage renal disease, but is still associated with a long term graft failure. To identify grafts with high failure risks before eGFR starts declining and irreversible graft changes occurs, as well as prevent cardiovascular morbidity is a challenge for transplant professionals.

Transplantation medicine is facing emerged need for identification of novel disease-specific biomarkers, with practical application in preventive screening, early diagnostic and improve prognostic and therapeutic possibilities

Methods

We evaluate 55 living donor kidney transplant patients (genetically and emotionally related). All patients underwent clinical examination and had a routine laboratory screening at the same time points (3,6,12,24,48 months), including determination of serum creatinine, blood urea nitrogen, blood glucose, blood cell counts, protein status, and 24/h proteinuria. Graft function was estimated by Nankivel equitation. Urine samples was collected according to the defined standard operation procedure (SOP) at 24 and 48 months for urinary proteomic classifier analysis of CKD273, HF1 and HF2. All patients underwent transthoracic echocardiography to evaluate left ventricular function.

Results

Our study showed a significant positive correlation between CKD 273 classifier and serum creatinine at 12, 24 and 48 months, urinary protein excretion at 48 months expressed as g/24h (r=0.34, p=0.04) and a negative correlation with GFR slope ml/min/year (r=--0,42, p<0,05) determined by Nankivell equation.

Patients with lower CKD score (<0,175) have better graft function, with lower serum creatinine in the follow up period from 12 to 48 months with higher eGFR at 24 and 48 months. Patients with proteinuria above 0,44 g/24 h at 48 months was associated with GFR decline of -7,82± 2,1 ml/min/year and -10,81±4,1 %/year. No any association between urinary proteomic classifiers with left ventricular changes (Diastolic dysfunction and subclinical systolic dysfunction) was found.

Conclusions

Urinary proteomics improve early diagnosis in progression of kidney disease and diagnosis of LV dysfunction in general population. We have found positive results of urinary proteomic classifier CKD 273 for early detection of kidney allograft dysfunction in kidney transplant recipients.. Further studies for urinary proteomic analysis in renal transplant recipients need to be done.

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