Publication:
Living related kidney donation for alternative complement pathway diseases: long-term outcomes

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Caliskan, Y.
Safak, S.
Dirim, A. B.
Velioglu, A.
Oto, O. A.
Yildiz, A.
Garayeva, N.
Yazici, H.
Ersoy, A.
Lentine, K. L.

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Publication Date

2022

Language

English

Type

Meeting Abstract

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Abstract

Purpose: Atypical hemolytic-uremic syndrome (aHUS) and C3 glomerulopathy (C3G) are rare conditions that cause severe kidney disease. Data to guide the evaluation of living related donor (LRD) candidates for aHUS and C3G are very limited. We examined the clinical course of LRDs to recipients with aHUS and C3G to understand the challenges and outcomes after donation. Methods: The cohort of recipients and their living donors (LD) was retrospectively identified from data at 5 transplant centers (1987-2021). LD were followed for postdonation kidney function measured by eGFR, proteinuria, cardiac events and death. Recipient graft outcomes were also examined. Results: The cohort comprised 24 LD to recipients with aHUS (46%) and C3G (54%) including 18 LRD, where relationship to recipient included father (7, 29%), mother (5, 21%), sibling (3, 12.5%), son (1, 4%), aunt (1, 4%) and unrelated (6, 25%). Outcomes were evaluated in 22 LRD over 5 years (IQR, 2.5-11) follow-up. None of the donors developed kidney failure (eGFR<15 ml/min/1.73m2 or dialysis). Last follow up serum mean (SD) creatinine, eGFR and proteinuria levels were 1.05 (0.16) mg/dL, 78.4 (15.7) ml/min/1.73m2, and 0.13 (0.22) g/g, respectively (Table 1). During follow up, 5 (23%) donors developed hypertension, but none developed cardiac events. One donor developed gastric cancer and another donor developed a brain tumor and died at 4th year after donation. Regarding recipients, 2 (18.2%) of aHUS and 8 (61.5%) of C3G recipients lost allografts at a median 11 (IQR 6-14.5) years after transplant (p=0.03).

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Source:

American Journal of Transplantation

Publisher:

Wiley

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Subject

Surgery, Kidneys, Transplantation

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