APOL1 is the
newest addition to the list of CKD risk factors- possibly never before in the
history of nephrology has a gene associated with such a high odds ratio with
disease - above 7 for hypertensive CKD & >10 for FSGS. A gene that
confers heterozygous survival advantage when present as a single variant
allele, but two variants lead to high CKD risk - APOL1 on chromosome 22. A similar picture of the survival advantage
is seen with sickle cell disease. For more on the fascinating story of APOL1 itself, see this open access review,
NephMadness coverage
from 2015, and the NephJC coverage of a more
recent research.
A recent study
has shown increased risk of CKD and subsequent ESKD in a population of black kidney
donors with high risk APOL1 genotype.
High risk is defined as presence of two variants (G1 and G2 – so any
combination G1/G1, G1/G2 or G2/G2 is high risk) and was associated with faster
progression of renal dysfunction and lower pre- and post-donation eGFR (pre-eGFR
98 versus 108; p= 0.03 and post-eGFR 58 versus 68; p=0.01) over a median follow
up of 12 years. The second part of the study involved comparison between these
donors and non donors from the CARDIA cohort (Coronary
Artery Risk Development in Young Adults), based on APOL1 genotype status. After median 11 years, there was no
difference in eGFR decline between the two groups when segregated based on
genotype status, indicating that it was the genotype which influenced the eGFR
decline and not the donation. Other salient
features in the study were:
- 2 donors in the high risk group developed ESRD at 10 and 18 years of donation (11 %, but there were only 19 in this group).
- 78% of the donors were first degree relatives of the recipients. So the fact that a substantial percentage of donors were at risk of subsequent renal disease in this study does raises some valid concerns. Should all black donors be genotyped before transplantation?
An original article
published in the Annals of Surgery recently studied eligible kidney donors
(n=3438) from the CARDIA cohort of 1985-86 and deduced some risk scores based
on the clinical and genetic profile of this population. They projected the 25
year pre-donation risk of CKD (eGFR <60ml/min) or microalbuminuria
or macroalbuminuria in an 18 year old and a 30 year old potential donor. This
risk is for people with no clinical risk factors (family
history/pre-hypertension/diabetes). The risk increases significantly if any of
these risk factors are present. See the table for some examples (EA
– European American; AA – African American):
How about the risk to the recipients? Case
reports
have shown development of post transplant FSGS in siblings and monozygotic
twins, both in the donor and in the recipient. Data from
other studies
have shown increased risk of allograft failure in recipients if the donor has a
high risk genotype. All these data clearly point to the risk of CKD and
subsequent ESKD in AA individuals (both donors & recipients) following
transplantation. This brings us back to the most pertinent question, should
people of African ancestry be genotyped for APOL1
prior to transplantation? The present studies are not well equipped to answer
this question. Though it may seem that one obviously should screen (‘11% of
donors with high risk variants develop ESRD!’ ‘High risk variants increase graft
failure in recipients!’), lets pause and consider this. We know that live donor
transplantation is the modality that offers the best survival. We also know
that minorities, in US as well as in UK and elsewhere, have a lower rate of
live donor transplantation (see NephJC coverage of a recent JAMA
study and the ATTOM study, as well as the
NephMadness coverage from 2017 on disparities in transplantation). So, would genotyping worsen the disparity?
Is our fate inextricably written in
our genes? Enter APOLLO.
APOLLO,
APOL1 Long-Term Kidney Transplantation Outcomes
Network, is
a prospective study aimed at genotyping
donors and recipients in transplants involving recent African ancestry in
United States and monitoring long term follow up. This will shed more light on
this question and even might have a decisive influence on the present KDRI
(kidney risk donor index), replacing the race column with APOL1 genotype. We
await this important piece of work with interest.
Post by Sriram Sriperumbuduri
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