Perfluoroalkyl substances and kidney function in chronic kidney disease, anemia, and diabetes

BN Conway, AN Badders, T Costacou… - … syndrome and obesity …, 2018 - Taylor & Francis
BN Conway, AN Badders, T Costacou, JM Arthur, KE Innes
Diabetes, metabolic syndrome and obesity: targets and therapy, 2018Taylor & Francis
Background Anemia often complicates chronic kidney disease (CKD), leading to insufficient
tissue oxygenation and hypoxic injury, the factor thought to underlie progression from CKD
to renal failure. Perfluorocarbons are potent oxygen transporters used in organ preservation
and synthetic blood development. Data are scarce on their relationship with kidney function,
especially in diabetes where anemia and hypoxia are more prevalent. We investigated the
relationship of perfluoroalkyl acids (PFAS) with kidney function and variation by diabetes …
Background
Anemia often complicates chronic kidney disease (CKD), leading to insufficient tissue oxygenation and hypoxic injury, the factor thought to underlie progression from CKD to renal failure. Perfluorocarbons are potent oxygen transporters used in organ preservation and synthetic blood development. Data are scarce on their relationship with kidney function, especially in diabetes where anemia and hypoxia are more prevalent. We investigated the relationship of perfluoroalkyl acids (PFAS) with kidney function and variation by diabetes and anemia status.
Methods
Data on 53,650 adults (5,210 with diabetes) were obtained from the C8 Health Project. CKD was defined as an estimated glomerular filtration rate (eGFR) <60 mL/min/1.73 m2. Four PFAS were investigated: perfluorohexane sulfonate (PFHxS), perfluorooctanoic acid, perfluorooctane sulfonate, and perfluorononanoic acid.
Findings
Each PFAS was positively associated with eGFR among those with CKD or anemia; this was the strongest among those with both CKD and anemia, followed by those with CKD uncomplicated by anemia. These relationships were more pronounced among those with diabetes (all P<0.01). In the absence of both CKD and anemia, PFAS was inversely associated with eGFR. Among persons with both anemia and diabetes, when further stratified by CKD stage, compared to an eGFR <30, ORs (95% CI) for being in the eGFR ≥ 90, 60–89, 45–59, and 30–45 range, respectively, were 3.20 (2.00–5.13), 2.64 (1.83–3.80), 3.18 (2.17–4.67), and 1.99 (1.38–2.86) for each ng/dL increase in PFHxS. Results were similar for each PFAS.
Interpretation
PFAS are inversely associated with kidney function in CKD and diabetes, with a stronger relation observed when anemia is present.
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