Abstract
Background: No reliable biomarker exists to predict responsiveness to intravenous (IV) iron (Fe) in iron deficient patients with chronic kidney disease (CKD). Our aim was to investigate if Hepcidin-25 (Hepc25) and soluble Transferrin Receptor (sTfR) and their Ratio sTfR/Hepc25 ratio prior to treatment can make a distinction between those predialysis patients with and those without adequate erythropoiesis after administration of IV ferric carboxymaltose (FCM).
Patients and methods: In this prospective study we enrolled 78 stable stage III-IV CKD patients with iron deficiency (serum ferritin levels lower than 100µg/L) treated with IV FCM 1000mg/100ml NaCl-0.9% and infused over a period of 20min. Patients were divided in two groups according to hemoglobin (Hb) increase within a month after treatment. The responders (Group R, n=40), showed above 1g/dL increase in Hb concentration. The non-responders (Group NR, n=38) had no such a favorable reaction. Patient data, clinical information and blood samples were collected prior to IV iron administration. Hematologic analysis was performed using a hematogy analyzer. Blood chemistry, including measurements of renal, nutrition and inflammation markers along with measurements of Hepc25, IL-6 and sTfR were performed using appropriate techniques. Receiver Operating Curve (ROC) analysis was applied in order to evaluate the diagnostic potential of Hepc25 and sTfR/Hepc25 ratio and conclusions about the specificity and sensitivity were drawn.
Results: As shown in Table 1, there were no significant differences at baseline between responders and non-responders in demographic and clinical parameters. No significant differences were revealed for serum creatinine, e-GFR, folic acid (FA), vitamin B12, hs-CRP and IL-6, with the notable exception of ferritin and Hepc25 levels that were lower and sTfR and sTfR/Hepc25 ratio that were higher in the responders as compared to non-responders (Table 1). Diagnostic efficacy was analyzed by ROC analysis. Cut off point of 1.49 for Hepc25 had sensitivity 84% and specificity 48%, and cut off point of 1.21 for sTfR/Hepc25 ratio had sensitivity 82% and specificity 52% to predict correctly response to Fe therapy (Table 2).
Conclusions: These results suggest that lower Hepc25 and ferritin levels, as well as higher sTfR and sTfR/Hepc25 ratio were significant predictors of favorable hemoglobin response within a month after IV administration of FCM in CKD patients. Further in vitro and in vivo experiments and clinical studies in a larger population of patients are needed to better elucidate the role of Hepc25 and sTfR/Hepc25 ratio in iron deficiency anemia in CKD.
Demographic, clinical and biochemical parameters in responders vs non-responders.
| . | Group R (n=40 . | Group NR (n=38) . | . | ||||||
|---|---|---|---|---|---|---|---|---|---|
| Age (years) | 72.7±11.2 | 74.5±10.3 | NS | ||||||
| Gender (M /F) | 27:13 | 25:13 | NS | ||||||
| Medications | |||||||||
| -RAS inhibitors | 21(27%) | 19(24%) | NS | ||||||
| rh EPO | 1(27%) | 20(26%) | NS | ||||||
| CCB | 10(13%) ) | 11(14% | NS | ||||||
| BMI (Κg/m2) | 25.5±3.3 | 25.1±3.4 | NS | ||||||
| Comorbidities | |||||||||
| -Cardiovascular Disease | 17(22%) | 15(19%) | NS | ||||||
| -Μechanical valve heart | 2(2%) | 2(2%) | NS | ||||||
| -Diabetes Mellitus | 20(26%) | 17(22%) | NS | ||||||
| -Polycystic Kidney Disease | 2(1%) | 1(1%) | NS | ||||||
| Hemoglobin (g/dL) | 10.9±1.6 | 11.1±1.3 | NS | ||||||
| Creatinine (mg/dL) | 2.4±1.1 | 2.5±1.1 | NS | ||||||
| eGFR(mL/min/1.73 m2) | 35.2±16.9 | 30.0±13.4 | NS | ||||||
| B12 (pg/mL) | 512.0±369.0 | 655.0±414.0 | NS | ||||||
| hs-CRP (mg/L) | 3.9±5.9 | 3.7± 4.9 | NS | ||||||
| IL-6 (pg/mL) | 6.2±5.3 | 5.78±4.5 | NS | ||||||
| sTfR (mg/L) | 2.27±0.99 | 1.76±0.76 | 0.014 | ||||||
| Log (1+Hepc25) | 0.552±0.343 | 0.728±0.348 | 0.027 | ||||||
| sTfR/Hepc25 | 1.91±1.53 | 0.80±0.72 | 0.002 | ||||||
| . | Group R (n=40 . | Group NR (n=38) . | . | ||||||
|---|---|---|---|---|---|---|---|---|---|
| Age (years) | 72.7±11.2 | 74.5±10.3 | NS | ||||||
| Gender (M /F) | 27:13 | 25:13 | NS | ||||||
| Medications | |||||||||
| -RAS inhibitors | 21(27%) | 19(24%) | NS | ||||||
| rh EPO | 1(27%) | 20(26%) | NS | ||||||
| CCB | 10(13%) ) | 11(14% | NS | ||||||
| BMI (Κg/m2) | 25.5±3.3 | 25.1±3.4 | NS | ||||||
| Comorbidities | |||||||||
| -Cardiovascular Disease | 17(22%) | 15(19%) | NS | ||||||
| -Μechanical valve heart | 2(2%) | 2(2%) | NS | ||||||
| -Diabetes Mellitus | 20(26%) | 17(22%) | NS | ||||||
| -Polycystic Kidney Disease | 2(1%) | 1(1%) | NS | ||||||
| Hemoglobin (g/dL) | 10.9±1.6 | 11.1±1.3 | NS | ||||||
| Creatinine (mg/dL) | 2.4±1.1 | 2.5±1.1 | NS | ||||||
| eGFR(mL/min/1.73 m2) | 35.2±16.9 | 30.0±13.4 | NS | ||||||
| B12 (pg/mL) | 512.0±369.0 | 655.0±414.0 | NS | ||||||
| hs-CRP (mg/L) | 3.9±5.9 | 3.7± 4.9 | NS | ||||||
| IL-6 (pg/mL) | 6.2±5.3 | 5.78±4.5 | NS | ||||||
| sTfR (mg/L) | 2.27±0.99 | 1.76±0.76 | 0.014 | ||||||
| Log (1+Hepc25) | 0.552±0.343 | 0.728±0.348 | 0.027 | ||||||
| sTfR/Hepc25 | 1.91±1.53 | 0.80±0.72 | 0.002 | ||||||
Sensitivity and specificity of Hepcidin and sTfR/H as predictors of responsiveness to IV FCM
| . | AUC . | 95%C.I. . | P-value . | Cut-off Point . | Sensitivity . | Specificity . | ||||
|---|---|---|---|---|---|---|---|---|---|---|
| Hepc25 | 0.648 | 0.52-0.77 | 0.025 | 1.49 | 84% | 48% | ||||
| sTfR/Hepc25 | 0.680 | 0.56-0.80 | 0.006 | 1.21 | 82% | 52% | ||||
| . | AUC . | 95%C.I. . | P-value . | Cut-off Point . | Sensitivity . | Specificity . | ||||
|---|---|---|---|---|---|---|---|---|---|---|
| Hepc25 | 0.648 | 0.52-0.77 | 0.025 | 1.49 | 84% | 48% | ||||
| sTfR/Hepc25 | 0.680 | 0.56-0.80 | 0.006 | 1.21 | 82% | 52% | ||||
No relevant conflicts of interest to declare.
Author notes
Asterisk with author names denotes non-ASH members.
This feature is available to Subscribers Only
Sign In or Create an Account Close Modal