Plasma hepcidin levels are elevated but responsive to erythropoietin therapy in renal disease

Ashby, Damien; Gale, Daniel P.; Busbridge, Mark; Murphy, Kevin G.; Duncan, Neill; Cairns, Tom; Taube, David; Bloom, Stephen R.; Tam, Frederick W.K.; Chapman, Richard; Maxwell, Patrick H.; Choi, P.

doi:10.1038/ki.2009.21

Cited by 282 publications

(335 citation statements)

References 32 publications

(31 reference statements)

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“…As shown by Swinkels et al (11), there was almost 10-fold difference between lower limit of detection in SELDI (in study by Swinkels et al [11]) and immunodot (study by Nemeth et al [4]) in urinary hepcidin. The same difference was found between the assay by Ganz et al (12) and the assay by Ashby et al (13). In the studies by Ganz et al (12) and Zaritsky et al (14) reported in this issue of CJASN (using the same ELISA), the difference between detection limit was 10-fold, with 0.5 ng/ml in the study by Ashby et al (13) and 5 ng/ml in the assay developed by Ganz et al (12).…”

supporting

confidence: 59%

“…The same difference was found between the assay by Ganz et al (12) and the assay by Ashby et al (13). In the studies by Ganz et al (12) and Zaritsky et al (14) reported in this issue of CJASN (using the same ELISA), the difference between detection limit was 10-fold, with 0.5 ng/ml in the study by Ashby et al (13) and 5 ng/ml in the assay developed by Ganz et al (12). Values of hepcidin in both studies varied the normal range for healthy volunteers was 2 to 55 ng/ml (fifth through 95th percentiles) versus 29 to 254 ng/ml for male patients and 18 to 288 ng/ml for female patients.…”

supporting

confidence: 59%

“…Both assays are immunoassays. Ganz et al (12) performed the assay by using a functional biotinylated synthetic peptide (hepcidin analog) as a tracer (Intrinsic LifeSciences, La Jolla, CA) and another one for the construction of the standard curve (Bachem, King of Prussia, PA), whereas Ashby et al (13) used synthetic hepcidin-25 (Bachem, UK) conjugated to Keyhole limpet hemocyjanin. Binding was assessed by competition with I 125 -labeled hepcidin-25, separated by secondary antibody.…”

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Hepcidin Assays

Małyszko¹

2009

Clinical Journal of the American Society of Nephrology

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Iron is the fourth most common element in the earth's crust and the most abundant transition metal in the human body. It is an essential element required for growth and survival. Maintaining the correct iron balance is crucial for health. All living organisms evolved sophisticated mechanisms to maintain appropriate iron levels in their cells and within their body. It was shown recently that the kidney is also involved in iron metabolism. Our understanding of the molecular control of iron metabolism has increased dramatically in the past 5 yr as a result of the discovery of hepcidin. This is a circulating antimicrobial peptide that is synthesized mainly in the liver, which was recently proposed as a factor that regulates the uptake of dietary iron and its mobilization from macrophages and hepatic stores.The major circulating bioactive forms of hepcidin consist only of the carboxy-terminal portion (peptides of 25, 22, and 20 amino acids) (1). The exact location of the final prohormone processing is unknown. Propeptide convertases could be located in the blood or in the cell membrane of capillaries. Still no reliable information is available on normal serum levels of mature hepcidin (20, 22, and 25 amino acids); however, 60 -amino acid prohepcidin is easily detectable in serum. Hepcidin-25, the major form of mature hepcidin, is cleaved from prohepcidin by convertases. Hepcidin-20 and hepcidin-22 may be directly generated from prohepcidin by convertases or indirectly by degradation of hepcidin-25. Hepcidin-25 and hepcidin-20 are a major form of hepcidin in urine, whereas hepcidin-22 is a minor one (2). The same may be true for serum. The nuclear magnetic resonance structure studies indicated that hepcidin-20 exists as a monomer, whereas hepcidin-25 readily aggregates (1).Hepcidin-25 was initially identified in human blood using a mass spectrometric assay (3). Then Park et al. (2) isolated urinary hepcidin-25 and hepcidin-20 using cation exchange chromatography and reverse-phase HPLC. There is no consensus on the best assay method for hepcidin, and assays for hepcidin detection and quantification in serum or urine have not been generally available. The detection and quantification of hepcidin in plasma and serum have been hampered by technical difficulties (small size of hepcidin; limited availability of the antigen; isolation of hepcidin from urine involves complex, time-consuming procedures). Moreover, its conservation among animal species complicates the elicitation of an immune response in host species. Urinary hepcidin assays seem to be preferable for studies on iron metabolism because serum hepcidin levels are below the detection limit of the currently used methods. This might be due to a rapid clearance of free serum hepcidin by its binding to ferroportin and its subsequent cellular internalization (4); however, reliable information still is not available on normal serum levels of mature hepcidin (20, 22, and 25 amino acids). The urinary hepcidin excretion could be due either to physiologic incomplete reabsorp...

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confidence: 59%

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confidence: 59%

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confidence: 99%

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Hepcidin Assays

Małyszko¹

2009

Clinical Journal of the American Society of Nephrology

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“…Of note, the CHD population investigated in our last study [24] was enrolled in a center characterized by a clinical policy favoring relatively low iron supplementation to avoid iron toxicity. Indeed, the median ferritin level in this CHD population was " only " 265 μ g/L (interquartile range 155 -411 μ g/L), while, e.g., in the previous study by Ashby and colleagues [15] the mean ferritin level in 94 CHD patients was 550 μ g/L (95% CI 291 and 1014 μ g/L, respectively). Moreover, again in the effort to select the most appropriate controls, we included only control subjects with biochemically documented normal iron status.…”

Section: Hepcidin As a Player In The Anemia Of Chdmentioning

confidence: 99%

“…It has therefore been hypothesized that in CHD patients increased hepcidin could aggravate functional iron deficiency by decreasing macrophage iron release and intestinal iron absorption, paving the way to the possible utilization of anti-hepcidin drugs for optimizing the management of anemia [9,21]. In regards to this point, it is of interest to note that administration of erythropoiesis stimulating agents (ESAs), by itself, has been reported to reduce hepcidin in patients with chronic kidney disease [15,22]. This is likely due to hypoxia-inducible factor via Epo-induced erythropoiesis [23], and suggests that the beneficial effect of Epo in CHD may be partly mediated by normalization of iron delivery.…”

Section: Hepcidin As a Player In The Anemia Of Chdmentioning

confidence: 99%

Hepcidin levels in chronic hemodialysis patients: a critical evaluation

Valenti

Pelusi

Campostrini

et al. 2014

Clinical Chemistry and Laboratory Medicine

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Altered systemic iron metabolism is a key element of uremia, and functional iron deficiency mainly related to subclinical inflammation makes it difficult to maintain proper control of anemia in chronic hemodialysis patients (CHD). In the last decade, the hepatic hormone hepcidin has been progressively recognized as the master regulator of circulating iron levels through the modulation of cellular iron fluxes in response to iron stores, as well as to erythroid and inflammatory stimuli. Hepcidin is cleared by the kidney and progression of renal disease has been associated to increased serum hepcidin levels. This, in turn, reduces iron availability for erythropoiesis, suggesting anti-hepcidin strategies for improving anemia control. Moreover, hepcidin has been recently implicated in the pathogenesis of long-term complications of dialysis, like accelerated atherosclerosis. Initial studies almost invariably reported a sustained increase of serum hepcidin in chronic hemodialysis patients. Noteworthy, such studies included relatively few patients and controls that were poorly matched for major determinants of serum hepcidin at population level, i.e., age and gender. More recent data based on accurately matched larger series challenge the view that hepcidin is intrinsically increased in hemodialysis patients, showing a marked inter-and intra-individual variability of hormone levels. Here we take a critical look to the data published so far on hepcidin levels in CHD, analyze the reasons underlying the discrepancies in available studies and the hepcidin variability in CHD, and point out the need for further studies in large series of well-characterized CHD patients and controls.

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Optimal Oral Iron Therapy for Iron Deficiency Anemia Among US Veterans

Patel,

Silvey,

Arora

et al. 2024

JAMA Netw Open

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ImportanceOptimal oral iron supplementation strategy is unclear in patients with iron deficiency anemia (IDA) who have either normal kidney function (NKF) or chronic kidney disease (CKD).ObjectiveTo investigate the association of different oral iron supplementation strategies with the change in hemoglobin and iron indices among patients with IDA with either NKF or CKD.Design, Setting, and ParticipantsThis retrospective cohort study was conducted between 2009 and 2019 at nationwide Veterans Health Administration facilities. Eligible participants included veterans with IDA (defined as hemoglobin &lt;12 g/dL and either iron saturation &lt;20% or ferritin &lt;50 ng/mL) who received their first outpatient prescription of oral iron. Patients were further divided into those with NKF (estimated glomerular filtration rate &gt;60 mL/min/1.73 m2) and CKD (estimated glomerular filtration rate ≥15 mL/min/1.73 m2 and &lt;60 mL/min/1.73 m2). Data analysis was conducted from February to October 2023.ExposuresPatients were classified into 3 groups based on their oral iron dosing schedule: daily (once a day), multiple doses per day (MDD; ≥2 times per day), or alternate-day dose (ADD).Main Outcomes and MeasuresThe primary outcomes were change of hemoglobin, ferritin, total iron binding capacity (TIBC), and iron saturation (ISAT), which were calculated with linear mixed-effects models.ResultsA total of 71 677 veterans with IDA (63 202 male [88.2%] and 8475 female [11.8%]; mean [SD] age, 68.47 [13.09] years), including 47 201 with NKF and 24 476 with CKD, were identifed. In patients with NKF in the daily group, hemoglobin increased from baseline (estimated per-30-day difference [SE], 0.27 [0.00] g/dL; P &lt; .001). In comparison with the daily group, hemoglobin increased more in the MDD group (estimated per-30-day difference [SE], 0.08 [0.03] g/dL; P &lt; .001), but no difference was noted in the ADD group (estimated per-30-day difference [SE], −0.01 [0.01] g/dL; P = .38). Ferritin, ISAT, and TIBC results were similar, except TIBC showed less change in the ADD group compared with the daily group. Patients with CKD showed similar trends but smaller magnitudes in changes. Among patients with NKF, the adjusted mean increase in hemoglobin was 1.03 g/dL (95% CI, 1.01-1.06 g/dL) for those in the daily group, 1.38 g/dL (95% CI, 1.36-1.40 g/dL) for those in the MDD group, and 0.93 g/dL (95% CI, 0.84-1.02 g/dL) for those in the ADD group at 90 days. Among patients with CKD, the adjusted mean increase in hemoglobin was 0.71 g/dL (95% CI, 0.68-0.73 g/dL) for those in the daily group, 0.99 g/dL (95% CI, 0.97-1.01 g/dL) for those in the MDD group, and 0.62 g/dL (95% CI, 0.52-0.73 g/dL) for those in the ADD group at 90 days.Conclusions and RelevanceIn this retrospective cohort study of veterans with IDA, there was no significant difference in the improvement of hemoglobin and iron indices between daily and ADD groups, but quickest improvement was observed in the MDD group. These findings suggest that the choice of oral iron therapy should depend on the rapidity of response desired and patient preference due to adverse effects.

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Plasma hepcidin levels are elevated but responsive to erythropoietin therapy in renal disease

Cited by 282 publications

References 32 publications

Hepcidin Assays

Hepcidin Assays

Hepcidin levels in chronic hemodialysis patients: a critical evaluation

Optimal Oral Iron Therapy for Iron Deficiency Anemia Among US Veterans

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