Effects of Vitamin D Replacement on Hormones Regulating Iron Metabolism in Individuals With Chronic Kidney Disease
NCT ID: NCT01988116
Last Updated: 2015-08-24
Study Results
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Basic Information
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COMPLETED
EARLY_PHASE1
40 participants
INTERVENTIONAL
2013-10-31
2015-06-30
Brief Summary
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Iron is an essential mineral which is a major component of proteins that carry oxygen in the blood. Problems with iron metabolism can lead to low blood levels (anemia), which can commonly happen in people with CKD.
New research over the last decade has uncovered a new hormone called 'hepcidin', which is made in the liver and released into the blood. Hepcidin controls how much iron is in the blood by preventing the absorption of iron from food. Blood levels of hepcidin C are found to be high in people with CKD, and a recent small study in people with normal kidney function showed that treatment with vitamin D decreased hepcidin levels.
Another protein, known as 'hemojuvelin', has been recently discovered and is also thought to control the amount of iron in the blood. The relationship between vitamin D and hemojuvelin has never been studied before.
In this study, investigators would like to examine the effects of vitamin D on iron metabolism and blood levels of hepcidin C and hemojuvelin in individuals with CKD.
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Detailed Description
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Vitamin D is hypothesized to exert a significant and independent effect on the iron metabolism. In the CKD population, low vitamin-D levels independently correlate with the severity of anemia. Hepcidin C levels are found to be elevated in the CKD population. Mechanisms underlying the effect of vitamin D on iron homeostasis potentially include vitamin D induced expression of erythropoietin receptors, increased proliferation of erythroid precursors, and reduction in hepcidin C levels due to reduction in IL-6 from the anti-inflammatory effects of vitamin D. More recently, a study revealed direct relationship between vitamin D replacement and a sustained fall in hepcidin C levels. The same group of researchers found the above relationship to be due to a direct effect of vitamin D on hepcidin expression.
Hemojuvelin (HJV) is a protein encoded by the HFE2 gene and is found in the membrane bound and the soluble form (sHJV) in the humans. Mutations in the HJV gene are responsible for Juvenile Hemochromatosis. It is an upstream regulator of hepcidin transcription and appears to be essential for hepcidin expression in the hepatocytes and has important role to play in iron homeostasis. Recently, an assay has become available to measure the sHJV levels in the serum.
Although, we know that hepcidin plays a central role in iron homeostasis and recent studies have given us insight into the role hemojuvelin and vitamin D play in iron metabolism, to date, no studies have examined the effect on vitamin D replacement on hepcidin, hemojuvelin levels and iron metabolism in individuals with CKD.
Hypothesis 1: Treatment with an activated vitamin D analog in the individuals with CKD results in a statistically significant fall in hepcidin C levels as compared to individuals provided with placebo.
Hypothesis 2: Treatment with an activated vitamin D analog results in decreased levels of soluble hemojuvelin in individuals with chronic kidney disease.
Hypothesis 3: Vitamin D replacement in the individuals with CKD results in improved iron parameters as compared to the placebo.
Conditions
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Study Design
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RANDOMIZED
PARALLEL
QUADRUPLE
Study Groups
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Oral Calcitriol
Oral Calcitriol 0.5 mcg once daily for 6 weeks
Oral Calcitriol 0.5 mcg once daily for 6 weeks
Placebo Arm
Placebo capsule 1 Capsule once daily for 6 weeks
Placebo
Interventions
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Oral Calcitriol 0.5 mcg once daily for 6 weeks
Placebo
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
Exclusion Criteria
* Subjects currently receiving nutritional vitamin D (cholecalciferol or ergocalciferol) in dosages greater than 2000 IU/day.
* Subjects receiving erythropoiesis stimulating agents.
* Subjects receiving intravenous iron therapy.
* Subjects receiving oral iron therapy started within 3 months prior to recruitment.
* Subjects with severe anemia defined as Hb \< 8.0 g/dL for males and Hb \<7.0 g/dL for females.
* Subjects with iron deficiency anemia defined as serum ferritin \<100ng/ml and Transferring Saturation \< 20%.
* Pregnancy and lactation.
* Subjects with hypercalcemia defined as serum calcium level of \> 10.0 mg/dL.
* Subjects with serum phosphorus concentration of \> 4.5 mg/dL.
* Subjects with acute kidney injury or rapidly declining GFR.
* Subjects receiving any form of renal replacement therapy including hemodialysis, peritoneal dialysis, and patients with renal transplant.
* Subjects with focus of active inflammation or infection determined clinically.
19 Years
ALL
No
Sponsors
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University of Alabama at Birmingham
OTHER
Responsible Party
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Principal Investigators
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Bhupesh Panwar, MD
Role: PRINCIPAL_INVESTIGATOR
University of Alabama, Nephrology Division
Orlando M Gutierrez, MD,MMSc
Role: STUDY_DIRECTOR
University of Alabama, Nephrology Division
Locations
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University of Alabama
Birmingham, Alabama, United States
Countries
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References
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Panwar B, McCann D, Olbina G, Westerman M, Gutierrez OM. Effect of calcitriol on serum hepcidin in individuals with chronic kidney disease: a randomized controlled trial. BMC Nephrol. 2018 Feb 9;19(1):35. doi: 10.1186/s12882-018-0823-7.
Other Identifiers
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F130725013
Identifier Type: -
Identifier Source: org_study_id
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