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| Name | Class |
|---|---|
| University Hospital Frankfurt, Department of Anaesthesiology | UNKNOWN |
| IRON4U | UNKNOWN |
| University Hospital Frankfurt Institute for Biostatistics & Mathematical Modelling | UNKNOWN |
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Iron deficiency anaemia (IDA) in postoperative patients with confirmed preoperative iron deficiency (ID) in a population with planned major surgery who need fast replenishment of iron as judged by the treating physician will be treated with i.v. iron using Polyglucoferron, Ferric Carboxymaltose or oral iron
In this study, patients with confirmed and documented preoperative non-anaemic iron deficiency (diagnosis up to 28 days before surgery in routine pre-surgery monitoring) who develop anaemia within 12 to 72 hours after start of surgery (with additional confirmation at Baseline) and for whom fast replenishment of iron stores is necessary, will be included and substituted within 24h after Screening Visit/V1. Peri- or postoperative anaemia will be assessed as soon as possible but earliest 12 h after surgery. For short term safety analysis iron in urine will be measured in the first urine after the end of i.v. administration in the first 35 patients who are eligible for analysis in each i.v. treatment group. Only those patients are eligible for whom haematuria and/or proteinuria are excluded using dip stick test. The Ferric Carboxymaltose treatment arm will be closed if a sufficient number of patients is included for safety analysis.The study will then be continued for assessment of co-primary efficacy endpoint: The effectiveness of postoperative i.v. iron substitution with Polyglucoferron compared to conventional oral iron substitution with Ferrous sulfate (treatment 28 - 35 days) to normalize Hb-values or to increase Hb-values by at least 1.5 g/dl until visit 4 will be evaluated as well as patient related outcomes, such as the decreased need for allogenic blood transfusions. In addition, the well-being of the patient will be assumed to improve after treatment using the SF36 questionnaire.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Polyglucoferron | Experimental | once intravenously, dosing according to Hb-levels and body weight, 500 - 2000 mg |
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| Ferric Carboxymaltose | Active Comparator | Once intravenously (a second administration is allowed), dosing according to Hb-levels and body weight (500 - 2000 mg, max. single dose of 1000 mg) |
|
| Ferrous sulfate | Active Comparator | capsules, orally, dosing 50 mg - 200 mg (50 mg: 1 capsule in total, 200 mg: 4 capsules in total, taken as 2 capsules twice daily), duration of treatment 28 days |
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| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Polyglucoferron | Drug | intravenous administration |
|
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| Measure | Description | Time Frame |
|---|---|---|
| Proportion of patients who achieve normalized Hb-levels or increased Hb of at least 1.5 g/dl | Proportion of patients in the Polyglucoferron i.v. arm compared to oral iron substitution with Ferrous sulfate at visit 4 compared to Baseline (BL) | Baseline to approximately 30 days post-baseline (visit 4) |
| pre post difference of volumen-corrected urine iron levels | Pre-post difference of volume-corrected urine iron levels measured before and in the first urine after the end of i.v. administration, defined as short term safety surrogate marker after administration of the i.v. treatments, compared between Polyglucoferron and Ferric Carboxymaltose (volume corrected iron urine is defined as the ratio between urine iron and urine creatinine). | urine sampled prior to administration and approximately 1 to 8 hours post-baseline |
| Measure | Description | Time Frame |
|---|---|---|
| Proportion of patients with normalization of Hemoglobin (Hb) at visit 4 | measurement of normalization of Hb defined in World Health Organization (WHO) classification | 30 days after baseline (Visit 4) |
| Level of Hb until visit 4 |
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Inclusion Criteria:
Exclusion Criteria:
Pregnancy in female patients or breastfeeding women
Female patients not willing to use a safe method of contraception (PEARL index <1) for the full study period
Severe physical inability, e.g., American society of anesthesiologists (ASA) physical status IV or V
Patients receiving blood transfusion 24 week prior surgery
Non-iron deficiency anaemia, e.g., known Vitamin B12 or folate deficiency, haemoglobinopathy, or unexplained anaemia
Anticipated medical need for erythropoiesis-stimulating agents during the main study period
Patients with hemodynamic instability due to any ongoing bleeding. Absence of ongoing bleeding will be confirmed determined either by decision of two independent physicians or by removal of drainage, whichever occurs earlier in routine care)
Patients with any contraindication to the investigational products, e.g.,
Chronic kidney disease, defined as Glomerular Filtration Rate (GFR) <30 mL/min
Active uncontrolled immune-mediated diseases such as rheumatoid arthritis or inflammatory bowel disease
Primary haematologic disease
Drug or alcohol abuse according to WHO definition
Potentially unreliable patients, and those judged by the investigator to be unsuitable for the study
Current or previous participation in another clinical trial during the last 90 days before screening
Exclusion criteria related to Ferrous sulfate
Exclusion criteria related to Ferric Carboxymaltose:
Exclusion criteria related to Polyglucoferron
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| Name | Affiliation | Role |
|---|---|---|
| Patrick Meybohm, MD | University Hospital of Goethe-University Frankfurt | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Department of Anaesthesiology, Intensive Care Medicine and Pain Therapy, University Hospital of Goethe-University | Frankfurt | Hessia | 60590 | Germany |
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| ID | Term |
|---|---|
| D018798 | Anemia, Iron-Deficiency |
| ID | Term |
|---|---|
| D000747 | Anemia, Hypochromic |
| D000740 | Anemia |
| D006402 | Hematologic Diseases |
| D006425 | Hemic and Lymphatic Diseases |
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| ID | Term |
|---|---|
| C522335 | ferric carboxymaltose |
| C020748 | ferrous sulfate |
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2:2:1 distribution Polyglucoferron, Ferric Carboxymaltose i.v., or oral iron substitution with Ferrous sulfate. After safety assessment of first 35 patients treated with Polyglucoferron or Ferric Carboxymaltose i.v. respectively, Ferric Carboxymaltose arm will be closed.
Remaining patients will be distributed in an 2:1 mode to Polyglucoferron or oral iron
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| Ferric carboxymaltose | Drug | intravenous administration |
|
|
| Ferrous Sulfate | Drug | oral administration |
|
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determination of levels of Hemoglobin (Hb) (comparison to baseline)
| Baseline to 30 days after baseline (visit 4) |
| Level of Transferrin Saturation (TSAT) until visit 4 | determination of levels of Transferrin Saturation (TSAT) (mean values in comparison to baseline) | Baseline to 30 days after baseline (visit 4) |
| Level of serum-iron until visit 4 | determination of levels of serum-iron (mean values in comparison to baseline) | Baseline to 30 days after baseline (visit 4) |
| Level of serum-transferrin until visit 4 | determination of levels of serum-transferrin (mean values in comparison to baseline) | Baseline to 30 days after baseline (visit 4) |
| Level of serum-ferritin until visit 4 | determination of levels of serum-ferritin (mean values in comparison to baseline) | Baseline to 30 days after baseline (visit 4) |
| Value of serum-phosphate levels at visit 4 (i.v. groups only) | measurement of serum-phosphate levels (mean values in comparison to baseline) | baseline and 30 days after baseline (visit 4) |
| Overall tolerability and number, incidence, seriousness, severity, relationship of Adverse Events (AE) and serious adverse events (SAE) until 30 days after Investigational medicinal product (IMP) administration | determination of number, incidence, seriousness, severity and causality of adverse events and serious adverse events | baseline to 30 days after last IMP administration |
| Level of c-reactive protein on each available visit | Documentation of values of C reactive protein (description of changes in values in comparison to baseline) | baseline to 30 days after baseline (visit 4) |
| Values of ALT on each available visit | Documentation of values of ALT (description of changes in values in comparison to baseline) | baseline to 30 days after baseline (visit 4) |
| Values of AST on each available visit | Documentation of values of AST (description of changes in values in comparison to baseline) | baseline to 30 days after baseline (visit 4) |
| Values of gamma-glutamyltransferase on each available visit | Documentation of values of gamma-glutamyltransferase (description of changes in values in comparison to baseline) | baseline to 30 days after baseline (visit 4) |
| Values of urea nitrogen on each available visit | Documentation of values of urea nitrogen (description of changes in values in comparison to baseline) | baseline to 30 days after baseline (visit 4) |
| Values of serum creatinine on each available visit | Documentation of values of serum creatinine (description of changes in values in comparison to baseline) | baseline to 30 days after baseline (visit 4) |
| Values of white blood cells on each available visit | Documentation of values of white blood cells (description of changes in values in comparison to baseline) | baseline to 30 days after baseline (visit 4) |
| Values of thrombocytes on each available visit | Documentation of values of thrombocytes (description of changes in values in comparison to baseline) | baseline to 30 days after baseline (visit 4) |
| Changes in systolic blood pressure on each available visit | Documentation of vital signs as systolic blood pressure | baseline to 30 days after baseline (visit 4) |
| Changes in body temperature on each available visit | Documentation of body temperature | baseline to 30 days after baseline (visit 4) |
| Changes in pulse rate on each available visit | Documentation of pulse rate | baseline to 30 days after baseline (visit 4) |
| Changes in diastolic blood pressure on each available visit | Documentation of vital signs as diastolic blood pressure | baseline to 30 days after baseline (visit 4) |
| Assessment of general conditions on each available visit | Documentation of clinical assessments of general condition will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of Skin on each available visit | Documentation of clinical assessments of Skin will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of eyes on each available visit | Documentation of clinical assessments of eyes will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of ears on each available visit | Documentation of clinical assessments of ears will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of mouth on each available visit | Documentation of clinical assessments of mouth will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of nose on each available visit | Documentation of clinical assessments of nose will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of throat on each available visit | Documentation of clinical assessments of throat will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of cardiovascular system on each available visit | Documentation of clinical assessments of cardiovascular system will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of respiratory system on each available visit | Documentation of clinical assessments of respiratory system,will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of abdomen on each available visit | Documentation of clinical assessments of abdomen will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of gastrointestinal tract on each available visit | Documentation of clinical assessments of gastrointestinal tract will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| clinical assessments of kidneys on each available visit | Documentation of clinical assessments of kidneys will be made by investigator - changes to preceding visits and in comparison to baseline will be documented | baseline to 30 days after baseline (visit 4) |
| AEs related to injection/ infusion site reactions (i.v. treatment arms only) and hypersensitivity reactions | Documentation of numbers of adverse events related to injection/infusion site reactions (i.v. treatment arms only) and hypersensitivity reactions | baseline to 30 days after last IMP administration |
| Number of deaths from any cause until visit 4 | documentation of number of deaths | baseline to 30 days after baseline (visit 4) |
| Proportion of units of allogenic red blood cell transfusion from BL until visit 4 | Documentation of number of units of allogenic red blood cell transfusion | Baseline to 30 days after baseline (visit 4) |
| Proportion of patients with need of allogenic red blood cell transfusion from BL until visit 4 | Documentation of the use of allogenic red blood cell transfusion | Baseline to 30 days after baseline (visit 4) |
| treatment effect on change in Quality of Life (SF36) at visit 4 compared to BL | documentation of quality of life in the Short Form Health Survey (SF36) with 36 items relying upon patient self-reporting. It contains eight sections: vitality, physical functioning, bodily pain, general health perceptions, physical role functioning, emotional role functioning, social role functioning, mental health. The SF-36 consists of eight scaled scores which are the weighted sums of the questions in their section. Each scale is directly transformed into a 0-100 scale on the assumption that each question carries equal weight. The lower the score the more disability. The higher the score the less disability i.e., a score of zero is equivalent to maximum disability and a score of 100 is equivalent to no disability. | Baseline to 30 days after baseline (visit 4) |
| Duration of hospital stay (days) until visit 4 | documentation of days in hospital | Baseline to 30 days after baseline (visit 4) |
| Level ofl iron in plasma after end of iron administration (for the i.v. groups (safety analysis group) only) | measurement of iron level in plasma | time points directly after administration of intravenous (i.v.) treatment (approximately 15 minutes post-baseline) |
| Level of iron in plasma after urine sampling (for the i.v. groups (safety analysis group) only) | measurement of iron level in plasma | time points after urine sampling (approximately 1 to 8 hours post-baseline) |
| D000090463 |
| Iron Deficiencies |
| D019189 | Iron Metabolism Disorders |
| D008659 | Metabolic Diseases |
| D009750 | Nutritional and Metabolic Diseases |