Adult Dosing

Iron deficiency anemia

• Start 0.5 mL (25 mg) IM/IV test dose given 1 hr prior to therapy
• Total dose in mL = [0.0442 × LBW × (desired Hb - observed Hb)] + (0.26 x LBW)
• Max dose: 100 mg/dose

Iron replacement

• Start 0.5 mL (25 mg) IM/IV test dose given 1 hr prior to therapy
• Total dose (mg) = Blood loss (mL) x hematocrit
• Max: 100 mg/dose

• LBW: Lean body weight in kg
• Males: LBW = 50 kg + 2.3 kg for each inch of patient's height over 5 ft
• Females: LBW= 45.5 kg + 2.3 kg for each inch of patient's height over 5 ft
• Do not mix iron dextran with other medications or add to parenteral nutrition solutions for intravenous infusion

Pediatric Dosing

• Safety and effectiveness in pediatric patients <4 months of age have not been established

Iron deficiency anemia

>4 months, 5-15 kgs (11-33 lbs)

• Start 0.25 mL (infants), 0.5 mL (children) IM/IV test dose given 1 hr prior to therapy
• Total dose in mL = [0.0442 × W × (desired Hb - observed Hb)] + (0.26 x W)
• Max: 0.5 mL/dose if wt <5 kgs; 1 mL/dose if wt 5-10 kgs; 2 mL/dose if wt >10 kgs

>4months, >15 kgs

• Start 0.5 mL (25 mg) IM/IV test dose given 1 hr prior to therapy
• Total dose in mL = [0.0442 × LBW × (desired Hb - observed Hb) ] + (0.26 x LBW)

Iron replacement

>4 months

• Start 0.25 mL (infants), 0.5 mL (children) IM/IV test dose given 1 hr prior to therapy
• Total dose (mg) = Blood loss (mL) x hematocrit
• Max: 0.5 mL/dose if wt <5 kgs; 1 mL/dose if wt 5-10 kgs; 2 mL/dose if wt >10 kgs

• W: Weight in kg
• LBW: Lean body weight in kg
• Males: LBW = 50 kg + 2.3 kg for each inch of patient's height over 5 ft
• Females: LBW = 45.5 kg + 2.3 kg for each inch of patient's height over 5 ft
• Do not mix iron dextran with other medications or add to parenteral nutrition solutions for intravenous infusion

[Outline]

• Adult Dosing
• Pediatric Dosing

• Treatment of patients with iron deficiency anemia in whom oral administration of iron is unsatisfactory or impossible

• Hypersensitivity to any of the ingredients of the product
• Anemias not due to iron deficiency
• Hemochromatosis
• Hemosiderosis
• Acute infectious kidney diseases
• Infants <4 months of age

• Anaphylactic-type reactions, including fatalities, are associated with parenteral iron dextran injection
• During parenteral iron dextran administration, resuscitation equipment and personnel trained in the detection and treatment of anaphylactic-type reactions should be readily available
• Administer a test dose of parenteral iron dextran prior to the first therapeutic dose. If no signs or symptoms of anaphylactic-type reactions follow the test dose, administer the full therapeutic dose
• Observe for signs and symptoms of anaphylactic-type reactions during all parenteral iron dextran administrations. Fatal reactions have followed the test dose of iron dextran injection. Fatal reactions have also occurred in situations where the test dose was tolerated
• Iron dextran should be used only in patients in whom clinical and laboratory investigations have confirmed an iron deficient state not amenable to oral iron therapy
• Patients with a history of drug allergy or multiple drug allergies may be at increased risk of anaphylactic-type reactions to iron dextran injection

Renal Dose Adjustment

• Acute infectious kidney disease: Contraindicated

Hepatic Dose Adjustment

• Serious impairment: Dose adjustments not defined, extreme caution advised

• Anaphylactic-type reactions, including fatal reactions, are associated with parenteral iron dextran. Administer where resuscitation equipments and personnel trained in treatment of anaphylactic-type reactions are readily available [US Black Box Warning]
• Administer test dose prior to first therapeutic dose; continue with full therapeutic dose if no signs/symptoms of anaphylactic-type reactions occur. Observe for signs/symptoms suggestive of anaphylactic-type reactions during all injections. Fatal reactions have occurred following test dose and even when test dose was tolerated [US Black Box Warning]
• Use only if clinical and laboratory investigations have confirmed iron deficient state not amenable to oral iron therapy [US Black Box Warning]
• Patients with a history of drug allergy or multiple drug allergies may be at increased risk of anaphylactic reactions [US Black Box Warning]
• Concomitant use of angiotensin-converting enzyme inhibitor drugs may increase the risk for reactions to an iron dextran product
• Large IV doses, such as total dose infusions (TDI), have been associated with an increased incidence of adverse events such as arthralgia, backache, chills, dizziness, moderate to high fever, headache, malaise, myalgia, nausea, and vomiting. The adverse reactions are usually delayed 1 to 2 days after administration and symptoms usually subside within 3 to 4 days
• Contraindicated in patients with acute phase of infectious kidney disease
• Iron dextran may exacerbate CV complications in patients with preexisting CV disease
• Risk of carcinogenesis may attend the IM injection of iron-carbohydrate complexes, and these complexes have been found to produce sarcoma in experimental animals when administered in large doses or small doses injected repeatedly at the same site
• Several cases have been reported with tumors at the injection site in humans who had previously received IM injections of iron-carbohydrate complexes
• Unwarranted therapy with parenteral iron will cause excess storage of iron and possibly cause exogenous hemosiderosis, especially in patients with hemoglobinopathies and other refractory anemias
• Use with caution in patients with history of significant allergies or asthma
• Hypersensitivity, including anaphylaxis, may occur. Epinephrine should be immediately available in such acute hypersensitivity reactions
• Acute exacerbation of joint pain and swelling after IV administration have been seen in iron deficiency patients with rheumatoid arthritis
• Ensure to determine hemoglobin, hematocrit, serum ferritin, and transferrin saturation before starting therapy and periodically during treatment

Cautions: Use cautiously in

• Serious hepatic impairment

Pregnancy Category:C

Breastfeeding: Excreted in breast milk in trace amounts. Manufacturer advises caution.

• CV: Chest pain, chest tightness, shock, cardiac arrest, hypotension, hypertension, tachycardia, bradycardia, flushing, arrhythmias
• NEURO: Convulsions, seizures, syncope, headache, weakness, unresponsiveness, paresthesias, dizziness, disorientation, numbness, unconsciousness
• MISC: Febrile episodes, malaise, sweating, shivering, chills, hemosiderosis
• RESP: Respiratory arrest, dyspnea, bronchospasm, wheezing
• DERM: Urticaria, pruritus, purpura, rash, cyanosis
• GU: Hematuria
• GI: Abdominal pain, altered taste, nausea, vomiting, diarrhea
• HEMA: Leucocytosis, lymphadenopathy
• MUSC: Arthralgia, arthritis, myalgia, backache, sterile abscess, atrophy or fibrosis, underlying tissue discoloration (staining)
• LOCAL: Cellulitis, swelling, inflammation, local phlebitis

• Anti-anemic (iron supplement); enters the bloodstream and is transported to the organs of the reticuloendothelial system (liver, spleen, bone marrow) where it is separated from the dextran molecule and becomes part of iron stores
• Metabolism: Removed from plasma by the cells of the reticuloendothelial system, which split the drug into its components
• Excretion: Unknown
• Half-Life: 5-20 hours

US Trade Name(s)

• Dexferrum
• INFeD
• Proferdex

US Availability

Dexferrum, INFeD, Proferdex

• INJ: 50 mg/mL (2 mL vials)

Canadian Trade Name(s)

• Dexiron
• Infufer

Canadian Availability

Dexiron, Infufer

• INJ: 50 mg/mL

UK Trade Name(s)

• CosmoFer

UK Availability

CosmoFer

• INJ: 50 mg/mL (2, 5, 10 mL amp)

Australian Trade Name(s)

• N/A

Australian Availability

• N/A

[Outline]

Nutrition/Electrolytes

Iron Products