Lenograstim RDNA
Lenograstim RDNA Uses, Dosage, Side Effects, Food Interaction and all others data.
Lenograstim RDNA is the glycosylated recombinant form of human granulocyte colony stimulating factor. Lenograstim RDNA accelerates neutrophil recovery significantly after chemotherapy, with beneficial effects on clinical end-points such as incidence of laboratory-confirmed infection and length of hospital stay. Chemotherapy dose intensity has also been increased in patients receiving lenograstim, notably those with breast or small cell lung cancer, although improvements in tumour response and survival have not been demonstrated. Lenograstim RDNA also assists neutrophil recovery in patients undergoing bone marrow transplantation, and stimulates the production of peripheral blood stem cells (PBSCs) for autologous transfusion after aggressive chemotherapy.
Lenograstim RDNA has been confirmed as a valuable adjunct to minimise the haematological toxicity of myelosuppressive chemotherapy in patients with malignant disease. The drug also enhances neutrophil recovery in patients undergoing stem cell rescue, and assists peripheral blood progenitor cells mobilisation.
Trade Name | Lenograstim RDNA |
Generic | Lenograstim |
Lenograstim Other Names | Lenograstim, Lenograstim (genetical recombination), Lenograstim rDNA |
Type | |
Groups | Approved, Investigational |
Therapeutic Class | Haematopoietic Agents |
Manufacturer | |
Available Country | |
Last Updated: | September 19, 2023 at 7:00 am |
Uses
Lenograstim RDNA (rHuG-CSF) 13.4 million International Units (equivalent to 105 micrograms) per ml after reconstitution
Lenograstim RDNA (rHuG-CSF) 33.6 million International Units (equivalent to 263 micrograms) per ml after reconstitution
The drug is used to reduce the risk of life-threatening infection in patients with neutropenia, particularly after cytotoxic chemotherapy. Lenograstim RDNA is used for a treatment to reduce the duration of neutropenia and the severity of infections in patients with non-myeloid malignancy who have undergone autologous or allogeneic bone marrow transplantation, or treatment with established cytotoxic chemotherapy and in addition to reduce the incidence of infection associated with established cytotoxic chemotherapy. Lenograstim RDNA is also used to mobilise peripheral blood progenitor cells (PBPCs) with Lenograstim RDNA alone, or after myelosuppressive chemotherapy, in order to accelerate haematopoietic recovery by infusion of such cells, after myelosuppressive or myeloablative therapy. Lenograstim RDNA is also used to accelerate the engraftment of these cells after their reinfusion.
Lenograstim RDNA is also used to associated treatment for these conditions: Neutropenia, Mobilization of hematopoietic stem cells therapy
How Lenograstim RDNA works
Lenograstim RDNA is the glycosylated recombinant form of human granulocyte colony stimulating factor. Lenograstim RDNA accelerates neutrophil recovery significantly after chemotherapy, with beneficial effects on clinical end-points such as incidence of laboratory-confirmed infection and length of hospital stay. Chemotherapy dose intensity has also been increased in patients receiving lenograstim, notably those with breast or small cell lung cancer, although improvements in tumour response and survival have not been demonstrated. Lenograstim RDNA also assists neutrophil recovery in patients undergoing bone marrow transplantation, and stimulates the production of peripheral blood stem cells (PBSCs) for autologous transfusion after aggressive chemotherapy.
Dosage
Lenograstim RDNA dosage
Intravenous-Neutropenia following bone marrow transplantation:
- Adult: 19.2 million IU/m2 or 150 mcg/m2 daily by IV infusion started the day after transplantation for a maximum of 28 consecutive days.
- Child: >2 yr: 19.2 million IU/m2 or 150 mcg/m2 daily by IV infusion started the day after transplantation for a maximum of 28 consecutive days.
Subcutaneous-
Mobilisation of peripheral blood progenitor cells for autologous peripheral blood stem cell transplantation:
- Adult: As monotherapy: 1.28 million IU/kg or 10 mcg/kg daily for 4-6 days (5-6 days in healthy donors). Following adjunctive myelosuppressive chemotherapy: 19.2 million IU/m2 or 150 mcg/m2daily, started the day after completion of chemotherapy for a maximum of 28 consecutive days.
Subcutaneous-
Chemotherapy-induced neutropenia:
- Adult: 19.2 million IU/m2 or 150 mcg/m2 daily, start the day after completion of chemotherapy for a maximum of 28 consecutive days.
Side Effects
Musculoskeletal pain, bone pain, splenic enlargement, nausea, fever, thrombocytopenia, anaemia, epistaxis, headache, diarrhoea, dysuria, osteoporosis, cutaneous vasculitis, anorexia, Sweet's syndrome, toxic epidermal necrolysis.
Toxicity
Species observed : Human (Man) Test type: TDLo ( Lowest Published Toxic Dose) Route of exposure: Subcutaneous Dose/Duration: 21428mg/kg/15 Toxic Effect: Skin and appendages: Dermatitis, allergic ( after systemic exposure )
Species observed : Rodent - Rat Test type: LD50 Route of exposure: Oral Dose/Duration: >5mg/kg Toxic Effect: Details of toxic effects not reported other than lethal dose value
Species observed : Rodent - Rat Test type: LD50 Route of exposure: Subcutaneous Dose/Duration: >5mg/kg Toxic Effect: Details of toxic effects not reported other than lethal dose value
Species observed : Rodent - Rat Test type: LD50 Route of exposure: Intravenous Dose/Duration: >5mg/kg Toxic Effect: Details of toxic effects not reported other than lethal dose value
Species observed : Mammal - Dog Test type: LD50 Route of exposure: Intravenous Dose/Duration: >5mg/kg Toxic Effect: Details of toxic effects not reported other than lethal dose value
Species observed : Mammal - Dog Test type: LD50 Route of exposure: Subcutaneous Dose/Duration: >5mg/kg Toxic Effect: Details of toxic effects not reported other than lethal dose value
Precaution
Premalignant or malignant myeloid condition; sickle-cell disease; osteoporotic bone disease; signs of pulmonary infiltrates (withdraw treatment). Monitor CBC during therapy. Pregnancy and lactation.
Interaction
Increased risk of myelosuppression with myelosuppressive antineoplastic agents; increased pulmonary toxicity with bleomycin and cyclophosphamide.
Volume of Distribution
Apparent distribution volume (Vd area) is approximately 52 ± 5 mL/kg body weight.
Elimination Route
During repeated dosing (iv and sc routes), peak serum concentrations (at the end of iv infusion or after sc injection) are proportional to the injected dose. Repeated dosing with lenograstim by the two injection routes results in no evidence of drug accumulation.
Half Life
The pharmacokinetic profile of lenograstim is similar in healthy volunteers and cancer patients with elimination half-life (t½β) values of 2.3 - 3.3 hrs (volunteers); 2.8-7.5 hrs (cancer patients) following sc administration, and 0.8 - 2.1 hrs (volunteers); 1.1 - 4.0 hrs (cancer patients) following iv administration.
Clearance
Plasma clearance of lenograstim increased 3-fold (from 50 up to 150 mL/min) during repeated sc dosing.
Elimination Route
Lenograstim RDNA is poorly excreted in urine as intact compound (less than 1% of the dose).
Pregnancy & Breastfeeding use
Pregnancy category is not classified.
Contraindication
Myeloid malignancies. Not to be used for 24 hr before or after cytotoxic chemotherapy.
Storage Condition
Should be stored in cool and dry place
Innovators Monograph
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Lenograstim RDNA contains Lenograstim see full prescribing information from innovator Lenograstim RDNA Monograph, Lenograstim RDNA MSDS, Lenograstim RDNA FDA label