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Cetuximab- Erbitux

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Structure Mechanism of action Production Administration Monitoring Side effects Toxicology

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JSS SCIENCE AND TECHNOLOGY UNIVERSITY Sri Jayachamarajendra College of Engineering JSS TI Campus, Mysuru 570006 PHARMACEUTICAL BIOTECHNOLOGY BT550 “Cetuximab: Structure, Mechanism of action, Application, Side effects” MANASAY 5TH SEMESTER BIOTECHNOLOGY 01JST18BT012
CETUXIMAB •Drug type: Cetuximab is an anti-cancer ("anti-neoplastic") targeted therapy. This medication is classified as a "monoclonal antibody" and "Epidermal Growth Factor Receptor (EGFR) Inhibitor. •Trade name: Erbitux® •Other name: C225 •Half life: 114 hours (range 75-188 hours) •Clearance rate: Female patients had 25% lower intrinsic clearance than male patients. Manufacture •Eli lilly and company •Merck KGaA Sales •Cetuximab is given by intravenous therapy and costs up to $30,000 for eight weeks of treatment per patient. •Merck KGaA had 887 million euros ($1.15 billion) in Erbitux sales in 2012, from head and neck as well as bowel cancer, while Bristol-Myers Squibb generated $702 million in sales from the drug. •Erbitux was the eighth best-selling cancer drug of 2013, with sales of $1.87 billion
Cetuximab is used for treatment of Metastatic Colorectal Cancer (cancer spread beyond the colon or rectum) Non-small Cell Lung Cancer Squamous Cell Cancer of the Head and Neck Squamous Cell Skin Cancer
Structure •Recombinant, human/mouse chimeric monoclonal antibody •Binds specifically to the extracellular domain of the human epidermal growth factor receptor (EGFR). •Composed of the Fv regions of a murine anti-EGFR antibody with human IgG1 heavy and kappa light chain constant regions . •Molecular weight : 152 kDa •Chemical formula C6484H10042N1732O2023S36 •Produced in mammalian (murine myeloma) cell culture.
ERBITUX (cetuximab) injection for intravenous use, is a sterile, preservative-free, clear, colorless solution, which may contain a small amount of visible, white, amorphous cetuximab particulates in a single-dose vial. Each 1 mL of solution contains : •2 mg of cetuximab •sodium chloride (8.48 mg) •sodium phosphate dibasic heptahydrate (1.88 mg) •sodium phosphate monobasic monohydrate (0.41 mg) •Water for Injection •USP at pH of 7.0 to 7.4.
Mechanism of Action
 Cell culture and harvesting  Purification  Gene construct  Cell banking system  Control of steps  Biochemical characterisation  Control of drug substance  Product development and finished product  Process validation Production
Storage and handling  Store vials under refrigeration at 2 C to 8 C  Do not freeze or shake  Increased particulate formation may occur at temperatures at or below 0 C  Discard any remaining solution in the infusion container after 8 hours at controlled room temperature or after 12 hours at 2 C to 8C.  Discard any unused portion of the vial.
Administration •The administration of the drug is via IV infusion with a loading dose lasting over 2 hours, weekly maintenance dose over 1 hour. •Do not shake or dilute. •Administer via infusion pump or syringe pump. •Following the infusion, an observation period of 1 hour is recommended; longer observation time following an infusion reaction may be necessary. •Dosing prescribed as initial loading dose 400 mg/m2 infused over 120 minutes and maintenance dose of 250 mg/m2 infused over 60 minutes for both colorectal cancer, metastatic, and head and neck cancer (squamous cell)
Monitoring  Vital signs during infusion and observe for at least 1-hour post-infusion.  Patients developing dermatologic toxicities should be monitored for the development of complications.  Periodic monitoring of serum magnesium, calcium, and potassium are recommended to continue over an interval consistent with the half-life (8 weeks); monitor closely (during and after treatment) for cetuximab plus radiation therapy.
Side Effects:  Generalized weakness, fatigue,  Weight loss and poor appetite  Diarrhea, Nausea and Vomiting  Abdominal pain, Constipation  Inflammation of the mouth  Low magnesium level  Low blood counts.white cells may temporarily decrease (neutropenia).  Difficulty breathing, Cough  Liver problems (hepatotoxicity and elevated liver enzymes)  Headache  Nail changes - inflammation of the skin surrounding a fingernail or toenail
Toxicity  Cardiopulmonary arrest  Infusion reactions  Dermatologic toxicity  Interstitial lung disease  Electrolyte abnormality
THANK YOU

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Cetuximab- Erbitux

  • 1. JSS SCIENCE AND TECHNOLOGY UNIVERSITY Sri Jayachamarajendra College of Engineering JSS TI Campus, Mysuru 570006 PHARMACEUTICAL BIOTECHNOLOGY BT550 “Cetuximab: Structure, Mechanism of action, Application, Side effects” MANASAY 5TH SEMESTER BIOTECHNOLOGY 01JST18BT012
  • 2. CETUXIMAB •Drug type: Cetuximab is an anti-cancer ("anti-neoplastic") targeted therapy. This medication is classified as a "monoclonal antibody" and "Epidermal Growth Factor Receptor (EGFR) Inhibitor. •Trade name: Erbitux® •Other name: C225 •Half life: 114 hours (range 75-188 hours) •Clearance rate: Female patients had 25% lower intrinsic clearance than male patients. Manufacture •Eli lilly and company •Merck KGaA Sales •Cetuximab is given by intravenous therapy and costs up to $30,000 for eight weeks of treatment per patient. •Merck KGaA had 887 million euros ($1.15 billion) in Erbitux sales in 2012, from head and neck as well as bowel cancer, while Bristol-Myers Squibb generated $702 million in sales from the drug. •Erbitux was the eighth best-selling cancer drug of 2013, with sales of $1.87 billion
  • 3. Cetuximab is used for treatment of Metastatic Colorectal Cancer (cancer spread beyond the colon or rectum) Non-small Cell Lung Cancer Squamous Cell Cancer of the Head and Neck Squamous Cell Skin Cancer
  • 4. Structure •Recombinant, human/mouse chimeric monoclonal antibody •Binds specifically to the extracellular domain of the human epidermal growth factor receptor (EGFR). •Composed of the Fv regions of a murine anti-EGFR antibody with human IgG1 heavy and kappa light chain constant regions . •Molecular weight : 152 kDa •Chemical formula C6484H10042N1732O2023S36 •Produced in mammalian (murine myeloma) cell culture.
  • 5. ERBITUX (cetuximab) injection for intravenous use, is a sterile, preservative-free, clear, colorless solution, which may contain a small amount of visible, white, amorphous cetuximab particulates in a single-dose vial. Each 1 mL of solution contains : •2 mg of cetuximab •sodium chloride (8.48 mg) •sodium phosphate dibasic heptahydrate (1.88 mg) •sodium phosphate monobasic monohydrate (0.41 mg) •Water for Injection •USP at pH of 7.0 to 7.4.
  • 7.  Cell culture and harvesting  Purification  Gene construct  Cell banking system  Control of steps  Biochemical characterisation  Control of drug substance  Product development and finished product  Process validation Production
  • 8. Storage and handling  Store vials under refrigeration at 2 C to 8 C  Do not freeze or shake  Increased particulate formation may occur at temperatures at or below 0 C  Discard any remaining solution in the infusion container after 8 hours at controlled room temperature or after 12 hours at 2 C to 8C.  Discard any unused portion of the vial.
  • 9. Administration •The administration of the drug is via IV infusion with a loading dose lasting over 2 hours, weekly maintenance dose over 1 hour. •Do not shake or dilute. •Administer via infusion pump or syringe pump. •Following the infusion, an observation period of 1 hour is recommended; longer observation time following an infusion reaction may be necessary. •Dosing prescribed as initial loading dose 400 mg/m2 infused over 120 minutes and maintenance dose of 250 mg/m2 infused over 60 minutes for both colorectal cancer, metastatic, and head and neck cancer (squamous cell)
  • 10. Monitoring  Vital signs during infusion and observe for at least 1-hour post-infusion.  Patients developing dermatologic toxicities should be monitored for the development of complications.  Periodic monitoring of serum magnesium, calcium, and potassium are recommended to continue over an interval consistent with the half-life (8 weeks); monitor closely (during and after treatment) for cetuximab plus radiation therapy.
  • 11. Side Effects:  Generalized weakness, fatigue,  Weight loss and poor appetite  Diarrhea, Nausea and Vomiting  Abdominal pain, Constipation  Inflammation of the mouth  Low magnesium level  Low blood counts.white cells may temporarily decrease (neutropenia).  Difficulty breathing, Cough  Liver problems (hepatotoxicity and elevated liver enzymes)  Headache  Nail changes - inflammation of the skin surrounding a fingernail or toenail
  • 12. Toxicity  Cardiopulmonary arrest  Infusion reactions  Dermatologic toxicity  Interstitial lung disease  Electrolyte abnormality