Drug Interaction:
Interacting drugs -summary
+ Nilotinib
CYP450 3A4 inducers eg. carbamazepine, dexemethasone, phenobarbital, rifabutin,
rifampin, rifapentine, St Johns wart
Avoid concomittant use . If coadministration is necessary, the dose of nilotinib
need to reduced
CYP450 3A4 inhibitors eg. atazanavir, clarithromycin, indinavir, itraconazole,
ketoconazole, nefazodone, nelfinavir, ritonavir, saquinavir, telithromycin,
voriconazole
Avoid concomittant use. If coadministration is necessary reduce the dose of nilotinib
to half the original daily dose
P-glycoprotein + Nilotinib or Nilotinib + p-glycoprotein
Nilotinib is a substrate of P-glycoprotein. If nilotinib is coadministered with drugs
that inhibit P-glycoprotein increased concentration of nilotinib are necessary.
Excercise caution
Nilotinib +
CYP3A4 substrate eg cyclosporine.idazolam, pimozide
coadmininstration of nilotinib and midazolam increased exposure.
Use caution when administering nilotinib with CYP3A4 substrates
Warfarin
avoid concurrent use if possible
Indication:
Approved by (DCI) Drug Controller GENERAL - India For Marketing
(Ref- IDMA Publication)
Name of Drug Indication Date of Approval
1.Nilotinib Capsules 29-09-2010
150mg
Treatment of newly diagonised adult patients with philadelphia
chromosome positive Chronic Myeloid Leukemia (PH+CML)
in chronic phase
2.Nilotinib Capsules 10-07-2010
200mg
For the treatment of Chronic accelerated phase Philadelphia
Chromosome Positive Chronic Myelogenous Leukemia (CML)
in adult patients resistent to or intolerant to prior therapy that
included Imatinab
Chronic Myelogenous leukemia ( CML )
Adverse Reaction:
Serious adverse drug reactions-
electrolyte abnormalites, elevated serum lipase, hepatotoxicity, myelosuppression,
and QT prolongation andsuden deaths
Most commonly reported adverse drug reactions-
febrile neutropenia, intracranial hemorrhage, leukopenia, neutropenia, pneumonia,
pyrexia and thrombocytopenia
Sudden death and QT prolongation reported
CNS - asthenia 12% fatigue 26% headache 30%
Dermatologic - pruriitus 26% rash 30%
GI - abdominal pain 10% constipation 20% diarrhea 20% nausea 28%
vomiting 19%
Musculoskeletal - arthalgia 16% back pain 8% bone pain 9%
muscle spasms 10% myalgia 12%
pain in extremity 12%
Respiratory - cough 15% dyspnea 10% nasopharyngitis 14%
Miscellaneous - peripheral edema 10% pyrexia 12%
Contra-Indications:
Hypokalemia, hypomaganesemia, or long QT syndrome
Special Precautions/Warnings-
QT prolongation ad suden deaths- nitotinib prolongs QT interval. Sudden death have reported in patients receiving nilotinib
Do not use nilotinib in patients with hypokalemia, hypomaganesemia or long QT syndrome
Hyopkalemia and hypomaganesemia should be corrected prior to administration of nilotinib
and should be periodically monitored.
Myelosuppresion- myelosuppression was generally reversible and usually managed by
withholding nilotinib temporarily or reducing the dose
Elevated serum lipase - use of nilotinib can cause increases in serum lipase . Caution is
recomended in patients with a history of pancreatitis. Check serum lipase periodically
Hepatoxicity - use of nilotinib may result in elevation of alkaline phosphatase,
AST/ALT and bilirubin. Check hepatic function tests periodically
Electrolyte imbalance - use of nilotinib can cause hyperkalemia, hypocalcemia,
hypokalemia, hyponatremia, and hypophosphatemia. Electrolye imbalance corrected prior to initiating treatment with nilotinib. Monitor electrolytes periodically during treatment
Renal function impairment - because nilotinib and its metabolites are not renally excreted
a decrease in renal clarance is not anticipated in patients with renal function impairment
Hepatic function impairment - caution is recommended in patients with hepatic function
impairment. Closely monitor these patients for QT interval prolongation
Pregnancy- nilotinib can cause fetal harm when administered to a pregnant woman.
Lactation- decide whether to discontinue breast feeding or the drug taking into account
the importance of the drug to the mother.
Children- safety and effectiveness in children have not been established
Elderly- no major differences were observed for safety in patients 65 years of age
and older compared to younger than 65 years of age.
Monitoring- perform complete blod dell counts every 2 weeks for the first 2 months and then monthly therafter.
Obtain ECG at baseline 7 days after initiation and periodically thereafter.
Monitor patients with hepatic function impairment closely for QT prolongation
Dosages/ Overdosage Etc:
Indication-
Chronic Myelogenous leukemia ( CML )
Dosage -
400mg twice daily . Treatment should continue as long as the patient does not show evidence of progression or unacceptable toxicity
If the dose is missed the patient should not take a make-up but should resume taking the next prescribed dose.
Patient Information:
1. Nilotinib doses should be taken twice daily, approximately 12 hours apart, and should not be taken with food.
2. Swallow capsules whole with water
3. Advice patients to take nilotinib on an empty stomach at least 2 hours after a meal
4.Advice patients that no food should be consumed for atleast 1 hour after the dose is taken.
5. Advice patients not to consume grapefruit juice and other food that are known to inhibit
CYP3A at any time during the treatment
6. Advice patients that use of nilotinib during pregnancy may cause harm to the fetus and
should not be taken during pregnancy, unless necessary.
7.Instruct women of child bearing potential to use contraceptives if taking nilotinib.
8. Sexually active women taking nioltinib should use adequate contraceptives
Interaction with Food:
Should not be taken with food
To be taken an empty stomach at least 2 hours after a meal. No food should be consumed
for atleast 1 hour after the dose is taken.
Pregnancy and lactation:
Pregnancy-
Nilotinib can cause fetal harm when administrated to a pregnant woman.
Lactation-
Decide whether to discontinue breast feeding or the drug taking into account
the importance of the drug to the mother.
Children-
Safety and effectiveness in children have not been established
Elderly-
No major differences were observed for safety in patients 65 years of age
and older compared to younger than 65 years of age.