Systemic Anti-Cancer Therapy Regimen Library
HyperCVAD [over 60 years] - Part B with CNS prophylaxis for High Risk (LEU ALL - HyperCVAD Part A and B followed by POMP Maintenance [over 60 years])
Treatment Overview
Alternates with a cycle of Part A every 21 days, or sooner if counts have recovered.
Intrathecal therapy included in this regimen is for CNS prophylaxis for patients with High Risk.
High dose metHOTREXATe
- metHOTREXATe levels MUST be measured once every 24 hours.
- Intravenous alkalinized fluids MUST be commenced at least 6 hours before the start of metHOTREXATe infusion and MUST continue until the metHOTREXATe serum level is less than 0.05 µmol/L – 0.1 µmol/L (level as per institutional practice). Additional oral alkalinization can be considered as Ural® 2 sachets orally the night before and 2 sachets the morning of high dose metHOTREXATe infusion.
- Before commencing the high dose metHOTREXATe infusion, urinary pH MUST be 7.5 or above (pH 7.5 to 8.0).
- Closely monitor renal function, electrolytes, fluid balance, and weight.
- foliNIc acid MUST start 36 hours after start of metHOTREXATe infusion and MUST continue to be administered until serum metHOTREXATe level is less than 0.05 µmol/L – 0.1 µmol/L (level as per institutional practice).
This regimen contains a medicine where one or more biosimilars may exist. Any biosimilars used have been reviewed by the regulator (Medsafe) and relevant specialists were consulted nationally. Where regulators, in consultation with relevant specialists, have agreed that there are no clinically significant differences in either safety or effectiveness between a biosimilar and originator product, these drugs may be used interchangeably.
Cycles 1 to 4 - 21 days
foliNIc acid: MUST start 36 hours after start of metHOTREXATe infusion and MUST continue to be administered every 6 hours until serum metHOTREXATe level is less than 0.05 µmol/L – 0.1 µmol/L (level as per institutional practice).
cytarabine: Check metHOTREXATe level and renal function post high dose metHOTREXATe prior to administration of cytarabine:
- If metHOTREXATe level greater than 20 µmol/L post completion of metHOTREXATe infusion, OR
- Urine output is reduced, OR
- Serum creatinine has increased, cytarabine dose should be withheld and reviewed by the haematologist.
Intrathecal metHOTREXATe: For Ommaya reservoir reduce dose to 6 mg intraventricularly.
filgrastim: Give filgrastim 5 micrograms/kg subcutaneously ONCE daily from Day 4 until neutrophil recovery past the nadir.
Cycle details
Cycles 1 to 4 - 21 days
| Medication | Dose | Route | Days | Max Duration |
|---|---|---|---|---|
| methylprednisolone | 50 mg Twice daily | intravenous | 1, 2, 3 | 1 minutes |
| potassium chloride 20mmol/1000mL + sodium chloride 0.18% + glucose 4% | 125 mL/m²/hour | intravenous | 1 to 4 | |
| sodium bicarbonate | 50 mmol | intravenous | 1 to 4 | |
| acetazolamide * | 250 mg Four times daily | oral administration | 1 to 4 | |
| metHOTREXATe | 200 mg/m² | intravenous | 1 | 120 minutes |
| metHOTREXATe | 800 mg/m² | intravenous | 1 | 22 hours |
| foliNIc acid (as calcium folinate) | 50 mg flat dosing | intravenous | 2 | 2 minutes |
| foliNIc acid (as calcium folinate) | 30 mg flat dosing Every six hours | intravenous | 2, 3, 4 | 2 minutes |
| cytarabine | 1000 mg/m² Twice daily | intravenous | 2, 3 | 3 hours |
| prednisolone acetate 1% (10 mg/mL) eye drops * | 1 Drop Every four hours | application to the eye | 2 to 5 | |
| metHOTREXATe | 12 mg flat dosing | intrathecal injection | 2 | |
| filgrastim | 5 microgram/kg Once daily | subcutaneous injection | 4 | |
| cytarabine | 100 mg flat dosing | intrathecal injection | 8 |
foliNIc acid: MUST start 36 hours after start of metHOTREXATe infusion and MUST continue to be administered every 6 hours until serum metHOTREXATe level is less than 0.05 µmol/L – 0.1 µmol/L (level as per institutional practice).
cytarabine: Check metHOTREXATe level and renal function post high dose metHOTREXATe prior to administration of cytarabine:
- If metHOTREXATe level greater than 20 µmol/L post completion of metHOTREXATe infusion, OR
- Urine output is reduced, OR
- Serum creatinine has increased, cytarabine dose should be withheld and reviewed by the haematologist.
Intrathecal metHOTREXATe: For Ommaya reservoir reduce dose to 6 mg intraventricularly.
filgrastim: Give filgrastim 5 micrograms/kg subcutaneously ONCE daily from Day 4 until neutrophil recovery past the nadir.
Full details
Cycles 1 to 4 - 21 days
Day: 1
| Medication | Dose | Route | Max duration | Details |
|---|---|---|---|---|
| methylprednisolone | 50 mg Twice daily | intravenous | 1 minutes | |
| potassium chloride 20mmol/1000mL + sodium chloride 0.18% + glucose 4% | 125 mL/m²/hour | intravenous |
Instructions:
|
|
| sodium bicarbonate | 50 mmol | intravenous |
Instructions:
|
|
| acetazolamide * | 250 mg Four times daily | oral administration |
Instructions:
When required.
|
|
| metHOTREXATe | 200 mg/m² | intravenous | 120 minutes | |
| metHOTREXATe | 800 mg/m² | intravenous | 22 hours |
Instructions:
Starting immediately after the 120 minute metHOTREXATe infusion. |
Day: 2
| Medication | Dose | Route | Max duration | Details |
|---|---|---|---|---|
| methylprednisolone | 50 mg Twice daily | intravenous | 1 minutes | |
| potassium chloride 20mmol/1000mL + sodium chloride 0.18% + glucose 4% | 125 mL/m²/hour | intravenous |
Instructions:
|
|
| sodium bicarbonate | 50 mmol | intravenous |
Instructions:
|
|
| acetazolamide * | 250 mg Four times daily | oral administration |
Instructions:
When required.
|
|
| foliNIc acid (as calcium folinate) | 50 mg flat dosing | intravenous | 2 minutes |
Instructions:
Administer 36 hours after start of metHOTREXATe infusion for 1 dose, follow with 30 mg dosing every 6 hours. |
| foliNIc acid (as calcium folinate) | 30 mg flat dosing Every six hours | intravenous | 2 minutes |
Instructions:
|
| cytarabine | 1000 mg/m² Twice daily | intravenous | 3 hours |
Instructions:
Every 12 hours. Check metHOTREXATe level and renal function post high dose metHOTREXATe prior to administration of cytarabine:
|
| prednisolone acetate 1% (10 mg/mL) eye drops * | 1 Drop Every four hours | application to the eye |
Instructions:
Instil ONE drop into each eye every FOUR hours on days 2 to 5. |
|
| metHOTREXATe | 12 mg flat dosing | intrathecal injection |
Instructions:
|
Day: 3
| Medication | Dose | Route | Max duration | Details |
|---|---|---|---|---|
| methylprednisolone | 50 mg Twice daily | intravenous | 1 minutes | |
| potassium chloride 20mmol/1000mL + sodium chloride 0.18% + glucose 4% | 125 mL/m²/hour | intravenous |
Instructions:
|
|
| sodium bicarbonate | 50 mmol | intravenous |
Instructions:
|
|
| acetazolamide * | 250 mg Four times daily | oral administration |
Instructions:
When required.
|
|
| foliNIc acid (as calcium folinate) | 30 mg flat dosing Every six hours | intravenous | 2 minutes |
Instructions:
|
| cytarabine | 1000 mg/m² Twice daily | intravenous | 3 hours |
Instructions:
Every 12 hours. Check metHOTREXATe level and renal function post high dose metHOTREXATe prior to administration of cytarabine:
|
| prednisolone acetate 1% (10 mg/mL) eye drops * | 1 Drop Every four hours | application to the eye |
Instructions:
Instil ONE drop into each eye every FOUR hours on days 2 to 5. |
Day: 4
| Medication | Dose | Route | Max duration | Details |
|---|---|---|---|---|
| potassium chloride 20mmol/1000mL + sodium chloride 0.18% + glucose 4% | 125 mL/m²/hour | intravenous |
Instructions:
|
|
| sodium bicarbonate | 50 mmol | intravenous |
Instructions:
|
|
| acetazolamide * | 250 mg Four times daily | oral administration |
Instructions:
When required.
|
|
| foliNIc acid (as calcium folinate) | 30 mg flat dosing Every six hours | intravenous | 2 minutes |
Instructions:
|
| prednisolone acetate 1% (10 mg/mL) eye drops * | 1 Drop Every four hours | application to the eye |
Instructions:
Instil ONE drop into each eye every FOUR hours on days 2 to 5. |
|
| filgrastim | 5 microgram/kg Once daily | subcutaneous injection |
Instructions:
|
Day: 5
| Medication | Dose | Route | Max duration | Details |
|---|---|---|---|---|
| prednisolone acetate 1% (10 mg/mL) eye drops * | 1 Drop Every four hours | application to the eye |
Instructions:
Instil ONE drop into each eye every FOUR hours on days 2 to 5. |
Day: 8
| Medication | Dose | Route | Max duration | Details |
|---|---|---|---|---|
| cytarabine | 100 mg flat dosing | intrathecal injection |
Instructions:
Adhere to local institution policy for intrathecal administration. |
Supportive Care Factors
| Factor | Value |
|---|---|
| Antifungal prophylaxis: | Routine antifungal prophylaxis recommended |
| Antiviral prophylaxis for herpes virus: | Routine antiviral prophylaxis recommended |
| Emetogenicity: | Medium |
| Folinic acid rescue for high dose methotrexate: | Mandatory |
| Gastroprotection: | Gastroprotection is recommended |
| Growth factor support: | Recommended for primary prophylaxis |
| Hydration: | Routine hydration recommended |
| Ocular toxicity risk: | High - administer corticosteroid eyedrops to minimise corneal toxicity |
| Pneumocystis jirovecii pneumonia (PJP) prophylaxis: | Routine antibiotic prophylaxis recommended |
| Tumour lysis syndrome prophylaxis: | Tumour lysis syndrome prophylaxis may be considered |
Antiviral prophylaxis for hepatitis B virus: Guidance is limited to high-risk anti-cancer medicines. Clinicians will need to assess individual patient risk for other anti-cancer medicines.
Emetogenicity: MEDIUM day 1 to 3, high dose metHOTREXATe may be highly emetogenic in certain patients.
Gastroprotection: Use an H2 receptor antagonist as a gastroprotective agent for short term use while patient is receiving corticosteroid treatment doses. Do not use proton pump inhibitors with high dose metHOTREXATe.
PJP prophylaxis: If trimethoprim + sulfamethoxazole is used as prophylaxis, it is recommended to withhold at least 48 hours prior to high dose metHOTREXATe administration and until serum metHOTREXATe level is less than 0.05 µmol/L – 0.1µmol/L (as per institutional practice).
Tumour lysis syndrome prophylaxis: May be considered if not in complete remission.
References
* The medicines, doses, combinations, and schedule in this treatment regimen have been carefully reviewed against international best practice guidelines by specialists in medical oncology around New Zealand and this advice has been accepted for publication by Te Aho o Te Kahu (the Cancer Control Agency). Sometimes medicines that are used in routine clinical practice have not been through a formal review process by the NZ Medicines Regulator Medsafe and are therefore considered unapproved or off-label. These medicines are legally able to be prescribed through sections 25 and 29 of the Medicines Act and by obtaining informed consent from patients. All treatment regimens listed on this website have been through robust peer review and are considered an accepted standard of care, whether prescribed through sections 25 or 29 or carrying formal Medsafe Approval.
s29: This symbol indicates that some formulations of the associated medicine are legally only able to be prescribed under section 29 of the Medicines Act. You can see which formulations are section 29 by hovering over the s29 symbol. You can access full medication details from the New Zealand Formulary by clicking on the medication name. Each clinician retains full responsibility for ensuring they have complied with all relevant obligations and requirements of section 29 including obtaining informed patient consent prior to prescribing the applicable medicine.