Urological Cancer Chemotherapy Protocols

Department of Medical Oncology Chemotherapy Protocols
Protocol: BEP 3-day (Bleomycin/Etoposide/Cisplatin)
Indications: Germ cell tumours
Schedule:
Drug Dose iv/infusion/oral q
Bleomycin 30,000iu 200mls N. Saline/30mins Days 2, 8 & 15
Etoposide 165mg/m2 1L N. Saline/1hr Days 1, 2 & 3
Cisplatin 50mg/m2 1L N. Saline/4hrs Days 1 & 2
Cycle frequency: Every three weeks Total number of cycles: 3 or 4
Dose modifications: Discuss with Consultant
Administration and safety:

• Anti-emetic group – High
• Delay if neutrophils < 1.0 x 109/L or platelets < 100 x 109/L
• No Bleomycin with 4th cycle
• Ensure adequate renal function
• Pre & post hydration, mannitol, potassium & magnesium
• Do not cap BSA
Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea &

vomiting, mucositis, alopecia, peripheral neuropathy, nephrotoxicity, ototoxicity,
pneumonitis, pulmonary fibrosis, constipation, diarrhoea, carcinogenesis, infertility
Symptomatic treatment of side effects: Mouth care, encourage oral fluids
Investigations
Pre-treatment:
• History and Examination
• Performance score, weight
• FBC
• U & E’s, LFTs, Mg2+, Ca2+, creatinine, urate, creatinine clearance
• LDH, AFP, HCG
• ECG, lung function (inc. DLCO), CXR, Audiometry
• Staging investigations as per protocol
Prior to each cycle (and Day 8 & 15 Bleomycin):

• FBC
• U & E’s, LFTs, Mg2+, Ca2+, creatinine
• LDH, AFP, HCG
• CXR (Day 1 only)
Mid Treatment: Limited CT scan Day 20 after 1st cycle. See at start of each cycle
Post Treatment: Review in Medical Oncology Clinic 4 weeks after last cycle
Reference: Williams et al, 1987. N. Engl. J. Med., 316; pages 1435-1440
3rd Edition 62
Protocol: BEP 5-day (Bleomycin/Etoposide/Cisplatin)
Indications: Germ cell tumours
Schedule:
Etoposide 100mg/m2 1L N. Saline/1hr Days 1-5
Cisplatin 20mg/m2 1L N. Saline/4hrs Days 1-5
Bleomycin 30,000iu 200mls N. Saline/30min Days 2, 8 & 15
Cycle frequency: Every three weeks Total number of cycles: 3 or 4

• Anti-emetic group - High
• No Bleomycin with 4th cycle
• Pre and post-hydration and mannitol
• Do not cap BSA

Investigations
Pre-treatment:
• FBC
• LDH, AFP, HCG
Prior to each cycle (and Day 8 & 15 Bleomycin):

• FBC
• LDH, AFP, HCG
Mid Treatment: Limited CT scan Day 20 after 1st cycle. See at start of each cycle
Reference: Nichols et al, 1998. J. Clin. Oncol., 16; pages 1287-1293
3rd Edition 63
Protocol: Carboplatin
Indications: Seminoma – stage 1 adjuvant
Schedule:
Carboplatin AUC 7 500mls 5% dex/1hr Day 1
Cycle frequency: Once Total number of cycles: 1

• Anti-emetic group - Moderately high
• Carboplatin dose by EDTA or creatinine clearance. If calculated using formula
then AUC 7 plus 10%

vomiting
Symptomatic treatment of side effects: Mouth care
Investigations
Pre-treatment:
• FBC
• U & E’s, LFTs, creatinine, urate, creatinine clearance
• LDH, HCG and AFP
• ECG
Post Treatment: Review in Medical Oncology Clinic 2 weeks after treatment
Reference: Oliver et al, 2005, Lancet, 366; pages 267-268
3rd Edition 64
Protocol: VIP (Vinblastine/Ifosfamide/Cisplatin)
Indications: Germ cell tumours - Recurrent
Schedule:
Vinblastine 0.11mg/kg/day 250mls N. Saline/30min Days 1 & 2
Ifosfamide 1200mg/m2 1L N. Saline/4hrs Days 1-5
Cycle frequency: Every three weeks Total number of cycles: 4

• Etoposide (75 mg/ m2 days 1-5) instead of Vinblastine in some cases
• Mesna dose guidelines
• Do not cap BSA

vomiting, mucositis, alopecia, cardiotoxicity, peripheral neuropathy, nephrotoxicity,
ototoxicity, constipation, haemorrhagic cystitis, diarrhoea, carcinogenesis, infertility
Investigations
Pre-treatment:
• FBC
• LDH, AFP, HCG
• ECG, lung function (inc. DLCO), Audiometry, CXR
Prior to each cycle:

• FBC
• LDH, AFP, HCG
• CXR
Mid Treatment: See at start of each cycle
Reference: Loehrer et al, 1998. Ann. Intern. Med., 109; pages 540-546
3rd Edition 65
Protocol: TIP (Paclitaxel/Ifosfamide/Cisplatin)
Indications: Germ cell tumours – Recurrent
Schedule:
Paclitaxel 175mg/m2 500mls 5% dex/3hrs Day 1
Ifosfamide 1000mg/m2 1L N. Saline/4hrs Days 1-5
Dose medication: Discuss with Consultant

• Pre-medication (chlorpheniramine, ranitidine, dexamethasone) prior to Paclitaxel
• Mesna 1g/m2 per 24 hours
• MgSO4 and KCI in pre-hydration, with 100mls mannitol (20%) iv bolus if urinary
output low
• Do not cap BSA

ototoxicity, constipation, haemorrhagic cystitis, diarrhoea, carcinogenesis, infertility
Investigations
Pre-treatment
• FBC
• LDH, AFP, HCG
• ECG, lung function (inc. DLCO), Audiometry, CXR

• FBC
• LDH, AFP, HCG
• CXR
Mid Treatment: See at start of each year
Post treatment: Review in Medical Oncology Clinic 4 weeks after last cycle
Reference: Mead et al, 2005. Br. J. Cancer, 25; pages 178-184
3rd Edition 66
Protocol: Modified Wetlauffer (M-BOP)
Indications: Recurrent Germ cell tumours
Schedule:
Bleomycin 15,000iu 250mls N. Saline/30 min Days 1, 8 & 15
Vincristine 2mg iv Days 1, 8 & 15
Cisplatin 50mg/m2 1L N. Saline/2hrs Days 1, 2, 8, 15 & 16
Methotrexate 25mg iv Day 8
Cycle frequency: 35 days Total number of cycles: 4

• No Bleomycin if low DLCO
• Pre and post hydration, mannitol, potassium & magnesium
• Prophylactic PPI and co-trimoxazole
• Do not cap BSA

Investigations
Pre-treatment:
• FBC
• LDH, AFP, HCG
Prior to each cycle

• FBC
• LDH, AFP, HCG
Reference: Shamash et al, 1999. Ann. Oncol., 10; pages 685-692
3rd Edition 67
Protocol: BOPq10 (Bleomycin/Vincristine/Cisplatin)
Indications: Germ cell tumours - adjuvant
Schedule:
Bleomycin 30,000iu 200mls N. Saline/30mins Day 1
Vincristine 2mg iv Day 1
Cycle frequency: 10 days Total number of cycles: 2

• Do not cap BSA

pneumonitis, pulmonary fibrosis,constipation, diarrhoea, infertility
Investigations
Pre-treatment:
• FBC
• U & E’s, LFTs, Mg2+, Ca2+, creatinine, urate, creatinine clearance,
• LDH, AFP, HCG

• FBC
• LDH, AFP, HCG
Reference: Kaye et al, 1998. J. Clin. Oncol., 16; pages 692-701
3rd Edition 68
Protocol: EP (Epirubicin/Cisplatin)
Indications: Germ Cell – Recurrent, Refractory
Schedule:
Drug Dose in/infusion/oral q
Epirubicin 45mg/m2 iv Days 1 & 2

Anti-emetic group – High
Delay if neutrophils < 1.5 x 109/L or platelets < 100 x 109/L
Ensure adequate renal function
Hickman line required
Pre & post hydration, mannitol, potassium & magnesium

diarrhoea, carcinogenesis, infertility
Investigations
Pre-treatment:
• FBC
• LDH, AFP, HCG
• ECG

• FBC
• LDH, AFP, HCG
• CXR
Reference: Bedano et al, 2005, ASCO Abstract 4526.
3rd Edition 69
Protocol: Interferon alpha
Indications: Renal Cell Carcinoma – Metastatic, Recurrent
Schedule:
Interferon α2a 5mU s/c X3/wk for 2wks
Then 10mU s/c X3/weekly
Cycle frequency: For three months Total number of cycles: 2

• Anti-emetic group - Low
• Self-administration
• Plan Bevacizumab if required
Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea, flu-

like symptoms, anorexia, lethargy, joint aches
Symptomatic treatment of side effects: Mouth care, Paracetamol, administer treatment in

evening
Investigations
Pre-treatment:
• FBC
• U & E’s, LFTs, creatinine, urate
• LDH
• ECG

• FBC
• U & E’s, LFTs, creatinine
• LDH
Mid Treatment: See monthly and re-assess after 3 months
Reference: MRC, 1999. Lancet, 353; pages 14-17
3rd Edition 70
Protocol: Cisplatin/Gemcitabine
Indications: Bladder Cancer - Advanced
Schedule:
Cisplatin 70mg/m2 1L N. Saline/2hrs Day 1
Gemcitabine 1000mg/m2 200mls N. Saline/30mins Days 1, 8 &15
Cycle frequency: Every four weeks Total number of cycles: 4

• If unable to tolerate, omit day 15 and give treatment every 3 weeks

vomiting, mucositis, alopecia, amenorrhoea, peripheral neuropathy, nephrotoxicity,
ototoxicity, diarrhoea, carcinogenesis, infertility
Investigations
Pre-treatment:
• FBC
• LDH
• ECG
• CXR

• FBC
• LDH
• CXR
Mid Treatment: After every two cycles
Reference: van der Maase et al, 2000. J. Clin. Oncol., 18; pages 3068-3077
3rd Edition 71
Protocol: CMV (Cisplatin/Methotrexate/Vinblastine)
Indications: Bladder – Advanced, Recurrent
Schedule:
Methotrexate 30mg/m2 iv Days 1 & 8
Vinblastine 4mg/m2 iv Days 1 & 8

• Cisplatin to start 12 hours after methotrexate

Investigations
Pre-treatment:
• FBC
• LDH
• ECG

• FBC
• LDH
Reference: Harker et al, 1985. J. Clin. Oncol., 11; pages 1463-1470
3rd Edition 72
Protocol: MOPq10 (Methotrexate/Vincristine/Cisplatin)
Indications: Bladder – Advanced, Recurrent
Schedule:
Methotrexate 60mg/m2 iv Day 1
Vincristine 2mg iv Day 1
Cycle frequency: Every 10 days Total number of cycles: 4

• Cisplatin to start 12 hours after methotrexate
• Calcium Folinate rescue (15mg qds x 4 doses) for all patients with
hydronephrosis

Investigations
Pre-treatment:
• FBC
• LDH
• ECG

• FBC
• LDH
Mid Treatment: After each cycle
Post Treatment: Review in Medical Oncology Clinic 4 weeks after last cycle.
Reference: Boshoff et al, 1995. Eur. J. Cancer, 31A; pages 1633-1636
3rd Edition 73
Protocol: MP (Mitozantrone/Prednisolone)
Indications: Prostate Cancer – Recurrent, Metastatic, Hormone refractory
Schedule:
Mitozantrone 12mg/m2 100mls N. Saline/10mins Day 1
Prednisolone 10mg od oral Daily

• Anti-emetic group - Moderate
Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea,

mucositis, steroid side effects, discoloured urine, liver function tests, diarrhoea
Investigations
Pre-treatment:
• FBC
• LDH
• ECG

• FBC
• LDH
Reference: Tannock et al, 1996. J. Clin. Oncol., 14; pages 1756-1764
3rd Edition 74
Protocol: Docetaxel/Prednisolone
Indications: Prostate Cancer – hormone refractory
Schedule:
Docetaxel 75mg/m2 250mls N. Saline/1hr Day 1
Prednisolone 5mg bd oral Days 1-21
Cycle frequency: Every three weeks Total number of cycles: up to 10

• Anti-emetic group – Low
• Pre-medication dexamethasone 8 mg (oral or iv) at 12 hours, 3 hours and I hour
before docetaxel infusion

vomiting, mucositis, alopecia, peripheral neuropathy, fluid retention, hypersensitivity
reaction, skin rash, and side-effects of steroids.
Investigations
Pre-treatment:
• Performance score, weight, CXR
• FBC
• LDH, PSA
• ECG

• FBC
• LDH, PSA
Mid Treatment: Re-assess after 2 cycles
Reference: Tannock et al, 2004. N. Engl. J. Med., 351; pages 1502-1512
3rd Edition 75

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Department of Medical Oncology Chemotherapy Protocols

Protocol: BEP 3-day (Bleomycin/Etoposide/Cisplatin)

Indications: Germ cell tumours

Cycle frequency: Every three weeks Total number of cycles: 3 or 4

Dose modifications: Discuss with Consultant

Administration and safety:

Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea &

Symptomatic treatment of side effects: Mouth care, encourage oral fluids

Prior to each cycle (and Day 8 & 15 Bleomycin):

Reference: Williams et al, 1987. N. Engl. J. Med., 316; pages 1435-1440

Protocol: BEP 5-day (Bleomycin/Etoposide/Cisplatin)

Indications: Germ cell tumours

Cycle frequency: Every three weeks Total number of cycles: 3 or 4

Dose modifications: Discuss with Consultant

Administration and safety:

Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea &

Symptomatic treatment of side effects: Mouth care, encourage oral fluids

Prior to each cycle (and Day 8 & 15 Bleomycin):

Reference: Nichols et al, 1998. J. Clin. Oncol., 16; pages 1287-1293

Indications: Seminoma – stage 1 adjuvant

Cycle frequency: Once Total number of cycles: 1

Dose modifications: Discuss with Consultant

Administration and safety:

Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea &

Symptomatic treatment of side effects: Mouth care

Post Treatment: Review in Medical Oncology Clinic 2 weeks after treatment

Reference: Oliver et al, 2005, Lancet, 366; pages 267-268

Protocol: VIP (Vinblastine/Ifosfamide/Cisplatin)

Indications: Germ cell tumours - Recurrent

Cycle frequency: Every three weeks Total number of cycles: 4

Dose modifications: Discuss with Consultant

Administration and safety:

Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea &

Symptomatic treatment of side effects: Mouth care, encourage oral fluids

Prior to each cycle:

Mid Treatment: See at start of each cycle

Protocol: TIP (Paclitaxel/Ifosfamide/Cisplatin)

Indications: Germ cell tumours – Recurrent

Cycle frequency: Every three weeks Total number of cycles: 4

Dose medication: Discuss with Consultant

Administration and safety:

Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea &

Symptomatic treatment of side effects: Mouth care, encourage oral fluids

Prior to each cycle:

Mid Treatment: See at start of each year

Reference: Mead et al, 2005. Br. J. Cancer, 25; pages 178-184

Protocol: Modified Wetlauffer (M-BOP)

Indications: Recurrent Germ cell tumours

Cycle frequency: 35 days Total number of cycles: 4

Dose modifications: Discuss with Consultant

Administration and safety:

Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea &

Symptomatic treatment of side effects: Mouth care, encourage oral fluids

Prior to each cycle

Reference: Shamash et al, 1999. Ann. Oncol., 10; pages 685-692

Protocol: BOPq10 (Bleomycin/Vincristine/Cisplatin)

Indications: Germ cell tumours - adjuvant

Cycle frequency: 10 days Total number of cycles: 2

Dose modifications: Discuss with Consultant

Administration and safety:

Toxicities: Myelosuppression and risk of neutropenic sepsis or haemorrhage, nausea &

Symptomatic treatment of side effects: Mouth care, encourage oral fluids

Prior to each cycle: