Chemotherapy Side Effects

Chemotherapy: Adverse Effects
Pyrimidine-analog antimetabolites: Flurouracil Cytarabine Gemcytabine Purine-analog antimetabolites: Fludarabine Cladribine Pentostatin 6-mercaptopurine 6-thioguanine Other Antimetabolites Methotrexate Hydroxyurea Plant Alkaloids: Vinblastine Vincristine Paclitaxel/doxetaxel	Topoisomerase inhibitors: Etoposide/teniposide doxorubicin daunorubicin idarubicin dactinomycin mitoxantrone Alkylating Agents: cyclophosphamide ifosfamide melphalan busulfan mechlorethamine chlorambucil thiotepa Nitrosoureas Platinum compounds cisplatin carboplatin Antitumor Antibiotics bleomycin mitomycin Other Drugs: dacarbazine procarbazine L-asparaginase

Pyrimidine-analog antimetabolites:
- Fluorouracil (5-FU)
  - schedule-dependent toxicity
  - bolus infusion: mainly bone marrow suppression
  - continuous infusion: GI toxicity
  - myocardial ischemic syndrome (uncommon)
  - Reversible neurological effects:
    - headaches
    - ataxia
    - somnolence
  - Dermatologic (common):
    - dermatitis
    - skin atrophy
    - hyperpigmentation
- Cytarabine (ARA-C)
  - Continuous infusion: significant myelosuppression
  - GI toxicity (including oral mucositis)
  - High-dose protocols: cholestatic jaundice; cerebral/cerebellar toxicity
  - Neurotoxicity (increased risk with age > 40; diminished renal function
  - Conjunctivitis: (preventable by ophthalmic corticosteroids)
- Gemcitabine (Gemzar):
  - Myelosuppression (dose limiting)
  - lethargy; malaise

Purine Analog antimetabolites:
- Fludarabine (Fludara)
  - Reversible, usually mild, neurotoxicity
  - myelosuppression
  - immunosuppression (opportunistic infection in some patients)
- Cladribine (Leustatin)
  - myelosuppression
  - immunosuppression
  - GI toxicity (mild)
- Pentostatin (Nipent)
  - immunosuppression
  - myelosuppression
  - renal dysfunction
  - CNS toxicity; lever toxicity
- 6-mercaptopurine (6MP)
  - Patients receiving allopurinol -- 75% reduction mercaptopurine does (elimination depends on xanthine oxidase activity, which is inhibited by allopurinol)
  - cholestatic jaundice
  - myelosuppression
  - mild gastrointestinal effects
- 6-thioguanine (6-TG):
  - cholestatic jaundice (more common with 6-mercaptopurine (
  - myelosuppression
  - gastrointestinal toxicity (mild)

Other Antimetabolites:
- Methotrexate:
  - Severe gastrointestinal toxicity}avoided by administration of leucovorin
  - Significant bone marrow hypoplasia}avoided by administration of leucovorin
  - methotrexate may cumulative in fluid spaces (pleural effusions or ascites) -- may lead to severe toxicities as the drug elimination is prolonged.
  - Very high-dose methotrexate:
    - acute renal injury (may be prevented by hydration and urine alkalinization)
    - Normal renal function is required for methotrexate elimination.
  - liver toxicity
  - idiosyncratic pneumonitis
- Hydroxyurea (Hydrea):
  - leukopenia (reversible upon discontinuation of drug)
  - mild GI toxicity
  - mild dermatologic changes with prolonged therapy

Plant Alkaloids:
- Vincristine (Oncovin):
  - Neurotoxicity -- dose limiting
    - peripheral sensory neuropathy and/or autonomic neuropathy
    - Non-myelosuppressive
- Vinblastine (Velban):
  - Dose limiting bone marrow hypoplasia (also seen with vinorelbine)
  - Significant neurotoxicity less frequently observed with vinblastine or vinorelbine than with vincristine)
- Paclitaxel (Taxol)/docetaxel (Taxotere)
  - infusion hypersensitivity (infusion vehicle may contribute)-- preventable by glucocorticoids.
  - paclitaxel:
    - Bradyarrhythmias (A-V blockade)
    - chest pain (atypical)
  - Myelosuppression: dose limiting
  - Peripheral neuropathy --common
  - Alopecia-- common

Topoisomerase inhibitors:
- Etoposide (VP-16,VePe-sid)/teniposide (Vumon)
  - Leukopenia: dose limiting
  - IV administration:
    - hypotension
    - fever
    - bronchus spasm
    - anaphylaxis
- Anthracyclines and related compounds (doxorubicin (Adriamycin), daunorubicin (DaunoXome), idarubicin (Idamycin))
  - Myelosuppression
  - GI toxicity
  - Severe vesicants (blistering, tissue necrosis at injection site)
  - Long-term administration: limited by cumulative dose-dependent myocardial toxicity
  - Irreversible cardiomyopathy: significant risk with cumulative doses > 500 milligrams/m^2
    - conference cyclophosphamide administration or radiation therapy may lower acceptable cumulative dose.
  - dactinomycin (Cosmegen):
    - Limited clinical use
    - Myelosuppression
- Anthracenedione (mitoxantrone (Novantrone))
  - Cardiotoxicity
  - significant myelosuppression

Alkylating agents:
- Depression in spermatogenesis
- Depression in oogenesis
- mutagenic
- carcinogenic
- secondary leukemias
  - Patients receiving alkylating agents for treatment of Hodgkin's or non-Hodgkin's lymphoma:
    - 2% incidence of secondary myeloid leukemia (further increased incidence by addition of radiation therapy)
    - not all alkylating agents equally leukemogenic
      - Melphalan: higher incidence compared to cyclophosphamide (in treating ovarian carcinoma)
  - Most common dose limiting toxicity: myelosuppression
- Cyclophosphamide (Cytoxan):
  - Hemorrhagic cystitis (acrolein metabolite)
    - prevented by adequate hydration and through the use of the bladder protectant, mesna
  - chronic bladder inflammation
  - antidiuretic effect (action on distal tubule)
  - immunosuppression (myelosuppressive)
  - acute myocardial necrosis (rare)
- Ifosfamide (Ifex):
  - More urotoxic then cyclophosphamide (Cytoxan) (commonly administered with mesna)
  - Less myelosuppressive than cyclophosphamide
  - Neurotoxicity: reversible change in mental status.
- Melphalan (Alkeran):
  - Especially leukemogenic
  - pulmonary fibrosis (rare)
- Busulfan (Myleran)
  - Myeloid stem cell toxicity
  - bone marrow hypoplasia
  - interstitial pneumonitis (rare)
  - progressive pulmonary fibrosis (rare)
- Mechlorethamine (Mustargen):
  - Severe vesicant (blistering)
- Chlorambucil (Leukeran)--structurally similar to mechlorethamine, generally well tolerated
- Thiotepa -limited clinical use
- Nitrosoureas (carmustine {BCNU}; lomustine {CCNU})
  - Delayed, cumulative myelosuppression
  - Increase in hepatic enzyme levels (moderate, reversible)
  - Prolonged treatment: progressive renal insufficiency
  - Leukemogenic
- Platinum agents: Cisplatin (Platinol) and Carboplatin (Paraplatin) (not true alkylating agents, but do cause DNA cross-linking):
  - Cisplatin (Platinol): Renal toxicity {toxic to proximal and distal renal tubule epithelial cells}
    - Adequate hydration and the use of high-ceiling diuretics (furosemide) or osmotic diuretics (mannitol) decrease likelihood of Nephrotoxicity
    - nausea
    - vomiting
    - sensory neuropathy
    - high-frequency hearing loss -- not uncommon
    - Mild myelosuppression
  - Carboplatin (Paraplatin):
    - less nephrotoxic then cisplatin
    - less ototoxic than cisplatin
    - less nausea and vomiting than cisplatin
    - more myelosuppressive than cisplatin

Antitumor antibiotics:
- Bleomycin (Blenoxane):
  - Pulmonary toxicity: chronic interstitial pneumonitis (most serious toxicity)
  - Test does required -- bleomycin infusion may cause hypersensitivity reactions
  - little myelosuppressive effect
- Mitomycin (Mutamycin):
  - Delayed myelosuppression
  - may produce progressive renal failure-microangiopathic anemia (hemolytic-uremic syndrome)

Other drugs:
- Dacarbazine (DTIC):
  - some myelosuppression
  - nausea/vomiting (may be severe)
- Procarbazine (Matulane):
  - Peripheral sensory neuropathy
  - Mood and mental status changes
  - nausea/vomiting (may be severe)
- L- asparaginase (El-spar):
  - hypersensitivity reactions; anaphylaxis
  - hepatotoxicity-- occasional
  - pancreatitis-- occasional
  - thromboses-- occasional

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