Cancer chemotherapy Flashcards

1
Q

3 main approaches to dealing with established cancers:

A
  • 1) Surgical excision
  • 2) Radiotherapy
  • 3) Chemotherapy
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2
Q

Four types of traditional agent

A
  • Alkylating agents
  • Anti metabolites
  • Cytotoxic antibiotics
  • Plant derivatives
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3
Q

Main drawbacks of chemotherapy of cancer

A
  • Target cell proliferation not the more lethal properties of invasiveness and metastasis
  • Non-specific cell killers rather than being aimed at the particular changes which make a cell malignant
  • The development of resistance (particularly multidrug resistance) to anticancer drugs
  • Leaves some remaining cells
  • Healthy cells which have a high rate of growth and multiplication include cells of the bone marrow, hair, GI mucosa and skin therefore side-effects often relate to these body systems
  • Severity of side effects varies between drugs – the summary of product characteristics (SPC) can be referred to on the eMC website for details on specific side-effects of each drug.
  • May be drug specific e.g. anthracyclines and cardiotoxicity; vinca alkaloids and neuropathy; high dose cisplatin and ototoxicity
  • Side effects often occur 7-14 days post treatment. These can be cumulative over many cycles
  • Patient compliance due to side-effects Not completing the therapy regimen
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4
Q

Specific side-effects: Tumour Lysis Syndrome

A
  • An acute side-effect and a metabolic emergency
  • Occurs due to rapid cell lysis (death) & large amounts of cell metabolites in blood.
  • It is characterized by hyperuricaemia, hyperphosphataemia, hyperkalaemia and hypocalcaemia
  • If untreated can lead to acute renal failure, cardiac arrest and death.
  • Risk assess patient prior to chemotherapy
  • Monitor and respond to deranged urea and electrolytes / fluid balance: dialysis may be required
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5
Q

Specific side-effect: Bone Marrow

A
  • Myelosuppression – reduced production of cells which provide immunity, oxygen transport and clotting common with many chemotherapy agents (except Vincristine and Bleomycin)
  • Only actively dividing cells in the bone marrow are affected (i.e. stem cells)
  • Monitor full blood count prior to then daily during treatment cycles
  • Occasional use of recombinant human granulocyte-colony stimulating factors (e.g. Filgrastim) recommended to reduce incidence/duration of myelosupression
  • Cells with shorter life span are more affected
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6
Q

Specific side-effect: Gastro-intestinal

A

loss of appetite

nausea and vomitting

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7
Q

Specific side-effect: Gastro-intestinal constipation

A
  • Due to reduction in gastric motility, reduced fluid intake and activity, side-effects of concurrent anti-emetics e.g. granisetron.
  • Management – add laxatives
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8
Q

Specific side-effect: Gastro-intestinal diarrhoea

A
  • can cause severe dehydration and electrolyte disturbances
  • Manage by stopping oral chemo
  • May need to give IV fluid support
  • Consider adding anti-diarrhoeal e.g. loperamide
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9
Q

Specific side-effect: Mucositis

A
  1. Ulceration, dry mouth, pain, taste alterations
    • Prevention and management:
    • Assess the oral cavity regularly
    • Encourage good oral hygiene and regular dental visits
    • Anti-bacterials and anti-virals
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10
Q

Specific side-effect: Other

A
  • Fatigue: Often multi-factorial, treat cause if known, involve physio/occupational therapists in care
  • Body image side-effects – hair loss, weight loss/gain, appearance of intervention wounds
  • Peripheral neuropathy – counsel patient about need for care if injured, consider analgesia for nerve pain
  • Altered renal function – care with drug choices, doses and frequency
  • Delayed effects: infertility, secondary malignancy
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11
Q

personalised medicine

A

– genomic/genetic testing
– proteomic profiling
– metabolomic analysis (study metabolites)

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12
Q

preventative care aims

A

i. improved prevention based on underlying predisposition;
ii. earlier diagnosis of disease as a result of identifying abnormality earlier;
iii. more precise diagnosis based on cause; and
iv. targeted interventions through the use of companion diagnostics to identify and stratify patients for effective treatments.

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13
Q

pharmacogenetics

A

the study of the way a patient’s genome affects their response to drugs

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14
Q

Testing: in pharmacogenetics

A

Germline variants in the dihydropyrimidine dehydrogenase (DPYD) gene can confer an increased risk of severe toxicity when a patient is treated with the fluoropyrimidines, capecitabine or 5-fluorouracil.

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