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Gastrointestinal Toxicity Of Chemotherapy

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Mediated through the Chemoreceptor trigger zone. ... Methotrexate, Fluorouracile,Actinomycin-D, Doxorubicin, Bleomycin, Vinblastin ... – PowerPoint PPT presentation

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Title: Gastrointestinal Toxicity Of Chemotherapy


1
Gastrointestinal ToxicityOfChemotherapy
2
  • Chemotherapeutic agents have narrow therapeutic
    index and do not discriminate between normal and
    target cells???
  • Bone Marrow, spermatogonia, GI cells

3
Nausea and Vomiting
  • Most common toxicity
  • Mediated through the Chemoreceptor trigger zone.
  • Occurs 3-6 hours post administration and subsides
    after 36-48 hours.
  • Most common agents Cisplatinum,
    DTIC,Cyclophosphamide, VP-16, BCNU.

4
  • Emetogenic injury to the gastric mucosa
  • and the gastroesophageal junction (Mallory-Weiss
    tear) commonly occur and produce upper
    gastrointestinal bleeding.
  • These injuries can produce very significant
    bleeding in the setting of thrombocytopenia.

5
Treatment
  • Metoclopromide( High dose)
  • Dexamethasone
  • Serotonin antagonist

6
Mucositis
  • Methotrexate, Fluorouracile,Actinomycin-D,
    Doxorubicin, Bleomycin, Vinblastin
  • Enhanced with Radiation
  • Prevented with Leucovorin if MTX is used

7
  • Preclude oral intake ? Malnutrition
  • Pain
  • Infection

8
  • When esophagitis is suspected,endoscopy is the
    preferred diagnostic procedure and allows the
    early administration of appropriate therapy.
  • In addition to visual inspection,endoscopic
    brushings and biopsies can be obtained for
    microscopic examination, special stains, and
    culture.
  • Double-contrast esophagography will reveal
    evidence of esophagitis in severe cases, but
    sensitivity and specificity are limited.

9
Treatment
  • Conservative and symptomatic
  • Warm saline mouth wash
  • Topical anesthetics before ingestion
  • Nystatin
  • Fluid intake with straw and IV nutritional support

10
Pseudomenbranous Colitis
  • Clostridium difficile is the most common
    bacterial cause of infectious diarrhea in
    antibiotic-treated patients and in those
    undergoing cancer chemotherapy.

11
TYPHLITIS
  • Typhlitis refers to a clinical syndrome of fever
    and right-lowerquadrant tenderness in a
    neutropenic patient after cytotoxic chemotherapy.
  • Typhlitis (from the Greek word typhlon, meaning
    cecum)
  • Typhlitis appears to be more common among
    children than adults.

12
CHEMOTHERAPY-RELATED ILEUS
  • Vincristine treatment is associated with adynamic
    ileus and has been implicated in some cases of
    cecal perforation.
  • Although the etiology of vincristine-induced
    ileus is not known, improvement has been reported
    with the use of metoclopramide.

13
  • Cisapride may also be beneficial in that this
    agent improves motility throughout the intestinal
    tract whereas metachlopramides effect is limited
    to the upper gastrointestinal

14
DIARRHEA
  • Mucosal damage by cytotoxic agents produces net
    fluid secretion by the intestine and damage to
    intestinal villi with a loss of absorptive
    capacity.
  • 5-fluorouracil (5-FU),cisplatin,and irinotecan.

15
5FU
  • The toxic effects of 5-FU have been
  • shown to depend upon age and sex, being more
    common in women than men and worse in women over
    age 70.

16
CPT-11
  • A hyperacute diarrhea with abdominal cramping
    appears to be mediated by a cholingeric effect
    and can be effectively treated with atropine as
    well as loperamide.
  • The delayed (more than 24 hours post infusion)
    type of diarrhea induced by this agent correlates
    with the peak plasma concentration of the
    metabolite 7-ethyl-10-hydroxycamptothecin
    (SN-38).

17
  • Irinotecan induced diarrhea can be severe, and
    more than 18 of patients treated with this agent
    require hospitalization
  • Early and aggressive antidiarrheal therapy with
    loperamide and/or diphenoxylate can significantly
    reduce the proportion of patients developing
    uncontrolled diarrhea and its complications of
    dehydration and electrolyte imbalance.

18
ACUTE PANCREATITIS
  • Acute pancreatitis may occur secondary to
    medications
  • such as metronidazole, cortiosteroids, and
    furosemide.
  • During the course of chemotherapy, pancreatitis
    has been reported with azathioprine,ifosfamide,pre
    dnisone,L-asparaginase,cytosine ,arabinoside, and
    various regimens of combination chemotherapy
    including Vinca alkaloids, methotrexate,
    mitomycin C, 5-FU,
  • cyclophosphamide, cisplatin, and bleomycin
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