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Basic Concepts of Cancer

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... (p53 is #1 example) ... so need 2 hits Chemical damage to DNA Epigenetic modifications, base substitutions Aromatic hydrocarbons, aromatic amines Insecticides, ... – PowerPoint PPT presentation

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Title: Basic Concepts of Cancer


1
Basic Concepts of Cancer
2
Neoplasia
  • Disease of cell growth, division, and
    differentiation
  • Benign tumors
  • Localized, clear margins (encapsulated),
    non-invasive, slow growing, well differentiated
  • Functional adenomas if glandular tissue

3
Malignant neoplasms
  • Rapid growth, no clear margins (invasive)
  • Aneuploidy, uncontrolled cellular multiplication,
    lytic enzymes
  • Decreased cell adhesion, increased motility
    (metastatic)
  • Angiogenesis---abnormal vessels

4
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5
Classifications of malignancies
  • Carcinoma--epithelial
  • SarcomaCT or muscle
  • Glioma--glial cells
  • Neuroblastoma--neurons
  • Lymphoma
  • Leukemia

6
Cancer is a genetic disorder, but it is rarely
inherited
  • Epigenetic modifications
  • p53 proteinguardian of the genome
  • Errors in p53 show up in 50 of all cancers
  • Different mutations seem to prevail in different
    cancers
  • Telomeraseprevents normal shortening of
    telomeres at end of chromosomes
  • Absent in most somatic cells, present in 85 of
    cancers
  • Allows for infinite number of divisions

7
Multi-step Model for Cause of Cancer
  • One cell suffers multiple genetic mutations,
  • Proto-oncogenes induce cell proliferation and
    growth (normal function)
  • Defined by what happens when turned on
  • Tumor suppressor genes suppress cell growth
  • Defined by what happens when turned off
  • P53--guardian of genome, halts faulty cycle

8
Initiation--promotion--progression theory
  • Initiation is first insult or series of insults
    to genome

9
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10
Types of Initiation Steps
11
Changes in proto-oncogenes? oncogenes
  • Point mutationsalways dominant (ras gene,
    telomerase gene)
  • Gene amplification
  • Chromosomal rearrangement
  • Viral insertion and activation
  • human papillomavirus, hepatitis B and C, Epstein
    Barr (?)

12
Changes in tumor suppressor genes (p53 is 1
example)
  • Removes controls on cell cycle
  • Removes review/editing of DNA copying mistakes
  • Typically recessive mutations, so need 2 hits

13
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14
Chemical damage to DNA
  • Epigenetic modifications, base substitutions
  • Aromatic hydrocarbons, aromatic amines
  • Insecticides, asbestos
  • Anti-neoplastic drugs
  • Aflatoxins
  • Nitrosamines and nitrosamides in food, water

15
Physical damage to DNA
  • Breaks, deletions, translocations
  • Sunlight (ultraviolet)
  • Radiation--therapy or diagnostic use

16
Predisposing factors
  • Age, sex, heredity
  • 15-20 of all cancers are caused by
    infection(usually viruses)
  • Exposure to DNA damaging compounds
  • Precancerous lesions
  • Colon polyps
  • Metaplastic cells

17
Promotion Proliferation
  • Intracellular antioxidant enzymes should repair
    damaged DNA
  • Apoptosis should remove damaged cells
  • Cancers become more malignant with each
    generation of transformed cells

18
  • Immune surveillance by cytotoxic T cells should
    remove transformed cells
  • Tumor associated antigens presented by MHC 1
    molecules
  • Decrease in thymus activity with age means more
    cancers in older individuals

19
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20
Progression--becoming malignant
  • Rate of growth depends on cell cycle time and
    rate of angiogenesis
  • Epithelial cancers usually grow faster
  • To metastasize, must separate from original
    cluster of cells and invade blood or lymph vessel
  • Must penetrate basement membrane
  • Metastasis is NOT inevitable once penetrate
    vessels
  • First downstream capillary bed and lymph node are
    most vulnerable

21
Clinical Manifestations of Cancer
  • Fatigue is the 1 complaint
  • Starts early, for unknown reasons
  • May last months after tumor is gone
  • Causes most severe decrease in quality of life
  • Painmay not arise until late stages
  • caused by compression local tissue, inflammation,
    or nerve injury (therapy)

22
Cachexia
  • Malnutrition from metabolic demands of tumor,
    release of cachectin (TNF)
  • anorexia, weight loss
  • weakness, anemia

23
Additional problems
  • 60-80 of late stage cancer patients will
    experience clinical depression
  • Lack of sleep
  • Fear

24
Alterations in carbohydrate metabolism
  • Tumors metabolize glucose anaerobically
  • Patient must convert lactate back to pyruvate for
    use
  • Higher than normal insulin suggests post receptor
    abnormalities
  • Metabolic changes persist after tumor removal
  • TNF will increase insulin resistance in body

25
Alterations in protein metabolism
  • Patient loses muscle mass
  • Resembles situation in burn/sepsis/hyperthyroid
    patients
  • Protein metabolism shifts to support tumor
  • Acute phase protein response--liver makes
    proteins for tumor, not the body
  • Associated with poor prognosis
  • Alterations in amino acid levels that persist
    after tumor removal

26
Alterations in fat metabolism
  • Decrease in fat synthesis, increase in lipolysis
  • Lipid mobilizing factor found in urine
  • Increases cAMP levels, acts like lipolytic
    enzymes
  • TNF-alpha stimulates lipolysis
  • High levels of ?-3 fatty acids may have benefit

27
Other complications
  • Increased risk of infection due to leukopenia,
    therapy
  • Anemia
  • Bleeding disordersthrombocytopenia, vascular
    invasion, therapy
  • Malnutrition from GI dysfunction

28
Prognosis
  • Tumor Grading Systembased on microscopic exam of
    cells by pathologist
  • I Well differentiated
  • II Moderately well differentiated
  • III Poorly differentiated
  • IV Undifferentiated

29
Prognosis
  • Staging the tumor
  • Stages 1-4
  • Depends on number of sites, involvement of lymph
    nodes
  • Automatically get Stage 3 if tumor and/or mets
    cross the midline or the diaphragm

30
Prognosis
  • TNM Classification System
  • Tumor 1-4 (based on size)
  • Txcannot be assessed
  • Tiscarcinoma in situ
  • Nodes 0-3
  • Metastasis 0-1
  • Etiology of cancervarious cancers have specific
    progressions
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