Title: Cancer and the Immune System
1Cancer and theImmune System
- Amar Bhatt
- Shirley Masand
- Jaime Warmkessel
Immunology Chapter 22 April 22, 2003
2A Look Ahead
- Tumors and Metastasis
- Oncogenes and Cancer Induction
- Tumor Antigens
- Tumors and the Immune Response
- Immunotherapy
3FATAL SYSTEM ERROR
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4Cancer and theImmune System
5Cancer
- altered self-cells that have escaped normal
growth regulation mechanisms - neoplasm tumor
- benign vs. malignant
- metastasis spreading of cancerous cells via
blood or lymph to various tissues
6Metastasis
22.1
7Types of Cancers
- carcinoma endodermal/ectodermal tissue
- leukemia/lymphoma hematopoeitic stem cells
- sarcoma mesodermal connective tissues
8What makes cancer cancer?
- decreased requirements for growth factors and
serum - are no longer anchorage dependent
- grow independently of density
- normal cells
- eventually enter Go
- confluent monolayer CHECKPOINT FAILURE
- contact inhibition
9Malignant Transformation
- are like in vitro cancers
- two phases
- initiation (changes in genome)
- promotion (proliferation)
10Malignant Transformation
- chemical and physical carcinogens
- virally induced transformation
- cultured tumors good models for study
- cancer cells are basically immortal
11Oncogenes
- oncogene cancer gene often found in viral
genomes - proto-oncogene cellular counterpart which can
be turned into an oncogene
12What can go right?
- induction of cellular proliferation
- inhibition of cellular proliferation, a.k.a.
tumor-suppressor genes - regulation of programmed cell death
13What can go wrong?
- chromosomal translocations
- tandem repeats HSRs
- mutations in proto-oncogenes
- viral integration
- growth factors and their receptors
14Induction of Cancer
Fig. 22.2
15Induction of Cancer
16Lets Visualize!
- http//science.education.nih.gov/supplements/nih1/
cancer/activities/activity2_animations.htm
17Tumors of the Immune System
- Lymphomas
- Solid tumors w/in lymphoid tissue (bone marrow,
lymph nodes, thymus) - Hodgkins non-Hodgkins
- http//www.lymphomainfo.net/
- Leukemias
- Proliferate as single cells
- Acute or Chronic depending on the progression of
disease - Acute- appear suddenly and progress rapidly
arise is less mature cells (ie ALL, AML) - Chronic- much less aggressive and develop slowly
mature cells (ie CLL and CML)
18Tumor Antigens
- TSTAs
- Tumor Specific Transplantation Antigen
- TATAs
- Tumor Associated Transplantation Antigen
19TSTAs
- Unique to tumor cells
- DO NOT occur on normal cells in the body
- Novel proteins created my mutation presented on
class I MHC - Can either be chemically/physically induced or
virally induced tumor antigens
20Chemically/Physically Induced
- Specific Immunologic Response that can
- Protect against later challenge by live cells
- Of the same line but not other tumor-line
- Cells.
-
- Methylcholanthrene / UV light
Fig 22.7
21Virally Induced
- Express tumor antigens shared by all tumors
induced by the same virus - Burkitts Lymphoma
- Epstein Barr
- HPV
Fig 22.9
22TATAs
- NOT unique to tumor cells
- DO occur on normal cells in the body
- So wheres the problem?
- Fetal/adult presence
- Concentration of Growth Factors and Growth Factor
Receptors
23TATAs contd
- Oncofetal Tumor Antigens (AFP CEA)
- Normally appear in fetus before immunocompetence
- Later recognized as non-self
- Oncogene Proteins
- Human Melanomas
24Virally Induced Tumors
- Virally induced tumors have the same antigens for
each tumor caused by that virus. - HPV
25Immune Response to Tumors
- Mostly a cell-mediated response
- NK Cells
- Not MHC restricted
- Fc receptor binds to antibody coated tumor cell ?
ADCC - Chedieak-Higashi syndrome
- Macrophages
- Not MHC restricted
- Elicits ADCC
- TNF-alpha
- Immune Surveillance Theory
26So, you have a tumor cell.Now what?
- You need three things
- See the cancer
- Ternary complex and costimulation by B7
- Activate lymphocytes
- Release IL-2, IFN-gamma, and TNF-alpha
- Cancer cells must be susceptible to killing
- CTL lysis, macrophages, NK cells
Info From http//www.brown.edu/Courses/Bio_160/Pr
ojects1999/cancer/imevstca.htmlIntroduction
27But if the body has all these defenses, why do so
many people still have cancer?
28Conniving Cancer.
- Bad antibodies?
- Some antibodies do not protect against tumor
growth, but also ENHANCE it. - Release of immunosuppressive cytokines
- transforming growth factor-beta (TGF-beta),
interleukin-10 (IL-10) and vascular endothelial
growth factor (VEGF) - Hide and go Seeking Antigen
- Antigens actually seem to hide in the presence
of antibody - Also, some cancer cells completely shed
themselves of the antigen
29Source Chouaib et al 1997
30Conniving Cancer cont.
- Reduction in Class I MHC Molecules
31And the final blow
- Lack of Co- Stimulatory Signal
32Can you tell me how to get...
33 ...How to get to Therapy Street?
34Cancer Immunotherapy
- Manipulation of Co-Stimulatory Signal
- Enhancement of APC Activity
- Cytokine Therapy
- Monoclonal Antibodies
- Cancer Vaccines
35Manipulation of Co-Stimulatory Signal
- Tumor immunity can be enhanced by providing the
co-stimulatory signal necessary for activation of
CTL precursors (CTL-Ps) - Fig. 22.11a
-
36Manipulation of Co-Stimulatory Signal Cont.
- Basis for Vaccine
- Prevent metastasis after surgical removal or
primary melanoma in human patients
37Enhancement of APC Activity
- GM-CSF (Granulocyte-macrophage colony-stimulating
factor) - remember CSFs are cytokines that induce the
formation of distinct hematopoietic cell lines - Fig 22.11b
38Cytokine Therapy
- Use of recombinant cytokines (singly or in
combination) to augment an immune response
against cancer - Via isolation and cloning of various cytokine
genes such as - IFN-a, ß, and ?
- Interleukin 1, 2, 4, 5, and 12
- GM-CSF and Tumor necrosis factor (TNF)
39Cytokine Therapy Cont.
- I. Interferons
- Most clinical trials involve IFN-a
- Has been shown to induce tumor regression in
- hematologic malignancies i.e.
leukemias, - lymphomas, melanomas and breast
cancer - All types of IFN increase MHC I expression
- IFN-? also has also been shown to increase
MHC - II expressionon macrophages and
increase - activity of Tc cells, macrophages, and NKs
-
40Cytokine Therapy Cont.
- Tumor Necrosis Factors
- Kills some tumor cells
- Reduces proliferation of tumor cells without
- affecting normal cells
- How?
- Hemorrhagic necrosis and regression, inhibits
- tumor induced vascularization
(angio-genesis) - by damaging vascular endothelium
-
41Cytokine Therapy Cont.
- In Vitro-Activited LAK TIL cells
- A. Lymphocytes are activated against tumor
- antigens in vitro
- Cultured with x-irradiated tumor cells
in - presence of IL-2
- Generated lymphokine activated killer
- cells (LAKs), which kill tumor cells
- without affecting normal cells
-
42In Vitro-Activated LAK and TIF cells Cont.
- B. Tumors contain lymphocytes that have
- infiltrated tumor and act in anti-tumor
- response
- via biopsy, obtained cells and
- expanded population in vitro with
- generated tumor-infiltrating lympho-
- cytes (TILs)
-
43Monoclonal Antibodies
- Anti-idiotype
- Growth Factors
- -HER2
- Immunotoxins
44 45Cancer Vaccines
46HPV
- Human Papilloma Virus
- E6
- E7
-
47From Normal to Abnormal
48For more info
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