Title: Chapter 20 Tumor Immunology
1Chapter 20 Tumor Immunology
2Chapter 20 Tumor Immunology
Contents
- Introduction
- Part? Tumor antigens
- Part? Immune response to tumors
- Part ? Mechanism of tumor escape from
- immune surveillance
- Part? Immunotherapy of tumors
3Introduction
- Tumor immunology is mainly to study the
immunogenicity of tumor and the mechanism of
immune response to tumor, to demonstrate the
relationship between the status of immune system
and the generation, development of tumor, to
explore the method of tumor diagnosis, therapy
and prevention. - Immunosurveillance
4Part? Tumor antigens
- Tumor antigens Refer to all newly expressed
antigens or over expressed antigens during the
generation and development of the tumor.
5?.Classification of tumor antigens
- Base on their patterns of expression
- Tumor specific antigen (TSA)
- Tumor associated antigens (TAA)
61.Tumor-specific antigens (TSA)
- TSA Antigens that are only expressed on tumor
cells but not on normal cells. high specificity.
- Tumor high-specific antigens
- TSA---only expressed on one kind of tumor,
induced by physiochemical factors, such as X-ray - Tumor low-specific antigens
- TSA---expressed on more than one kind of
tumor, induced by virus
7Discovery of tumor specific transplantation
antigens, TSTA
?????????(methyl-cholanthrene,MCA)
8Conclusion from this experiment
- Tumors express antigens that are recognized as
foreign by the immune system of the tumor-bearing
host. - Immune response frequently fail to prevent the
growth of tumors. - The immune system can be activated by external
stimulator to effectively kill tumor cells and
eradicate tumors.
92.Tumor-associated antigens,TAA
- Antigens that are also expressed on normal cells,
but high expressed on tumor cells. Without tumor
specificity CEA, AFP
10?.Common human tumor antigens
- Embryonic antigens
- Tumor antigens induced by viruses
- proteins coded by Mutated oncogene or suppressor
oncogene - TATAS expressed on human melanoma cells
111. embryonic antigens
- embryonic antigens are proteins that are
express at high levels on cancer cells and in
normal developing fetal, but peter out or very
low level in adult. - Their main function is that they provide markers
that aid diagnosis of tumor. - Carcinoembryonic antigen (CEA)
- alpha-fetoprotein (AFP)
12(1) Carcinoembryonic antigen (CEA)
- High CEA level is normally restricted to cells of
the gut, pancreas, and liver in the course of 2-6
months of gestation, and low level is found in
serum of normal adult(lt5?g/ml). - CEA level of serum is increased in many
carcinomas ,such as the colon, pancreas, stomach,
and breast. - The level of serum CEA is used to monitor the
persistence or recurrence of the tumors after
treatment.
13- CEA levels in normal individuals are below 2.5
ng/ml, but it increases significantly in certain
malignancies, particularly colo-rectal cancers.
It may also rise in some nonmalignant conditions
(e.g., chronic cirrhosis, pulmonary emphysema,
heavy smoking). Levels 4-5-fold of normal have
been used to predict recurrence of colo-rectal
tumors.
14Carcinoembryonic antigenclinical use
- Adjunct in diagnosis
- Staging and prognosis
- Monitoring response to therapy
- Detection of tumor recurrence
15Carcinoembryonic antigenclinical use
16(2) alpha-fetoprotein (AFP)
- AFP is a circulating glycoprotein normally
synthesized and secreted by the yolk sac and
liver of fetal. - Serum levels of AFP is very low in serum of adult
(20ng/ml), and the concentration of AFP is up to
500ng/ml in serum of patients with
hepatocellular carcinoma. - higher rise in this protein is used for
monitoring hepatomas and testicular cancers. AFP
level may also be raised in some nonmalignant
conditions, such as cirrhosis, hepatitis and
other forms of liver damage.
17Alpha fetoprotein concentrations
- Normal concentration lt20 ng/ml
- Abnormal concentrations
- 100-350 possible hepatoma
- 350-500 probable hepatoma
- 500-100 likely hepatoma
- gt1000 HEPATOMA
18- 2. Tumor antigens induced by viruses
- HBV------ liver cancer
- HPV------ cervical carcinoma
- EBV------ B cell lymphoma and
- nasopharyngeal carcinoma
19- 3. Products of mutated genes
- Some tumor antigens are produced by mutated
genes, such as suppressor oncogenes p53 and
pro-oncogene ras
20- Some patients with cancer have circulating CD4
and CD8T cells that can respond to the products
of mutated genes such as Ras and P53. - Furthermore, in animals, immunization with
mutated Ras or P53 proteins induces CTLs and
rejection responses against tumors expressing
these mutants.
21- Overexpressed cellular proteins and
- abnormally expressed proteins
- gp100, MAGE in melanomas
- Cancer-testis antigens
22Part? Mechanism Immune Response
- T cells aßT,
?dT - NK cells
- Cellular immunity
- Macrophages
- Dendritic
cells - Humoral immunity
23?.Cell-mediated Immune Response
- T cells
- NK cells
- Macrophages(MF)
- Dendritic cells (DCs)
24- 1. T lymphocytes
- ??T cells
- The principal mechanism of tumor immunity is
killing of tumor cells by CTL - Tumor antigens
- DC cross presentation
CD4Th cells
CD8T
(CTL)
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27- (2) ??T cells
- Non-class?MHC restriction
- Its target cells are not hypersensitive to NK
cells - First line of defence of immune surveillance
28- 2. NK cells
- NK cells are broad-spectrum killer cells
- It can kill target cells with low level or non
MHC class ?molecule. - First line of defence of immune surveillance
29NK????MHCI??????
KIR2DS KIR2DL
KIR2D KIR3D
DAP12 ITAM
????????????(KIR)(MHC-G)
ITIM
KIR2DL KIR2DS
CD94/NKG2AITIM CD94/NKG2C??DAP12 -ITAM
??????????(KLR) (HLA-E-9?)
30activated
Tumor cell
31- 3. Macrophages(MF)
- ? APC
- ? release of lysosomal enzymes, reactive
- oxygen intermediates, nitric oxide
- ? ADCC
- ? secrete cytokines
- 4. Dendritic cells
- ? APC------Induce adaptive immune response
- ? Inhibit tumor growth directly
32 Antibodies ? Activating complement ? ADCC?
Opsonization
?. Humoral immune responses
33Antitumor Effector Mechanisms
CTL
NK cell
Tumor cell
Humoral Mechanisms
Macrophage
Kumar et al. Basic Pathology 6th ed. Figure 6-32
34Part? Mechanism of Tumor Immune Escape
- Factors related to tumor cells
- Factors related to the hosts
- immune system
35?. Factors related to tumor cells
- 1.low immunogenicity of tumor antigens and
antigenic modulation - (1) low immunogenicity of tumor antigens
- The failure of immunosurveillance may be the
fact that in the early development of a tumor,
the amount of antigen may be too small to
stimulate the immune system.
36Escape from immunosurveillance
Lack of Neo-antigens
37- (2) antigenic modulation is a phenomenon that
cell-surface tumor antigens are decrease or lose
because of attack of hosts humoral immune.
38- 2. covering or blocking of tumor antigens on the
surface of the tumor cells
39- 3. Diminution or absence of MHC class I molecule
- 4. Lack of co-stimulatory molecule on the surface
of tumor cells - 5. Immune inhibitors secreted by tumor cells
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41Escape from immunosurveillance
42?.Factors related to hosts immune system
- 1. Immunodeficiency
- 2. Suppressing immune function by tumor directly
or indirectly
43Parts ? immunotherapy of tumor
- Active immunotherapy
- Target immunotherapy
- Adoptive immunotherapy
- Cytokine therapy
- genetherapy
44Escape from immunosurveillance
Tumors shed their neo-antigens
45- Factors related to host
- Poor immune function
- Tumor inhibit immune function of host
46Escape from immunosurveillance
Tumors secrete Immunosuppressive molecules
47Part? Immunotherapy of tumors
- Active immunotherapy
- Target immunotherapy
- Adoptive immunotherapy
- Cytokine therapy
- Gene therapy
48- Stimulation of active host immune
- responses to tumors
- Vaccination with tumor cells and tumor antigens,
or with APC. - Augmentation of host immunity to tumors with
cytokines and costimulators - Nonspecific stimulation of the immune system
49- Vaccination with tumor cells and tumor antigens
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51- DC
- Use primed dendritic cells
- APCs can be fed tumor antigens in the laboratory
and then injected into a patient. The injected
cells are primed to activate T cells - Alternatively, DCs can be infected with a viral
vector that contains the gene for a tumor
antigen.
52Use of tumor specific/associated antigens
monoclonal antibodies
53- Adoptive immunotherapy
- Adoptive cellular immunotherapy is the
transfer of cultured immune cells that have
anti-tumor reactivity into a tumor-bearing host. - LAK, TIL, CD3AK, CTL
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55- Passive immunotherapy for tumors with
- T cells and antibodies
- Therapy with anti-tumor antibodies
- Monoclonal antibodies conjugated drugs
- Adoptive cellular therapy
- LAK,TIL,CD3AK,CTL
56- Cytokines may also be administered systemically
for the treatment of human tumors. - IL-2 works by stimulating the proliferation and
anti-tumor activity of NK cells and CTLs. - IFN-?works by increasing the cytolytic activity
of NK cells and class I MHC expression on various
cell types. - Their side effects limited this treatment.
57- Augmentation of host immunity to tumors with
cytokines and costimulators