This document discusses cancer immunotherapy. It begins by describing tumor antigens that can be recognized by the immune system, such as tumor-specific antigens, tumor-associated antigens, and antigens from oncogenic viruses. It then discusses how tumors evade the immune system and various approaches to immunotherapy, including active immunotherapies using vaccines made of tumor cells, purified antigens, or antigen-loaded dendritic cells. Passive immunotherapies discussed include adoptive cellular therapy, monoclonal antibodies, and immunotoxins. Clinical trials and effectiveness of different immunotherapies are also summarized.

1. CANCER
IMMUNOTHERAPY
BY
NEHA P PATEL
M.Sc PART I SEM II

4. Expermental evidence:-Methylcholantrene(MCA)-
induced tumors

5. 5
Evasion Of Immune System

6. 1.TUMOR SPECIFIC
ANTIENS -tyrosinase
2.TUMOR ASSOCIATED
ANTIGENS-p53

7. TYPE OF ANTIGENS EXAMPLES OF HUMAN TUMOR
ANTIGENS
1 . PRODUCTS OF
ONCOGENES ,
TUMOR SUPPRESSOR
GENES
ONCOGENES- RAS MUTATION,
- p210 PRODUCT OF Bcr/Abl
REARRANGEMENTS,
- OVEREXPRESSED Her-2/neu
TSG- -MUTATED p53
2 .MUTANTS OF
CELLULAR
GENES NOT INVOLVED
IN TUMORIGENESIS
-P19 A MUTATION IN MUTAGENIZED MURINE
MASTOCYTOMA
3.PRODUCTS OF GENES
THAT ARE SILENT IN MOST
NORMAL TISSUES.
MAGE,BAGE,GAGE PROTEINS EXPRESSED IN
MELANOMAS AND MANY CARCINOMAS
4.PRODUCTS OF
OVEREXPRESSED
GENES
TYROSINASE,
gp100,
MART IN MELANOMAS

8. TYPE OF ANTIGENS EXAMPLES OF HUMAN TUMOR
ANTIGENS
5.PRODUCTS OF
ONCOGENIC VIRUSES
-PAPILLOMAVIRUS E6 AND E7 PROTEINS (CERVICAL
CARCINOMAS)
-EBNA-1 PROTEIN OF EBV
-SV40 (SV40-INDUCED RODENTS TUMORS)
-HTLV-1
6.ONCOFETAL ANTIGENS -CEA ON MANY TUMORS
-ALPHA-FETOPROTEIN.(AFP)
7.GLYCOLIPIDS
&GLYCOPROTEINS
GM-2,GD-2 ON MELANOMAS
CA-125 & CA-19-9,ovarian cancer
MUC-1-breast cancer
8.DIFFERENTIATION
ANTIGENS NORMALLY
PRESENT IN TISSUE OF
ORIGEN
-PROSTATE SPECIFIC ANTIGEN
-MARKERS OF LYMPHOCYTES: CD-10,CD -20
Ig IDIOTYPES ON B-CELLS

9. Immune Response To Tumours

10. INDUCTION OF T-CELL RESPONSE TO TUMOR CELLS

11. [2] ANTIBODIES
TUMOR BEARING HOST MAY PRODUCE Abs AGAINST VARIOUS TUMOR Ags .
eg:-EBV ASSOCIATED LYMPHOMAS HAVE SERUM Abs AGAINST EBV –
ENCODED Ag EXPRESSED ON THE SURFACE OF THE LYMPHOMA CELLS
Abs MAY ACTIVATE COMPLEMENT SYSTEM OR KILL TUMOR CELLS BY ADCC

12.  Chediak-Higashi syndrome  NK cell impairment  increased
incidence of certain types of tumour
NK cells release TNF- + NK cytotxic factor
Mechanism-ADCC-Fcγ III
Activity increased by IL-2 & IL-12,INF’s
 capable of lysing a wide variety of tumour cells”.
Respond to low level of MHC I
[3] NK CELLS

14. Activated macrophages secrete lytic enzymes
Also secrete TNF-  tumour necrosis
Secrete nitric oxide (potential antitumour effects)
[4] Macrophages-activated by IFN-γ

17. Tumour cell present
Broken up to
release antigens
APC
APC recruits T cells
able to recognise
tumour antigens
T
T
Th
CTL
CTL recognise
and destroy other
tumour cells
CTL
Th cells educate
other T/B cells
B
Ab / ADCC /
cytokine attack

20. S.No Type of tumor vaccine Vaccine
preparation
Animal
models
Clinical trials
1. Killed tumor vaccine •Killed tumor
cells +
adjuvants
•Tumor cell
lysate+
adjuvants
•Melanoma
,colon
cancer
•sarcoma
•Melanoma,
colon
cancer
•Melanoma
2. Purified tumor antigens •Melanoma
antigen
•HSP
•Melanoma
•various
•Melanoma
•Melanomas
,renal cancer,
sarcoma
3. Professional APC
based
Dendritic cells
+ tumor
antigen
Melanoma ,
B-cell,
lymphoma
sarcoma
Melanoma ,
prostate
cancer,&
others

21. S.No
.
Type of vaccine Vaaccine
preparation
Animal model Clinical trials
4. Cytokine & co-
stimulator
enhanced
vaccines
•Tumor cells
transfected with
cytokine or B-7 genes
•APCs transfected
with cytokine +tumor
antigens
•Renal cancer,
sarcoma,B-cell
leukemia,
lung cancer
Melanoma
Sarcoma
& others
Melanoma,
renal cancer
& others
5. DNA vaccine Immunoglobulin with
plasmid encoding
tumor antigens
Melanoma Melanoma
6. Viral vector •Adenovirus vaccine
•Virus encoding
tumor antigens
+ cytokines
•Melanoma
•sarcoma
•Melanoma
• Melanoma

23. IMMUNOTHERAPY WITH GENE TRANSFECTED TUMOR CELLS
S.No. Cytokine Tumor
rejection
in animals
Inflammatory
infiltrate
Immunity
against
parental tumor
(animal model)
Clinical
trials
1. IL-2 YES;
mediated
by T- cell
Lymphocytes
neutrophils
In some cases
of renal
cancer,
melanoma
Renal
cancer,
melanoma
2. Il-4 yes Eosinophil ,
macrophages
No long lasting
immunity in
human trials
Melanoma
Renal
cancer
3. INF-γ Variable Macrophages,
Other cells
sometimes
4. TNF variable Neutrophils &
lymphocytes
No
5. GM-CSF yes Macrophages,
Other cells
Yes(long lived
T-cell immunity)
Renal
cancer
6. Il-2 sometimes Macrophages,
Other cells
Sometimes

24. S.No CYTOKINE TUMOR
REJECTION IN
ANIMALS
CLINICAL TRIALS TOXICITY
1. IL-2 YES Melanoma,renal cancer
,colon cancer,limited
success
Vascular
leak,shock,
pulmonary
edema
2. TNF Only with
local
administratio
n
Sarcoma,melanoma Septic syndrome
3. Il-12 YES, Variable Toxicity trials (phase I) in
melanoma,others
Abnormal liver
fuction
4. IL-6 Melanoma Renal cancer Fever ,liver,&CNS
toxicity,hyperte-
sion
5. GM-CSF NO In routine use to promote
bone marrow rcovery
Bone pain
SYSTEMIC CYTOKINE THERAPY FOR TUMORS

25. ACTIVATION OF TUMOR SPECIFIC T- CELL

26. Bacterial Extracts: Non-Specific Immune
Adjuvants
 BCG: Bacillus Calmette-Guerin (Attenuated
Bovine Tuberculosis Bacterium)
 Membrane Extracts of BCG
 C Parvum: Corynebacterium parvum (related
to diphtheria bacillus)
Bacterial Endotoxins: Muramyl Dipeptide
Chemical Adjuvants:
 Levamisole
 Poly IC (Poly-inosinic-Poly-cytidyllic acid)

27. PASSIVE IMMUNOTHERAPIES:
TRANSFER OF IMMUNE EFFECTORS INTO PATIENTS
RAPID RESPONSE
NOT LONG LIVED
TYPES OF PIT-
1.ADOPTIVE CELLULAR THERAPY
2.GRAFT VERSUS LEUKEMIA EFFECTS
3.MONOCLONAL ANTIBODIES
4.IMMUNOTOXINS

28. ADOPTIVE CELLULAR THERAPY

30. • Adminstration of monoclonal antibodies which target either tumour-
specific or over-expressed antigens.
• Kill tumour cells in a variety of ways:
Apoptosis
induction
Complement-
mediated
cytotoxicity
ADCC
NKMØ
Conjugated to
toxin / isotope

32. Complete regression of a
large liver metastasis from
kidney cancer in a patient
treated with IL-2.
Regression is ongoing
seven years later
Effective therapies
Rosenberg (2001) Nature, 411;381-4

33. Name Malignancy Target
Rituxan B cell lymphoma CD20
Herceptin Breast, lymphoma Her-2/neu
Campath B-CLL CD52
Erbitux Colo-rectal EGFR
Avastin Colo-rectal VEGF
Mylotarg AML CD33
(calicheamicin)
Bexxar B cell lymphoma CD20
(131In / 90Y)

34. Effectiveness of multiple antigen vaccines
Patient with multiple metastatic melanomas
treated with tyrosinase / gp100 / MART vaccine

35. Advances in immunotherapy
chimeric molecules→immune-stimulatory cytokine +antibody →
targets the cytokine's activity to a specific environment such as
tumor →destroying the cancer-causing cells without the unwanted
side-effects
•On Wednesday 7 September 2011 Scientists in Singapore suggested
antibody-based therapies can be used to target proteins inside cancer
cells.
•Mechanism of Ab entering the cell is not known. It will be the subject
of future research.
• An interesting recent variation on the idea of boosting host immune
responses against tumors is to eliminate normal inhibitory signals for
lymphocytes.
•In some animal models, blocking the inhibitory T cell receptor CTLA-4
has led to strong immune responses against transplanted tumors.