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Tumor Immunology Lymphocyte Tumor cell Priya Weerasinghe MD. PhD. Department of Pathology and Laboratory Medicine UT Medical School - Houston Texas Tumor Immunology Objectives: To study the generation of immune responses to tumor cells Tumor Antigens / Tumor Specific Transplantation Antigens (TSTAs) Categories of Tumor Antigens Carcinogen-induced Tumors Tumor antigens encoded by oncogenes Immunologic factors that influence the incidence of cancer Effective mechanisms in tumor immunity B cell responses to tumor Cell mediated responses to tumor Limitations in effectiveness of immune responses against tumors Immunodiagnosis Tumor immunoprophylaxis Immunotherapy How does immune responses against tumor cells occur? The expression of cell surface molecules give rise to tumor antigens on the surface of the tumor cell. Experiments on mice showed that when tumor cells were injected to syngeneic (MHC restricted) mice, cells formed nodules that grew for few days and then regressed. When the identical tumor cells were reinjected –tumor cells did not grow. i.e. these mice had generated an immune response towards the tumor cells. What are tumor antigens/tumor specific transplantation antigens (TSTAs)? Immunogenic tumor antigens: Immunogenic tumor antigens, similar to a response to foreign antigens, generates stimulation of effector mechanisms Non immunogenic tumor antigens: The self antigens that show some degree of immune tolerance. Tumor antigens (cont…) Some tumor antigens consist of molecules that are unique to the tumor cell but not to the normal cell. Some tumor antigens are qualitatively not different from those found on normal cells but are over expressed on the tumor cell. Eg: 1. HER in some breast and ovarian cancers- over expression of HER-2/neu-1 oncogene 2. ras oncogene on some human prostate cancer cells These commonly expressed tumor antigens can serve as targets for immune based therapy. Eg: 1 monoclonal antibodies against HER to treat breast and ovarian cancer. Carcinogen-induced tumor antigens Carcinogens can induce mutations in normal genes that were silent. These mutations can give rise to an array of different gene products. There is very little or no cross reactivity in these tumor antigens. This lack of cross reactivity is due to the random mutations induced by the chemical or physical carcinogen. Eg: When methylcholanthrene is applied repeatedly to genetically identical animals, tumors will develop. But tumor antigens will be different and there will be no cross reactivity. Same is true for physical carcinogens such as UV light or x ray. Categories of tumor antigens Category Normal cellular gene products Embryo nic Type of Antigen Name of Antigen Types of Cancer Oncofetal antigens MAGE-1 MAGE-2 CEA Several Several Lung, pancreas, breast, colon, stomach Liver, melanoma, carcinoma of bladder, lung, testis AFP Differe ntiation Normal intracellular enzymes Oncoprotein Carbohydrate Prostate specific antigen, CT antigen tyrosinase HER-2/neu Lewis Prostate Melanoma Breast, ovary Lymphoma Clonal amplifi cation Ig isotype Specific antibody of B cell clone Lymphoma Mutant cellular gene products Point mutatio ns Oncogene product Suppressor gene product CDK Mutant RAS protein Mutant P53 Several Viral gene products Transfo rming viral gene Nuclear protein E6 and E7 proteins of HPV Mutant CDK-4 Several Melanoma Cervical Activation of cellular proto-oncogenes in human cancer Proto-oncogene Activation mechanism Chromosomal change Associated cancer C-myc Genetic rearrangement Translocation: 814. 8-2 or 8-22 Burkitt’s lymphoma C-abl Genetic rearrangement Translocation 922 CML C-H-ras Point mutation Bladder carcinoma C-K-ras Point mutation Lung and colon carcinoma N-myc Gene amplification Neuroblastoma Immuno surveillance Immunologic resistance against the development of cancer or the ability of innate and adoptive immuno-responses that seek and destroy tumor cells. -Experimental studies of immunocompromised animals -Epidemiological studies of patients with various immunodeficiencies (primary, secondary or acquired) Immunologic resistance against the development of cancer APC T helper cell CD4 CD3 T helper cell CD4 1) The cells (CD4+) must recognize antigen presented by MHC class II molecules on an APC (antigen presenting cell) (dendritic cell or macrophage). Activated Th1 cell secretes IL-2 and IFN-, which activates CTLs. CD3 IFN‐ IL‐2 CD8 2) CD3 Tumor cell Activated CTL Activation of CTL + NK cells + macrophages Effector mechanisms in tumor immunity Dr. Andrejs Liepins/ Science Photo Library “Kiss of Death” Effector cells in tumor immunity CTLs – antigen specific and MHC restricted. CTLs express CD8. CTLs kill their targets by using Perforin, Granzymes, Cytokines (TNF-β, IFN-) Fas and Fas ligand. NK cells are morphologically large granular lymphocytes (LGLs). Non-T and non-B lymphocytes lack surface CD3, CD4, CD8 and CD19. They do not express immunoglobulins or TCRs. NK cells express CD16 and CD56. NK cells kill by releasing perforin, granzymes and cytokines (IFN- and TNF). Reaction- nonspecific (they do not use a T cell receptor). Lymphokine activated killer cells (LAK cells) are morphologically LGLs. Non-T non-B lymphocytes. Reaction– nonspecific. NK-ADCC- NK cells are the major cell type that carries out antibody-dependent cellular cytoxicity (ADCC). NK cells have Fc receptors (CD16) that recognize Fc portion of IgG. Effector mechanisms in tumor immunity Effector Mechanism Comment B cells and antibodies (ADCC, CDC) Role in immunity– poorly understood T cells (cytolysis, apoptosis) Virally- and chemically–induced tumors NK cells (cytolysis, apoptosis, ADCC) Tumor cells not expressing MHC class 1 alleles- rejected by NK cells LAK cells (cytolysis, apoptosis) Anti tumor response- to adoptive transfer to LAK cells Macrophages and neutrophils Activated– by using bacterial products Cytokines (apoptosis, recruitment of inflammatory cells) Using adoptively transferred tumor cells- eg: GM-CSF Limitations of effectiveness of immune responses against tumors Tumor Related Mechanisms of Escape Host Related Mechanisms of Escape Failure of tumor to provide a suitable antigenic target or an effective immune response; - lack of tumor antigen - lack of MHC class 1 -deficient antigen processing -antigen modulation -antigenic masking of tumor -resistance of tumor to tumoricidal pathways -lack of co-stimulatory signals -production of inhibitory cytokines -shedding of tumor antigens Failure of host to antigenic tumor cells: -immuno-supression or immunodeficiency -deficiency in inducing apoptosis and cell death signaling - infections or old age - deficiency in tumor antigen presentation by host APC - failure of host effector cells to reach the tumor (eg: stromal barrier) - failure of host to kill variant tumor cells - T reg hindrance to tumor immunity Immuno-diagnosis 1. Immunohistochemistry- Antibodies to specific antigens detected by amplified signals. Applications: Diagnosis on surgical specimens. to identify the original cancer to classify the type of cancer to predict the aggressiveness of the tumor 2. Morphoproteomics- -Combination of disciplines of histopathology, molecular biological and computational biology. -Customizing therapy for individual patients. Tumor immuno-prophylaxis Cervical cancer vaccine: -Gardasil (by Merck Pharmaceuticals) – Prevents human papilloma virus (HPV )16, 18, 6, 11. -Cervarix: (by GlaxoSmithKline) Prevents HPV 16 and 18 Tumor immuno-therapy -Stimulate the immune system, reject and destroy tumors. -BCG immunotherapy for early stage bladder cancer. -Imiquimod: topical immunotherapy Immuno-therapy Name Trade name Used to treat Target Year approved Rituximab Rituxan Non‐Hodgkin’s lymphoma CD20 1997 Trastuzumab Herceptin Breast cancer Erb b2 1998 Gemtuzumab ozogamicin Mylotarg Acute myelogenous leukemia (AML) CD33 2000 Alemtuzumab Campath Chronic lymphocytic leukemia CD52 (CLL) 2001 Ibritumomab tiuxetan Zevalin Non‐Hodgkin’s lymphoma CD20 2002 Panitumumab Vectibix Colorectal cancer EGFR 2006 Cetuximab Erbitux Colorectal cancer, Head and neck cancers EGFR 2004 Bevacizumab Avastin Colorectal cancer VEGF 2004 USMLE Questions 1. In antigen recognition by cytolytic T lymphocytes (CTLs), T cell receptor recognizes antigen bound to a. class I antigens b. Class 11 antigens c. Class 111 antigens d. C3b e. Fc 2. The most important factor related to the prognosis of breast cancer is a. The presence of activated oncogenes b. The histological type and grade c. The size of the tumor d. The status of axillary lymph nodes e. The presence of estrogen receptors 3. Oncogene activation has been implicated in the development of all these malignancies EXCEPT a. Carcinoma of the urinary bladder b. Neuroblastoma c. Chronic myelocytic leukemia d. Burkitt’s lymphoma e. Retinoblastoma