Cancer immunotherapy
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- Опубликовано: 2 окт 2024
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Cancer immunotherapy is the use of the immune system to reject cancer. The main premise is stimulating the patient's immune system to attack the malignant tumor cells that are responsible for the disease. This can be either through immunization of the patient (e.g., by administering a cancer vaccine, such as Dendreon's Provenge), in which case the patient's own immune system is trained to recognize tumor cells as targets to be destroyed, or through the administration of therapeutic antibodies as drugs, in which case the patient's immune system is recruited to destroy tumor cells by the therapeutic antibodies. Cell based immunotherapy is another major entity of cancer immunotherapy. This involves immune cells such as the Natural killer Cells (NK cells), Lymphokine Activated killer cell(LAK), Cytotoxic T Lymphocytes(CTLs), Dendritic Cells (DC), etc., which are either activated in vivo by administering certain cytokines such as Interleukins or they are isolated, enriched and transfused to the patient to fight against cancer.
Since the immune system responds to the environmental factors it encounters on the basis of discrimination between self and non-self, many kinds of tumor cells that arise as a result of the onset of cancer are more or less tolerated by the patient's own immune system since the tumor cells are essentially the patient's own cells that are growing, dividing and spreading without proper regulatory control.
In spite of this fact, however, many kinds of tumor cells display unusual antigens that are either inappropriate for the cell type and/or its environment, or are only normally present during the organisms' development (e.g. fetal antigens). Examples of such antigens include the glycosphingolipid GD2, a disialoganglioside that is normally only expressed at a significant level on the outer surface membranes of neuronal cells, where its exposure to the immune system is limited by the blood--brain barrier. GD2 is expressed on the surfaces of a wide range of tumor cells including neuroblastoma, medulloblastomas, astrocytomas, melanomas, small-cell lung cancer, osteosarcomas and other soft tissue sarcomas. GD2 is thus a convenient tumor-specific target for immunotherapies.
Other kinds of tumor cells display cell surface receptors that are rare or absent on the surfaces of healthy cells, and which are responsible for activating cellular signal transduction pathways that cause the unregulated growth and division of the tumor cell. Examples include ErbB2, a constitutively active cell surface receptor that is produced at abnormally high levels on the surface of breast cancer tumor cells.
The use of some agents can lead to the re-activation of latent tuberculosis (TB) and this must be assessed for before those agents are used therapeutically.[1][2]
Source: Dr. Lopamudra Roy
Please sir eski hindi vedio bna dijige please 🙏
Sir i have a question ? Which changes we can done hypothetically and animal become super immune animal and have super immune system against infection and cancer cells? Can we increase or decrease the number of cells like neutrophils macrophages or natural killer cells? Hypothetically? And can increase amount of natural killer cells which effectively work against cancers or other virus infected cells?
isn't CD28/B7 costimulation required for MHC II antigen presentation?
Yes sir, can u pls explain this question? Same doubt for me also
NO discussion on t cell genetic modification? come on! the rest of the video was simply awesome and good. good job
Very helpful and easily explanied thank you sir for simplifying such topics
Glad to hear that you're getting benefit from my lectures
Sankalp Rushi do you have notes??
Thanks for this informative post
You're welcome
Thank you so much for such a nice and clear explanation, Sir.
You're welcome
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