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Example Questions
Example Question #376 : Biology
Where in the body do T-lymphocytes mature?
Thymus
Lymph nodes
Bone marrow
Thyroid
Thymus
T-lymphocytes and B-lymphocytes both arise in the bone marrow from the lymphoid progenitor lineage of stem cells. B-lymphocytes remain in the bone marrow for maturation, while T-lymphocytes migrate to the thymus. In the thymus, T-lymphocytes are exposed to antigens from the body's own cells. If the T-cell reacts to the antigen, it is destroyed to prevent autoimmune disorders. This process is known as positive selection.
The thyroid is an endocrine gland, and is not a site for immune cell development. The lymph nodes are secondary immune tissues and are responsible for conducting the immune response and housing mature lymphocytes, not for immune cell development.
Example Question #377 : Biology
Which type of T-lymphocyte directly destroys infected cells?
Cytotoxic T-lymphocytes
Regulatory T-lymphocytes
Follicular helper T-lymphocytes
Helper T-lymphocytes
Cytotoxic T-lymphocytes
Cytotoxic T-lymphocytes, also known as kill T-cells, directly destroy infected cells by releasing their cytotoxic granules into the cells and causing them to lyse.
Helper T-lymphocytes produce cytokines, which are involved in cell signaling and propagating the immune response. Follicular helper T-lymphocytes control B-cells in lymph nodes. Regulatory T-lymphocytes inhibit the immune response.
Example Question #51 : Immune And Lymphatic Systems
Plasma cells and memory cells are categorized under which division of the immune system?
Non-specific defense mechanisms
Humoral immunity
Cell-mediated immunity
Innate immunity
Humoral immunity
The immune system can be broken down into two main categories: innate and adaptive. Innate immunity includes nonspecific defense mechanisms, and the adaptive side is broken down into two primary sections, humoral and cell-mediated immunity. The key players in cell-mediated immunity are T-cells (including helper, suppressor, memory and cytotoxic T-cells). The humoral response occurs through B-cells, which are the precursors for plasma cells and memory cells. Once a B-cell is exposed to a matching antigen, it will begin to produce two types of daughter cells: plasma cells and memory cells. Plasma cells produce large amounts of antibodies in order to fight the infection at hand, where memory cells will remain in the lymph nodes for the rest of the organism's life. Memory cells are key in an organism's quick secondary response to a microbe that was previously encountered.
Example Question #31 : Immune System
Which of the following cells would be categorized as an agranulocyte?
Monocyte
Basophil
Neutrophil
Eosinophil
Monocyte
Granulocytes are cells categorized because they have vesicles within their membrane that look similar to a granule. Basophils, eosinophils and neutrophils all present granule-like figures and are categorized as granulocytes. Although they derive from the same myeloid stem cells as the granulocytes, monocytes are categorized as agranulocytes.
Example Question #55 : Immune And Lymphatic Systems
Which of the following molecules is not associated with the function of cytotoxic T-cells?
Cytokines
MHC I
CD8
MHC II
MHC II
In terms of MHC restriction, students should be familiar with the fact that cytotoxic T-cells are CD8+ and MHC I restricted. The alternative T subset, the helperT-ell, is CD4+ and MHC II restricted. Both cells rely on cytokines for growth, survival, and their effector functions.
Example Question #32 : Immune System
Eosinophils are play a multi-facted role in the innate immune response especially against parasites. They have been shown to phagocytose different parasites, release cytotoxic granule proteins such as major basic protein (MBP), present antigens to T cells, and produce several different cytokines to promote the inflammatory process.
Eosinophils play a critical role in innate and adaptive immune response against parasitic infections. Which of the following is not a function of eosinophils?
Production of cytokines
Antigen presentation
Phagocytosis
Antibody production
Release of cytotoxic granule proteins
Antibody production
Eosinophils are unable to produce antibody, which are limited to the B cell lineage.
Example Question #33 : Immune System
What is the difference between helper T cells and cytotoxic T cells?
Helper T cells are more adept at cytokine production.
All of these
Helper T cells express CD4 while cytotoxic T cells express CD8.
Helper T cells express MHC II while cytotoxic T cells express MHC I.
Cytotoxic T cells directly kill pathogens while helper T cells assist other immune cells in the inflammatory response.
All of these
Generally, cytotoxic T cells express CD8, express MHC I, are adept at killing specific targets, and while they can produce some cytokines, helper T cells predominantly secrete more different kinds of cytokines and larger quantities of cytokines. Helper T cells express CD4, MHC II, and function primarily in producing cytokines to activate and induce other immune cells to function in the inflammatory response.
Example Question #1 : Adaptive And Innate Immunity
Which of these choices is not a function of T-cells?
Directly produce antibodies after the first response to an antigen
Increase the activity of immune cells (such as B-cells and macrophages) through the release of chemical messengers
Secrete cytokines
Inhibit the activity of both B- and T-cells
Locate and kill cells that contain antigens bound to MHC-I proteins
Directly produce antibodies after the first response to an antigen
The only choice that is not a function of any type of T-cell is the direct production of antibodies (which is performed by B-cells). Cytotoxic T-cells kill other cells that are bound to antigen/MHC-I complexes. Suppressor T-cells tone down the response of both B- and T-cells, and helper T-cells secrete cytokines, which increase the activity of many other immune cell types.
Example Question #52 : Immune And Lymphatic Systems
Sexually transmitted diseases are a common problem among young people in the United States. One of the more common diseases is caused by the bacterium Neisseria gonorrhoeae, which leads to inflammation and purulent discharge in the male and female reproductive tracts.
The bacterium has a number of systems to evade host defenses. Upon infection, it uses pili to adhere to host epithelium. The bacterium also uses an enzyme, gonococcal sialyltransferase, to transfer a sialyic acid residue to a gonococcal surface lipooligosaccharide (LOS). A depiction of this can be seen in Figure 1. The sialyic acid residue mimics the protective capsule found on other bacterial species.
Once infection is established, Neisseria preferentially infects columnar epithelial cells in the female reproductive tract, and leads to a loss of cilia on these cells. Damage to the reproductive tract can result in pelvic inflammatory disease, which can complicate pregnancies later in the life of the woman.
The first line of defense by a human host against a potential Neisseria infection is which of the following?
Innate immune defense
Antibody defense
Lymphocyte-mediated defense
Cytotoxic defense
Genetic immunity
Innate immune defense
Innate defenses, such as the skin or macrophages, are the first line of defense against infection. Other responses only become effective if a pathogen cannot be repelled by innate mechanisms.
Example Question #2 : Adaptive And Innate Immunity
Which of the following is not an example of innate immunity?
Removal of bacterial organisms by cilia
Antibody production by B-cells
Degradation of bacterial cell walls by saliva
Histamine release by mast cells
Antibody production by B-cells
All of the following are examples of non-specific defense mechanisms of the immune system, except for antibody production by B-cells. B-cells respond to specific antigens within the body via immunoglobulins located on the plasma membrane of B-cells. This type of response is known as adaptive immunity, and develops only after a particular pathogen has invaded the immune system.
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