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Monoclonal Antibodies An antibody An immunoglobulin synthesized
Monoclonal Antibodies An antibody An immunoglobulin synthesized

... produce a single MAb. 5. Each MAb is screened for its ability to attack the original cancer cells, and the hybridomas producing the desired antibody are kept. 6. The desired hybridoma cells are injected into a mouse where they form a tumor that produces large amounts of concentrated antibody. ...
Organs and Tissues of the Immune System
Organs and Tissues of the Immune System

... Direct Ag recognition, no need for MHC. Secrete cytokines that cause immune suppression at the mucosa. Oral tolerance. ...
Human Physiology - Daniela Sartori
Human Physiology - Daniela Sartori

... small non-antigenic molecules that become antigens when bound to proteins (form an antigenic determinant site) Useful for creating antibodies for research and diagnosis ...
Slide Presentation (Powerpoint)
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... Increased replication potential ...
35.3 Fighting Infectious Disease
35.3 Fighting Infectious Disease

... Smallpox is a deadly, highly-contagious disease that was once common throughout Europe, Asia, and North Africa. The war against smallpox began in the late 1700s when the British physician Edward Jenner developed a smallpox vaccine. In the 1900s, there was a worldwide effort to administer the vaccine ...
Viruses
Viruses

... – 4 = the pathogen should be taken from the second animal, grown in the lab, and shown to be the same as the original pathogen. ...
The Immune System
The Immune System

... • Natural Killer (NK) Cells- Patrol the body and attack virus-infected cells and cancer cells • Surface receptors (“nametags”) identify these infected/damaged cells • NK cells release chemicals that cause cells to kill themselves, apoptosis (programmed cell death) • Indiscriminate . . . can damage s ...
AP Biology - Al Young Studios
AP Biology - Al Young Studios

... 10. Distinguish between antigens and antibodies. 11. Explain how B cells and T cells recognize specific antigens. 12. Explain how the particular structure of a lymphocyte's receptor is determined. 13. Describe the mechanism of clonal selection. Distinguish between effector cells and memory cells. 14 ...
Chapter 24
Chapter 24

... (b) many will never encounter the antigen they were designed for i) Antigens have specific regions where antibodies bind i) antigenic determinants (1) specific regions on the antigen recognized by the antibody (2) antigenic determinant has complementary shape to antibody (3) several determinants on ...
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ovary - Hale AP Biology

... ◦ Differences in MHC molecules stimulate rejection of tissue grafts and organ transplants ...
UVic Grad Infosheets (draft 2)
UVic Grad Infosheets (draft 2)

... Genetic and biochemical characterization of genes and proteins involved in bacterial pathogenesis; particularly those in the pathogenicity island of Francisella tularensis which encodes a novel type VI secretion system. Substitution of essential genes from sychrophilic (cold-loving) bacteria into pa ...
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The specific immune response B and T cells

... 15.ref to secondary response; e.g. more rapid / greater AVP; e.g. suppressor cells AVP; e.g. function of suppressor cells 16.cell mediated response ...
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1. dia - Department of Immunology

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The Babraham Institute

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31_Immune responses to viruses BA

... 2. Killing by virus-specific CD8+ T lymphocytes – CD4+HIV+ targets 3. Syncytia formation – gp120 of infected T cells binds to uninfected T cells  fusion ...
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Final Immunology Overview

...  The innate immune response is present all the time and works immediately as soon as it encounters a pathogen. It doesn’t have any memory, so the next time it encounters that pathogen it won’t work faster, better, or more vigorously than it did the first time. It doesn’t recognize the pathogen in a ...
biopresibstandards
biopresibstandards

... is often lethal, even when antibiotic treatments are give. Anthrax spores have sometimes been used deliberately to infect more people and cause death. Monoclonal antibodies are being developed which neutralize one of the toxins and therefore sustain the patient’s life until their immune system produ ...
Elevated potassium levels suppress T cell activation within tumors
Elevated potassium levels suppress T cell activation within tumors

... transcription in CD8+ and CD4+ effector T cells. Moreover, polarization of CD8+ and CD4+ T cells in high K+ suppressed effector differentiation and promoted the formation of CD4+ Foxp3+ Treg cells. Surprisingly, this was not due to an attenuation of TCR induced Ca 2+ flux, but rather to reduced acti ...
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diagnosis of hiv infection the laboratory

... 2- 8 weeks of acquiring the infection( not useful for early infections) IgM- Gag proteins. IgG- p 24 antigen and the gp120…. gp 41 Persistently undetectable antibodies more than 3 months – rare. ...
22-23-Effector T-cells-Th-Tc
22-23-Effector T-cells-Th-Tc

22-23-Effector T-cells-Th-Tc
22-23-Effector T-cells-Th-Tc

The Body’s Defenses - Falmouth Schools in Falmouth Maine
The Body’s Defenses - Falmouth Schools in Falmouth Maine

... • Antibodies must recognize huge range of potential antigens found in pathogens (bacteria, viruses) but not recognize proteins produced by organism. • Antibodies - complex proteins assembled from multiple polypeptides joined by disulfide bridges between light and heavy chains. ...
Chapter 8 Immune Organs
Chapter 8 Immune Organs

... The first line of defense against foreign antigen. The site of immune response. Participate in delayed hypresensitivity. ...
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Molecular mimicry

Molecular mimicry is defined as the theoretical possibility that sequence similarities between foreign and self-peptides are sufficient to result in the cross-activation of autoreactive T or B cells by pathogen-derived peptides. Despite the promiscuity of several peptide sequences which can be both foreign and self in nature, a single antibody or TCR (T cell receptor) can be activated by even a few crucial residues which stresses the importance of structural homology in the theory of molecular mimicry. Upon the activation of B or T cells, it is believed that these ""peptide mimic"" specific T or B cells can cross-react with self-epitopes, thus leading to tissue pathology (autoimmunity). Molecular mimicry is a phenomenon that has been just recently discovered as one of several ways in which autoimmunity can be evoked. A molecular mimicking event is, however, more than an epiphenomenon despite its low statistical probability of occurring and these events have serious implications in the onset of many human autoimmune disorders. In the past decade the study of autoimmunity, the failure to recognize self antigens as ""self,"" has grown immensely. Autoimmunity is a result of a loss of immunological tolerance, the ability for an individual to discriminate between self and non-self. Growth in the field of autoimmunity has resulted in more and more frequent diagnosis of autoimmune diseases. Consequently, recent data show that autoimmune diseases affect approximately 1 in 31 people within the general population. Growth has also led to a greater characterization of what autoimmunity is and how it can be studied and treated. With an increased amount of research, there has been tremendous growth in the study of the several different ways in which autoimmunity can occur, one of which is molecular mimicry. The mechanism by which pathogens have evolved, or obtained by chance, similar amino acid sequences or the homologous three-dimensional crystal structure of immunodominant epitopes remains a mystery.
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