Lecture 2 Flashcards

1
Q

T-Cells

A

Develop and mature in the thymus; when a mature T cell is Ag-stimulated, it gives rise to cellular immunity

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2
Q

B-Cells

A

Develop and mature in the bone marrow and gives rise to humoral immunity (immunity that involves production of soluble molecules called immunoglobulins); recognize soluble Ags and develop into Ab-secreting cells

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3
Q

Humoral Adaptive Immunity

A

Mediated by Abs in the blood and mucosal secretions which are produced by B-cells; Abs recognize microbial Ags, neutralize the infectivity of the microbes, and target microbes for elimination by various effector mechanisms

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4
Q

Cellular Immunity (Cell-Mediated)

A

Controlled by responses of T-cells which often function in concert with Ag-presenting cells and phagocytes to eliminate microbes; mediates host defense against intracellular microbes, such as viruses and some bacteria, where they are inaccessible to circulating Abs; functions to kill infected host cells to eliminate reservoirs of infection

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5
Q

T-Helper Cells

A

Help B-cells to make effective Abs thus contributing to eradication of extracellular microbes; also activate tissue-resident macrophages to kill phagocytized microbes or cytotoxic T cells to directly destroy infected cells in cellular immunity; recognize Ags on the surfaces of Ag-presenting cells and secrete cytokines; express CD4 and provide help for B cell growth and differentiation

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6
Q

Paul Ehrlich

A

“Father of Humoral Immunity”; postulated that immune cells can secrete receptors which recognize microbial toxins and combat invading microbes; also coined the term Abs for the serum proteins that bind toxins

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7
Q

Elie Metchnikoff

A

“Father of Cell-Mediated Immunity”; discovered special immune cells and named them phagocytes which, he believed, are the principal effector mechanism of immunity; was unable to prove that specific immunity to microbes could be mediated by cells

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8
Q

Specificity

A

Ensures that the immune response to a microbe (or non microbial Ags) is selective to that microbe (or Ag)

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9
Q

Diversity

A

Enables the immune system to respond to a large variety of Ags

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10
Q

Memory

A

Increases the ability to combat repeat infections by the same microbe

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11
Q

Clonal Expansion

A

Increases the number of Ag-specific cells to keep pace with microbes

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12
Q

Specialization

A

Generates responses that are optimal for defense against different types of microbes

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13
Q

Contraction and Homeostasis

A

Allows the immune system to recover from one response so that it can effectively respond to newly encountered Ags

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14
Q

Nonreactivity to Self

A

Prevents injury to the host during responses to foreign Ags

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15
Q

Clonal Selection Hypothesis

A

Ag-specific clones of lymphocytes develop before and independent of exposure to Ag; the immune system generates a very large number of clones during the maturation of lymphocytes, thus maximizing the potential for recognizing diverse microbes; each Ag selects a preexisting clone of specific B-cells and stimulates the proliferation and differentiation of that clone (same principle applies to T-cells)

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16
Q

Clone

A

Lymphocyte of one specificity and its progeny

17
Q

Active Immunity

A

Conferred by a host response to a microbe or microbial Ags

18
Q

Passive Immunity

A

Conferred by adoptive transfer of antibodies or T-cells specific for the microbe

19
Q

Cytotoxic T-Cells

A

Recognize Ags on infected cells and kill these cells; express CD8 and recognize and kill virus-infected cells

20
Q

Regulatory T-Cells

A

Suppress and prevent immune responses to self Ags

21
Q

Primary Lymphoid Organs

A

Thymus and bone marrow

22
Q

Secondary Lymphoid Organs

A

Spleen, lymph nodes, and mucosa-associated lymphoid tissue

23
Q

Ag-Specific Receptors

A

Localized on the surface of T and B cells; structure varies from one cell to another but they are all identical on a single cell