Deck 14: The Immune Response in Time and Space

A)antigen is usually present in large amounts.
B)lymphocytes have a small chance of recognizing a particular antigen.
C)the chance of a naïve cell encountering its target antigen is moderately high.
D)there are relatively few antigen-presenting cells in the lymph nodes compared to lymphocytes.
E)All of the answers are correct.

A)Homing
B)Addressins
C)Chemokines
D)Dendritic cells
E)All of the answers are required.

A)thymic cortex
B)lymph node medulla
C)lymph node cortex
D)high-endothelial venule
E)None of the answers are correct.

A)are made of fibroblasts.
B)guide T-cell movements.
C)guide B-cell movements.
D)regulate lymphocyte direction.
E)All of the answers are correct.

A)Follicular dendritic cells
B)Fibroblastic reticular fibers
C)Chemokines CCL21 and CCL19
D)The chemokine CXCL13
E)Naïve B cells do not depend on any of the answer choices provided.

A)the naïve cells have not been activated.
B)the naïve cells have not encountered antigen.
C)the naïve cells will exit the lymph node.
D)space will be made for other cells to enter the lymph node.
E)the naïve cells will die by apoptosis.

A)coordinate killing of pathogens.
B)alert the adaptive immune system of an infection.
C)recognize specific pathogen.
D)both coordinate killing of pathogens and alert the adaptive immune system of an infection.
E)both coordinate killing of pathogens and recognize specific pathogens.

A)become less effective at phagocytosis.
B)become more effective at antigen processing.
C)become less effective at cross presentation.
D)recruit more adaptive immune cells than innate immune cells.
E)remain at the site of infection.

A)Antigen uptake > antigen processing > APC migration to lymph nodes > antigen presentation
B)APC migration to lymph nodes > antigen uptake > antigen processing > antigen presentation
C)APC migration to lymph nodes > antigen presentation > antigen uptake > antigen processing
D)Antigen uptake > antigen processing > antigen presentation > APC migration to lymph nodes
E)APC migration to lymph nodes > antigen uptake > antigen presentation > antigen processing

A)processed for presentation to B cells.
B)processed for presentation to T cells.
C)moved without processing over several hours to the lymph nodes.
D)taken in unprocessed form for presentation to T cells.
E)All of the answers are correct.

A)Small and soluble antigens travel through afferent lymphatics as opsonized particles.
B)Small and soluble antigens travel directly through the bloodstream.
C)Large particles and pathogens travel directly through the bloodstream.
D)Opsonized pathogens travel directly through the bloodstream.
E)Small particles are carried by macrophages.

A)CD169⁺ macrophages > follicular dendritic cells > antigen nonspecific B cells
B)Antigen nonspecific B cells > CD169⁺ macrophages > follicular dendritic cells
C)CD169⁺ macrophages > antigen nonspecific B cells > follicular dendritic cells
D)Antigen nonspecific B cells > follicular dendritic cells > CD169⁺ macrophages
E)None of the answers are correct.

A)normal B cells sample antigen on macrophages and leave it intact.
B)normal B cells sample antigen on macrophages and take part of it.
C)complement receptor-deficient B cells do not sample antigen on macrophages.
D)complement receptor-deficient B cells sample antigen on macrophages and take part of it.
E)None of the answers are correct.

A)Granulocytes
B)Antigen-presenting cells
C)Cytotoxic T cells
D)Dendritic cells
E)Neutrophils

A)interact with antigen-presenting cells.
B)reduce movement.
C)begin to divide.
D)move to interact with B cells.
E)All of the answers are correct.

A)antigen availability does not affect T-cell/APC interactions.
B)antigen quantity does not affect T-cell/APC interactions.
C)optimal proliferation of helper T cells requires only relatively brief APC exposure.
D)optimal proliferation of helper T cells requires several hours of APC exposure.
E)dendritic cell activation does not affect T-cell activation.

A)T cells provide signal 1 through the B-cell receptor.
B)T cells provide signal 2 through the B-cell receptor.
C)T cells activate B cells indirectly by activating follicular dendritic cells.
D)T cells activate B cells through CD40 signaling.
E)B cells will still activate because of dendritic cells.

A)All produce the same chemokine to activate but provide different CD40 signals.
B)All produce the same chemokine and the same CD40 signal as well.
C)All provide CD40 signaling but produce different chemokines.
D)All provide CD40 signaling but trigger distinct class switching.
E)All provide CD40 signaling but produce different chemokines and trigger distinct class switching.

A)antigen triggers B-cell production of CCR7, which leads it to interact with T cells.
B)antigen triggers T-cell production of CCR7, which recruits B cells.
C)T-cell help stimulates B cells to produce CCR7, then divide.
D)macrophages trigger B-cell production of CCR7, which leads it to interact with T cells.
E)None of the answers are correct.

A)CD28 is needed to activate class switching by turning on AICD.
B)CD28 is needed to interact with CD40 on the B cell.
C)CD28 is needed to signal through the B-cell receptor.
D)CD28 is needed to signal through the T-cell receptor.
E)None of the answers are correct.

A)the traditional model of trafficking is inaccurate.
B)the rate of hypermutation and selection does not require extensive movement.
C)only brief contacts by the B cells with helper T cells are needed.
D)both the traditional model of trafficking is inaccurate and only brief contacts by the B cells with helper T cells are needed.
E)both the rate of hypermutation and selection does not require extensive movement and only brief contacts by the B cells with helper T cells are needed.

A)follow chemokine trails.
B)do not home in to the lymph nodes.
C)do not require co-stimulation.
D)All of the answers are correct.
E)None of the answers are correct.

A)bone marrow.
B)afferent lymphatics.
C)the follicle border of lymph nodes.
D)the red pulp of the spleen.
E)All of the answers are correct.

A)up-regulate chemokine receptors to allow them to home in to site of infection.
B)down-regulate L-selectin, so they do not enter the high-endothelial venules (HEVs).
C)down-regulate chemokine receptors, so they do not enter the high-endothelial venules (HEVs).
D)up-regulate chemokine receptors and downregulate L-selectin.
E)down-regulate both L-selectin and chemokine receptors.

A)T-cell behavior followed patterns predicted by previous studies.
B)dendritic cell behavior followed patterns predicted by previous studies.
C)lymph-node architecture changed due to inflammation.
D)T cells divided at the site of infection.
E)All of the answers are correct.

A)Central memory T cells.
B)Effector memory T cells.
C)Tissue-resident memory T cells.
D)Memory B cells.
E)None of the answers are correct.

A)any infiltration of a skin graft depends on MHC mismatch.
B)deep infiltration of a skin graft depends on MHC mismatch.
C)host antigen-presenting cells enter the skin graft before migrating to lymph nodes.
D)both any infiltration of a skin graft depends on MHC mismatch, and host antigen-presenting cells enter the skin graft before migrating to lymph nodes.
E)both any infiltration of a skin graft depends on MHC mismatch and host antigen-presenting cells enter the skin graft before migrating to lymph nodes.

A)avoids being broken down and presented as antigen.
B)localizes quickly to lymph nodes and persists there.
C)reproduces inside macrophages.
D)is passed by dendritic cells to monocytes.
E)None of the answers are correct.

A)failure of tumor antigen presentation.
B)failure of activation of tumor-specific T cells.
C)failure of recruitment of T cells to the tumor.
D)failure of the T cells to produce cytotoxic effector molecules.
E)All of the answers are correct.

A)Listeria
B)Tissue grafts
C)Solid tumors
D)Type 1 diabetes
E)All of the conditions are contributed to by immune responses.