Adaptive Immune Response Flashcards

1
Q

How does a T cell kill a pathogen

A

An APC has to process the antigen - T cell can then bind and become active. Cytotoxic T cells kill the pathogen
Naive T cells cannot produce a response
Apc interacting with t lymphocyte (naive - not been activated by antigen yet)
amp gies 3 pieces of info
• invader
• what it looks like
• type o immune response

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2
Q

What are the features of APCs?

A

Features of Antigen Presenting Cells

• Strategic location (B and T cell interaction)

  • Skin (SALT)
  • Mucous membranes (GALT, NALT, BALT, GUALT)
  • Lymphoid organs (Lymph nodes, spleen)
  • Blood circulation (plasmacytoid and myeloid DCs)
• Pathogen capture
- Phagocytosis (whole microbe) 
- Macropinocytosis (soluble particles)
• Diversity in pathogen sensors (PRRs)
- Extracellular pathogens (bacteria) 
- Intracellular pathogens (viruses)
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3
Q

Name different types of APC, their location, and the type of T cll they present to

A

Dendritic cells (lymph nodes, mucous membranes, blood) - naive T cells

Langerhans cells (skin) - naive T cells

Macrophages (various tissues) - effector T cells

B cells (lymphoid tissues) - effector T cells & naive T cells

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4
Q

Describe what happens once the APC recognises the pathogen

A
  • Dendritic cells sense microbe PAMPS - tell T cells to activate the humoral immunity - best response to combat extacellular microbes
  • antibodies - means there is complement activation and phagocytosis
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5
Q

How is a virus removed?

A
  • viruses replicate inside cells - viral protein ins ide the cells dendritic cells have receptor
  • only way to clear infection is to kill viral infection cells - kill all viral infected cells - cytotoxic cells
  • hla??? Human version?? Mhc = mammalian??
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6
Q

What are class 1 and class 2 molecules on mhc/hla

A

Class I molecules Found on all nucleated cells - HLA A/B/C

Class II molecules Found on dendritic cells, macrophages, B cells - HLA-DP/DQ/DR

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7
Q

What are key features of MHC class i and ii molecules?

A

Key features of MHC class I and class II molecules
• Co-dominant expression
- Both parental genes are expressed
-> ↑ number of different MHC molecules
• Polymorphic genes
- Different alleles among different individuals
-> ↑ presentation of different antigens/microbes
• Main function
- MHC Class I: present peptides from intracellular microbes - MHC Class II: present peptides from extracellular microbes
• The more diverse the molecule the better ,the more diverse the microbe the immune response can be mounted against
• co dominant - 6 from each parent
• different alleleic varying - increase type of mucus - increase recognition - increases bility to activate T cells

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8
Q

Describe the structure of mhc class i and ii molecules

A
• Peptide binding cleft
- Variable region with highly
polymorphic residues
• Broad specificity
- Many peptides presented by the same
MHC molecule
• Responsive T cells
- MHC class I recognized by CD8+ T cells - MHC class II recognized by CD4+ T cells
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9
Q

What are the 2 antigen processing pathways

A

Endogenous and exogenous
• Both self and non-self peptides are presented
• All peptides from the same microbe are presented by different MHC molecules
• Susceptibility to infections depends on the types of MHC molecules

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10
Q

What is the endogenous pathway

A
  • When proteins produced in the cytoplasm - labelled for degradation - targeted - degrade by proteasome - uptaken by transporters - get into ER - expression of host Mhc class 1 - if you have right match for right mhc - makes a complex - complex shifted to cell surface - limitations.- if you dont have right Mhc, wont be able to present the right peptide
  • Mhc class.1 on all cells - call cells can get infected
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11
Q

What is the exogenous pathway

A

• Exo - antigen always in vesicle - vesicles fused with lysosomes - gives small peptides - fuse with another vesicle - Mhc class 2 waiting there - if there is a right match be peptide and much 2 - stable and expressed at the cell surface

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12
Q

What are ltnps?

A

Some patients called Elite controllers or long-term nonprogressors (LTNP)
can control viral replication

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13
Q

What is the difference between slow/rapid progress or

A

Slow - mhc molecules present key peptides for the survival of the virus - effective T cell response
Rapid - mhc molecules present mutated peptides less critical for the virus - poor recognition by T cells so poor T cell response

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14
Q

What are the clinical problems with mhc molecules

A

• Major causes for organ transplant rejection
- HLA molecules mismatch between donor and
recipient (Allograft) - Graft-Versus-Host reaction (GVH)
• HLA association and autoimmune disease
- Ankylosing spondylitis
• HLA-B27 -> 90% of patients - Insulin-Dependent Diabetes Mellitus
• HLADQ2 -> 50-75% of patients

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15
Q

What are intracellular/extracellular microbes and whats the difference

A
Extracellular Microbes - Bacteria - Parasites - Worms - Fungi 
-> mhc class ii -> cd4 +t cells -> humoral (b cells nd complement)

Intracellular Microbes - Viruses - Bacteria - Protozoa
-> cd4 + T cells -> cell dependent immunity (b cells and complement)
cd8 + T cells -> cytotoxic T cells

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16
Q

What are costimulatry proteins

A

?

17
Q

What’s the difference between the T cell response to intracellular and extracellular microbes?

A

See slide

18
Q

What’s are the acaracteristics of the antibody response

A

When host in contact - immunoglobulin produced - subsequent encounter - main igg bc it is best antibody response bc it can get deep into tisse
ratio between igg and igm can tell u if its chronic or acute
second response is faster and stronger - much more igg than igm. See listening for graph

19
Q

What are the fucntions of IgG

A

IgG Fc-dependent phagocytosis
Complement activation
Neonatal Immunity
Toxin/virus neutralization

20
Q

What are the fucntions of IgA

A

Mucosal immunity

21
Q

What are the functions of IgE

A

Immunity against helminths

Mast cell degranulation (allergies)

22
Q

What are teh fucntions of IgM

A

Complement activation

23
Q

What are medical advances derived from the study of tha adaptive immune response

A

• Disease prevention
- vaccination

• Immunoglobulin therapies
- immune deficiencies

• Immediate protection
- passive immunisation

• Diagnostic tests (antibody-based)

  • infectious diseases
  • autoimmune diseases
  • blood type and hla types