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Samenvatting - Immunopharmacology (WBFA015-05)

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samenvatting immunology

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Subido en
21 de enero de 2025
Número de páginas
56
Escrito en
2021/2022
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Resumen

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Immunopharmacology
Day 1 – Chapter 1
Case study: rheumatoid arthritis → chronic disease→ autoimmune that involves the joints

Bones prevent from grinding at each other because of cartilage and fluid→ rheuma→ attacks bone and
cartilage

TNFalpha→ expressed in high quantities

Symptoms

- Pain in joints→ because of inflammation
- Stiffness→ edema
- Muscle weakness
- Weight loss
- Fatigue
- Fever
o All 3 because of TNFalpha

Goal of treatment

- RA is most progressive at the start of the disease→ start treatment quickly and effectively to
prevent damage to joints

Drugs used in RA

- Painkillers
- NSAIDs-→ pain and inflammation
- Corticosteroids
- DMARDs→ methotrexate, biologicals
o Methotrexate → prevents rapid proliferation of cells
o Biologicals directed at immune components

Case study→

- New symptoms→ painful and swollen fingers
- Paracetamol or NSAIDs
- See slide for the recommendations
- Adalimumab → blocks TNFalpha
- Combination of methotrexate and adalimumab → magnify each other

Innate vs adaptive immunity

- Ehrlich→ adaptive
- Mechnikov→ innate



Humoralist → people that study side chains

,Toll-like receptor→activating the immune system→ function like alarm system

Overview innate and adaptive immunity

- Cellular alarm systems
- Epithelial layers→ safety in numbers
o Tissue-resident immune cells→ patrol and deal with a
problem when it occurs
o Not enough? Get help from bone marrow
- Cleaning up tissue
- Specialized help from lymphocytes→ t-helper/cytotoxic t
cells
- B cells and antibodies→ extracellular defense

Characteristics innate vs adaptive

Immune cells and their origin

All leukocytes (white blood cells) develop from stem cells in bone marrow OR yolk sac/fetal liver

First immune cells come from yolk sac→ fetal liver take over→ once bone marrow is developed →
immune cells get developed there

Macrophages → either derived from monocytes or fetal liver cells

Most macrophages in CNS are coming from fetal liver cells→ because brain closes off and monocytes
can’t reach it

Mostly myeloid cells are innate

Mostly lymphocytes are adaptive

But sometimes both!

Immune cells communicate through APC→ macrophages and
dendritic cells

Present them to T-cells

Dendritic cells→ functions like a messenger → travel from tissues to lymph nodes to look for help from
more specialized cells: B and T cells

APC patrol tissues, especially the ones that connect to the outside world

Lymphocytes patrol the body looking for antigens they recognize

Lymphoid structures

- The immune system can be seen as a diffuse, body-spanning organ
- Solid tissues
- Fluid tissues
- Fluid molecules

,- Solid lymphoid tissues are everywhere
- Primary lymphoid tissues → where lymphoid tissue is born→ development, selection and
maturation
o Bone marrow
o Thymus
- Secondary → get educated → go from naïve to experienced → sites for initiation of immune
responses
o Spleen
o Lymph nodes
o MALT

Antigen= any molecule that is specifically recognized by lymphocytes or antibodies

T and B cell development

Lymphatic circulation→ drains organs from fluids and immune cells

Lymph vessels end up in lymph nodes

Dendritic cells carrying an antigen comes in to the nod via the afferent lymphatic vessel→ see if antigen
is recognized by B or T cells→ not recognized → go to the next lymph node via the efferent vessel

Spleen

- Lymph node of the blood
- Function of removing old blood cells
- Checks the blood for pathogens
- Leaf-like structure
- B-cells and follicles on outside
- T-cells in the middle
- Red pulp→ macrophages to remove damaged cells (RBC) and invaders/reservoirs of monocytes
- White pulp→ B and T cells, for adaptive response against blood-born antigens

Circulation of T cells

- Naïve and experienced cells
- Both present in blood
- Naïve cells get into lymph node looking for something to recognize
- Effector cells leave the lymph node and go to active site

Lymphoid structures in tissue

- Tissues connected to outside world have their own lymphoid structures
- For faster response against threats:

Gut has most specialized immune cells→ exposed the most to microbes

- Then the bronchi
- Lastly the skin → least organized

Lymph nodes at work→ lymphs will grow

, Day 2 – Chapter 2
Innate immune system

Cellular alarm systems

- Antigen recognition system
- Limited number of receptors
- Distribution of receptors is clonal → same type of receptors → recognize the same patterns

Characteristics of microorganisms → PAMPS

- Components of cell wall
- LPS
- PAMPS

RNA/DNA viruses

- Bacteria have specific patterns→ LPS
- DNA is also different
- Differences are being recognized

What are characteristics of tissue damage

DAMPS

- ATP/DNA leak out
- Components that are normally not exposed leak out of the cell

Cellular alarm systems→ pattern recognition receptors

- Toll-like receptors (TLR)
- C-type lectin receptors
- NOD-like receptors (nucleotide oligomerization domain)
- RIG-like receptors (retinoic acid-inducible gene)

TLR

- Most common receptors
o Outside of cells
o Endosome
o Cytosol
- NOD/RIG- like receptors
o RIG→ viruses
o NOD→bacteria
- TLR→ recognize bacterial cells

TLR

- Different components on different locations of the cell
- TLR mostly made out of RNA
- What happens when a TLR recognize a component in the cell?
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