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Summary Immunology and Disease, RuG (English)

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This is a summary for the Immunology and Disease course in the second year of the Biology study at the Rug. I have made this exam and my summary really helped me, I hope it will help you as well. The way I write my summaries is easy to understand with a casual writing style. I will say that this exam is also for a large part a repetition of the Immunology course, so I would also advise to relearn that. If you need help for that, I have a summary written about that course as well, called; Immunology :) Love, Myrthe

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Subido en
27 de febrero de 2025
Número de páginas
30
Escrito en
2024/2025
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Immunology and disease
Index:

Immunopathologic reaction types ————————————————— page 2

Inflammation —————————————————————————— page 3

Pathogen responses ——————————————————————— page 4

Things that can go wrong ————————————————————— page 6

Vaccines ———————————————————————————— page 7

Immunoassays

- Immunohistochemistry —————————————————— page 9

- Flow cytometry ————————————————————— page 10

- ELISA ————————————————————————— page 11

Transplantology ————————————————————————— page 12

Cancer ————————————————————————————— page 15

Immunodeficiency ———————————————————————— page 17

Autoimmunity —————————————————————————— page 19

Mucosal immunity ———————————————————————— page 21

Allergies ————————————————————————————page 23

Bonus: Effects of old age on the immune system —————————— page 26




Page 1

,Immunopathologic reaction types:
There are in total 4 different types and in my opinion they go from least serious to
deadly serious;

Type 1: immediate hypersensitivity
It is an immune reaction against (sometimes harmless) agents. Upon first expo-
sure, B cells produce IgE antibodies that bind to Fcε receptors on mast cells
and basophils, sensitizing them. Upon re-exposure, the allergen cross-links IgE,
triggering mast cell degranulation and the release of histamine.
This is also what happens with allergies.

Type 2: antibody mediated toxicity
The IgM and IgG antibodies bind against the cell surface or extracellular matrix.
This can lead to opsonization and subsequent phagocytosis by macrophages,
activation of the complement system.

Type 3: immune complex mediated
This occurs when IgM or IgG antibodies form immune complexes with soluble
antigens. These complexes deposit in tissues, particularly in blood vessels.
Then the complement activation and leukocyte recruitment (especially neu-
trophils) lead to tissue inflammation and damage.

Type 4: T-cell mediated
Unlike the other types, this reaction is mediated by T cells rather than antibod-
ies. CD4+ T-cells recruit and activate macrophages and other immune cells,
leading to delayed inflammation. CD8+ T-cells can directly kill infected or ab-
normal cells. This reaction typically manifests 24–72 hours after antigen expo-
sure.




Page 2

, Inflammation:
Signs of inflammation:
• Tumor: Swelling
• Rubor: Redness
• Calor: Heat
• Dolor: Pain
• Functio Laesa: Loss of function

There are different types of inflammation; acute and chronic.

Acute inflammation response works in 7 steps;
1. A physical barrier (e.g. epithelial layer) breaks which allows entry for microbes.
2. The microbes activate sentinel cells*.
3. Sentinel cells secrete inflammatory cytokines.
4. Then the blood vessels dilate (vasodilation), which increases the blood flow, this
causes fluid and proteins to enter this area.
5. Complement, antibodies and antimicrobial protein kill the microbes.
6. Adhesion molecules cause leukocyte migration to the tissue.
7. Which then finally leads to the phagocytosis of the microbes.

*sentinel cells are dendritic cells (DC), macrophages and mast cells.

To stop the inflammatory response, regulatory T-cells (Treg) are the most important.
When sentinel cells can no longer sense PAMPs or DAMPs, the switch from pro-
inflammatory to anti-inflammatory mode, and they will start producing anti-
inflammatory cytokines.
Treg cells will also start producing anti-inflammatory cytokines. If it didn’t do this, then
it could lead to chronic inflammation.




Important pro-inflammatory cytokines are; TNF, IL-1, IL-6
Important anti-inflammatory cytokines are; IL-10, TGF-ß

They are produced by macrophages, mast cells and epithelial cells
Chronic inflammation stays active for weeks, months or even years! Instead of
resolving the issue, the immune system stays constantly activated, which will lead to
tissue damage and fibrosis, which is a fancy word for scarring.

Page 3
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Biology student, RuG

I study Biology at the RuG, for which I chose the major Biomedical sciences. For every course I make a new summary to help me study, but here I want you all to also profit from my hard work. I do my best to make the summaries as enjoyable as possible, while still containing all the necessary details. I hope you will enjoy studying biology as much as I do :)

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