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Lecture notes of pharmacology for nutritionists

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Lecture notes of pharmacology for nutritionists including the tutorials on behavioural pharmacology

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Uploaded on
March 18, 2025
Number of pages
12
Written in
2022/2023
Type
Class notes
Professor(s)
Michiel balvers and renger witkamp
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All classes

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Pharmacology:
Lecture 2:
Receptors:

-Ion channels:

-Multi-subunit ion channels

-Location: cell surface transmembrane

-Bindingion influxeffect on cell excitability

-Examples of ligands: acetylcholine, GABA, glutamate, glycine

Allosteric modulator: when a drug binds to a different part of the receptor.

-Protein kinases:

-Location: cell surface

-Ligands: growth factors, peptide hormones

-Proteins become activated after binding open or close

-Transcription factors:

-Location: cytoplasm

-Ligands: steroid hormones, thyroid hormone, vitamin D

-Activation/suppression DNA transcription

-G-protein coupled receptors:

-Location: cell surface, 7 TM

-Ligands: acetylcholine, a- B-adrenergic eicosanoids

-GTPGDP

-One of most important drug targets

Step 1: ligand binds to receptor, Bg get split off and move to target 2

Step 2: a splits off receptor and moves to target 1. a receives GTP before
move.

Step 3: GTP in a splits off P GDP. Target 1 and 2 activated

Step 4: ka and Bg bind back to receptor. What happens next depends on
target effector protein.

CAMP system:

-Second messenger

-Activated G-protein activates adenylyl cyclase ATP-cAMP activates protein kinase A

, -G-protein that activates cAMP formation: stimulatory G-protein

Regulating GPCR signaling-off signal

-GTP activated a-subunit has intrinsic GTP-ase activity

-Phosphodiesterase hydrolyses cAMP AMP

-Without these mechanisms, no turning off receptors

Receptor desensitization:

-Some receptors are phosphorylated via specific receptor kinases

-The phosphorylated receptor may then bind to a protein b-arrestin that promotes removal
of the receptor.

Inhibitory G-proteins: inhibits adenylate cyclase

-Cannabinoid receptors:

-Important endogenous regulation

-2 G-protein coupled receptors so far

-Many endogenous end exogenous cannabinoids

-Specific transporters

-Appetite stimulation

-Hallucinogenic euphoric

-Anti-inflammatory

We have our own endocannabinoid system in fatty acids increased in obesity

Receptor models:

Agonist: locked in active state

Antagonist: keeps receptor neutral, prevents agonist from binding

Competitive antagonist: binds at same site as agonist

Non-competitive antagonist: binds on different site

Reversible/irreversible

Inverse agonism : actively pushes receptor in active mode
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