Lecture 1- Textures in Ligand Binding Flashcards

1
Q

Why are receptor-ligand interactions important?

A
  1. Receptors mediate the actions of naturally occuring ligands (hormones, NT, light, odors) and drugs
  2. Receptors determin the quantitative relation between concentration of the ligand and pharmacologic effect
  • receptor affinity for a ligand determines the concentration of the ligand needed to generate the effect
  • # of receptors can limit the max effect a drug might have
  1. Receptors are responsible for how selective drugs act
  • shape, size, charge of a ligand determines IF and the AFFINITY a ligand will bind a receptor/specific site of a receptor of all the available ones in the cell
  • changes in the ligand chemical structure can increase or decrease the affinity for a receptor –> this can result in alterations of therapeutic or toxic effects
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2
Q

Ligands can…

A
  1. Can be intrinsic to a receptor
    * cleavage needed to activate it
  2. Need a trigger to become active
  • already present in the receptor
  • needs to get activated to induce its response
  1. Come from other cells
  • need to travel a certain distance
  • bloodstream
  • ex: hormones: produced by organs somewhere, trafficked in blood, reaches target
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3
Q

Class C GPCRs

A
  • Sushi domain creates disulfide bonds required to maintain tertiary structure: keeps a binding site alive!
  • For GPCRS, multiple classes
  • 7 transmembrane domains, integrated in PM
  • different extracellular domains can be present on a receptor
  • has long tails on outside of cell, that is what catches the ligand
  • two domains that are like pacmans: catch a ligand
  • thats where ligand binds

Class C GPCRS: ligands bind in extracellular portion

  • Variability among receptors even if there in same class
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4
Q

Class A GPCR

A
  • Structure of b2ar and rhodopsin with 2 ligands in them.
  • 2 different structures shown
  • could be seen as a snake or a barrel
  • creates hole in the middle
  • hole in middle (red) where the ligand binds to the receptor
  • To activate them, ligands need to penetrate into the barell
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5
Q

Diversity among extracellular domains affect ligand binding capacities

A
  • Long tail, may be masking the hole
  • Based on diff receptors, will have different affinities for the ligand to bind that place/receptor
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6
Q

Do different structures bind the same receptor?

A

Although different structures for those ligands, all bind the same receptor, but bind at different sites

  • binding at one site on receptor, has a ripple effect all across the receptor à differences in efficacy
  • bind ligand at one part, may be able to bind a little bit more or less of ligands
  • ligand pulls at one site, another ligand pulls at another site
  • gives you different efficacy for that receptor
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7
Q

Shape, size, and charges all play a role that shapes where the ligand will bind

A
  • Different a.a lining the binding pocket of that receptor
  • attraction and repulsion
  • If it attracts, frees up one side
  • Get first, second touch –> shapes and creates a stable conformation in the end
  • Movement of transmembrane domains and a.a, even the ligand flips sometimes
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8
Q

How do we get receptor activation

A
  • disruption of the ionic lock
  • EX: Ripple effect from binding of ligand à conformational change that rotates the glutamine, allows the receptor to open up and have a shape to where it gets activated
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9
Q

The rhodopsin receptor model

A
  • If the crystals are grown upside down in a strong magnetic field, fluid flows that disrupt crystal growth are suppressed.

Rhodopsin

  • green= ligand, always present in receptor
  • In dark, get a kink: 11-cis retinal holds transmembrane regions in the inactive conformation
  • rhodopsin exposure to light, get conformational change in retinal that allows it to become straight, changes the conformation of the receptor
  • Allows the revealing of sites that were not exposed previously
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10
Q

slide 20

A
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11
Q
A
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