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Biological Membranes - Biochemistry

Why are biological membranes important

25% of the genes in the human genome are for membrane proteins
They are important as they dictate how cell will interact with the environement

60% of marketed drugs target membrane proteins

Where are membranes found

All cells are enveloped by a plamsa menbrane and some internal organelle are also membrane bound like mitochondria and chloroplasts

How can you see membranes under a light microscope

They have to be stained with antiboides due to usually imvidble under a light micropscope but can be seen by electron microscopes

What does a hetergenerous structure mean

This means membranes are highly dynamic assemblies that is composed of mainly lipids and proteins
The proprotion of both is highly dependent on the function of the cell or organelle

What are the 3 major classes of lipids

Phospholipids
Cholesterol

Sphingolipids

What is the structure of a phosopholipid

Made up of a glycerol backbone withg 2 fatty acids chains bonded to it along then with a phosphate group that contains an alcohol- OH bonded to it on the end
The phosphate in the SN3 and the fatty acids on SN1 + 2 and the headgroup is attched to the phosphate

What are Sphingolipids

They are the main component of neuronal membranes and are primarily found in the plasma membrane
They can cause different behaviours in membrane due to fcorming local domains

They dont contain a glycerol backbone

Rather than an OH group bonded to a phosphate there is a N+ molecule

What are sterols

They have a hydroxyl group that CO group of a phospholipid and has a long axis that run parrallel to the membrane in order to help provide the membrane structural rigidity

What are the physicall properties of lipids

They have a hydrophillic head and hydrophobic fatty acid tails so overall are amphipathic

What happens to lipids in an aqueous solution

In an aqueous solution the lipids will form bilayers, this is due to trying minimise the delta G of the system
Hydrophillic intercation from the head intercat with the aqueous environment and the hydrophobic tails try to intercat with other hydrophobic sites, lead to the formation of a membrane biliater with the tails pointing in away from the water and the heads = facing out towards the water

This lead to formation of vesicles

What is the liquid crystalline state

Due to lipids have large acetyl chain mainly of cis-double bonds, this will prevent the close packing of acyl chain meaning then a bilayer with mobile acyl chain
In this phase the lioids move around in the plane of the bilayer at biological temperatures

What is lateral diffusion in the membrane

This allow rapid movement of molecules in the plane of the bilayer and occur rapidly with the neighbour

What is lipid flip-flop

This is unfavourable energetically and takes very long time, and is where 2 lipids that are opposite each other in the bilayer will swap sides of the bilayer that they are on, this can be done due enzymes called flippases and will preserve asymmetry in the bilayer

Why is membrane fluidity impirtant

At low temp the liquid crystalline lipid turns inot a gel phase with frozen acyl chain
Liquid crystalline is essential for fucntion of membrane proteins that need a fluid environment

Molecules need to move in the membrane to carry substrates between enzymes and start signalling events

Whar are the conformationla change in membrane proteins

Lipids based on glcyerol or sphingosine and sterols form major component of biological membranes
Others form bilayers within water due to the hydrophobic effect

All biological membranes are in liquid -crystalline phase

What are the major proteins that are in cell membranes

Protein channels
Transportters

Receptors

Structural proteins

Why are proteins important in the membrane

This is due to provide route for polar and larger molecules to cross the membrane as well as info carried by polar signalling molecules

Why do transmembranous proteins have an alpha helix shape

Channels, receptor and transporters all span the whole way across the membrane in an a-helix stucture to allow them to cross over the hydrophobic membrane core

What do transmembranous proteins do

They transmembrane helices anchor the membrane proteins
This is due to the protein sequence being hydrophobic in the transmembrane domain

The R groups project outwards to face the lipids to ensure that the protein is being anchored in the lipid bilayer

How is a path created over the whole membrane

Multiple amphipathic helices are able to cluster together in order to produce a polarv route across the bilayer
You need at least 4 amphipathic helices for this to be created

What do polar channels over the bilayer control

They are able to control the passive diffusion of ions over the membrane, this is because the channles have charged residues on the outisde of the channel so then control what type of ions can enter the channel
Also the diameter controls the ions size that can enter the channel and channel roation to bring R groups to the channle to prevent ion movement

What do transporters do

Used if need to pump the solute then use SYP hydrolysis or by a co-transportter of another ions that is being moved down a electrochemical gradient
There is no pumping used for transporter

How do ion gated channels work

Where have a + gate on the ion channel that is controlled by the R group of amino acids making up the gate so then only negtayive ions are able to pass through the channel and voce versa

How to fully close the channel

If there is a rearrangement of the helices in the channle so that there is no hole in the bilayer so then no passage of molecules due to closed channels

What are ligand gated ion channels

These are involved in nueorne transmission in the body
In the open state serine is facing towards the middle and larger leucine facing awat so a channel is created but when closed the larger leucine are projected to the middle so then no channel due to closed

What can channels not do

They cant move ion or any solute against their concentration gradient via pump or active transport
Unsuitbale for faciliatted diffusion of larger molecules like glucose or amino acids

What are the 2 types of transporters

Passive - Molecules move down the concentration gradient
Actove- Molecules move against their concentration gradient and so energy is needed from ATP hydrolysis

How do transporters work

They have 2 gates
where first 1 is opend to allow access to recognition site for the solute to be transported

This binding causes the other gate to open and the first gate to then close due to a confromational change to allow new gate to open and close the first one

What is the atomic resolution structure of the calcium ion pump

There is 10 alpha helices cross the bilayer to form the strucutre for 2Ca2+ ions to be transported across the bilayer
There is a binding site for ATP to provide energy for calcium transport

Why us calcium ion movement important

Needed in muscles to trigger contraction and to rapidly relax the muscles when Ca2+ ion removed
Also needed in synapses

Why is it hard for atomic resolution structure of membrane proteins to be made

Membrane proteins dont readily form 3D crystals and very few structures are resolved for crystallography and they are too large for liquid state NMR

What are problems caused from atomic resolution of membrane proteins

Limoted number of membrane proteins needed for function to take place, sio then limited number for crystallisation studies
Over expression of their genes doesnt work so always limited protein to study

Hard to remove 2d anchored protein without changing composition

Why is protein expression a challenge for studying proteins

For early structures easy due to high protein natural abundance their and are colourful
For smaller proteins like receptors harder due to expressed heterologously in bacteria that lack the post translational machinaery for effcient membrane protein expression so low abundnace

Why it hard to purify the and solubilize the proteins to study

Have to break down lipod bilayer by small detergent addition to remove the protein from membrane
Have to purify the protein but large amount end up denatured so hard to get large enough yield to study

Why is structural analysis of proteins hard

Cant do Xray cyrstallography due to hard to make crystals
Electron microscope have low resolution

NMR in solution need a micellar system and in soli9d state need the protein in a bilayer

How can indirect techniques be used to analyse membrane proteins

Sequence analysis can find potential transmembrane helices byt hard to fidn amphipathic helices
Can also use the location of the post translational modifications

Use labelling methods to find exposed extternal residues and hydrophobic reagent to determine transmembrane residues

What is a hydropathy plot

Each amino acid is assigned a value based on hydrophobicity
Average length or transmembrane helix is 20 a.a

Computer algorithm calcualte and plot hydrophobicity or residues to reveal the potential transmembrane helices

Can be used to determine the protein orientation due to - charge face inwards and + outwards of the bilayer

What us genomic analysis

Good tool for identyfying protein families
Families can be found due to function is reflected in the environment that the cell is in

What are B barrell structures

A less common bilayer spanning structure that form hydrophobic pores in the outer membrane of bacteria and mitochondria
In mitochondria only allow to pass molecules needed for ATP production, that are then transported across the inner membrane

In bacteria carry nutrienst like maltose and phosphate to pass through, they are too leaky for general membranes to use

What is a sucrose specific porin

Porin allows the direct diffusion of sucrose across the outer membrane of bacterium Typhimuriium and is pore is made of 16 B strands of proteins

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