1-14 Membranes and Microscopy

Question 1

What are the five major functions of biological membranes, and why are they important?

Answer 1

1. Selective permeability: control what enters and exits cells/organelles
2. Compartmentalization: organelles can have wildly different chemical environments and functions
3. Identification: unique identity of cells/organelles based on membrane units/conents
4. Signaling: transmembrane signaling transduction acts as “sentry system”; learn about external environments without having to expose the cell to them
5. Energy storage: membrane gradients can act to store energy

Disruption of function can lead to disease.

Question 2

What are the common features of biological membranes?

Answer 2

• Composition: lipids, proteins, carbohydrates
• Structure: asymmetric, sheet-like bilayers that can form closed compartments
• Held together by noncovalent interactions
• Fluid under physiological conditions
• Relatively impermeable to polar, hydrophilic molecules
• Most specific functions carried out by membrane proteins

Question 3

What are the primary properties of lipids in biological membranes?

Answer 3

• Amphipathic
• Mostly phospholipids: polar head group + backbone + nonpolar hydrocarbon tail

Question 4

What are the hydrophobic and hydrophilic parts of phosphoglycerides?

Answer 4

Hydrophobic: fatty acid chain

Hydrophilic: phosphorylated alcohol

Question 5

What are the hydrophobic and hydrophilic parts of sphingomyelin?

Answer 5

Hydrophobic: fatty acid chain and hydrocarbon chain of sphingosine

Hydrophilic: phosphoryl choline

Question 6

What are the hydrophobic and hydrophilic parts of glycolipids?

Answer 6

Hydrophobic: fatty acid chain and hydrocarbon chain of sphingosine

Hydrophilic: One or more sugars

Question 7

What are the hydrophobic and hydrophilic parts of cholesterol?

Answer 7

Hydrophobic: everything except -OH

Hydrophilic: -OH group

Question 8

How do membrane lipids act in aqueous solution?

Answer 8

They will aggregate and bury their hydrophobic tails while exposing their hydrophilic heads. They can form either spherical micelles or bilayers.

Due to the prevalence of phospholipids, most membrane lipids will preferentially form bilayers.

Question 9

What is the most energetically favorable shape for lipid bilayers in aqueous solution, and why?

Answer 9

Lipid bilayers will spontaneously close on themselves to form closed vesicles, thereby shielding hydrophobic regions and exposing hydrophilic regions as much as possible.

This phenomenon is primarily driven by the hydrophobic effect, but it’s also supported by van der Waals forces (close packing of hydrocarbon tails) and interactions between polar head groups and water (electrostatic and H bonding).

Question 10

What are the typical movements of bilayer lipids?

Answer 10

• Lateral diffusion
• Flexion
• Rotation

RARELY, lipids will flipflop between layers. This is typically mediated by proteins.

Question 11

What factors influence the fluidity of membranes?

Answer 11

• Temperature: at physiological temp., membranes are disordered and fluid. Below phys. temp., they are ordered and gel-like.
• Length and degree of saturation: long, saturated HC chains interact more strongly due to van der Waals interactions. In unsaturated chains, double bonds produce kinks that prevent tight packing and allow for more fluidity.
• Cholesterol content: tends to decrease fluidity because it blocks large motions of saturated HC chains; however, it also can prevent membranes from solidifying to gel phase because it prevents nearby fatty acyl chains from packing too tightly.

Question 12

What are lipid rafts?

Answer 12

Membrane subdomains that tend to be thicker, be less fluid, and contain higher content of sphingolipids (sphingomyelin and glycolipids), cholesterol, and some proteins. They float within the bilayer and are thought to help aggregate membrane proteins for transport and/or assembly.

Question 13

Why are lipid bilayers asymmetric?

Answer 13

Outer half: mostly phosphotidylcholine, sphingomyelin, glycolipids
Inner half: mostly phosphotidylserine and phophotidylethanolamine
(cholesterol is distributed evenly)

The asymmetry is important for cell signaling across the membrane and identification of live/dead cells.

ex) Phosphatidylserine moves inner half –> outer half during apoptosis, signaling for phagocytosis.

Question 14

What determines a molecule’s ability to pass through a lipid bilayer?

Answer 14

• Polarity: nonpolar molecules can cross easily; polar molecules cannot
• Size: small molecules will cross more easily than large ones

Aquaporins will allow water molecules to pass more easily.

Question 15

How do drugs get into cells, and what are the drawbacks?

Answer 15

• Passive diffusion: drug is hydrophobic enough to pass through the bilayer but hydrophilic enough for easy distribution. Cons: structurally limiting
• Hijacked transporters: drug looks like some other molecule that is normally transported by membrane transport proteins. Cons: structually limiting (but manipulatable)
• Liposome delivery: drug is packaged in liposomes and targets cells with a membrane protein tag. Cons: difficult to control, inefficient, liposome contents not always released easily
• Protein transduction: drug is coupled to and taken up by protein sequences that interact directly with the bilayer. Cons: new, not used therapeutically

Question 16

What are the general properties of membrane proteins?

Answer 16

• Allow selective permeability to polar substances
• Carry out most of the membrane’s specific functions
• Classification as either peripheral or integral
• Ability to diffuse laterally (unless contained)

Question 17

What is the difference between integral and peripheral membrane proteins?

Answer 17

Integral membrane proteins penetrate the lipid bilayer and require detergents to be released.

Peripheral membrane proteins bind to either the membrane surface or integral membrane proteins. They can be released without disrupting the bilayer.

Question 18

What are two important properties of integral membrane proteins?

Answer 18

1. Amphipathy: hydrophobic areas interact directly with lipids; hydrophilic areas interact with polar head groups and the aqueous environment.
2. Defined topology: once fixed in the membrane, topology is fixed, too (no flip-flopping).

Question 19

How can the lateral diffusion of membrane proteins be constrained?

Answer 19

• *A)** Anchoring the protein to an intracellular structure, like the cytoskeleton
• *B)** Anchoring the protein to an extracellular structure, like the ECM
• *C)** Protein-protein interactions between cells, like neurological synapses
• *D)** Barriers established by junction proteins

Question 20

What is the fluid mosaic model?

Answer 20

The lipid bilayer acts as the solvent for membrane proteins, which can diffuse laterally but cannot flip-flop.

Question 21

Where are membrane lipids produced?

Answer 21

In the endoplasmic reticulum.

Question 22

How are phospholipids produced in and later released from the endoplasmic reticulum?

Answer 22

• In the cytosolic half of the ER, new phospholipids are both synthesized by enzymes from free fatty acids and inserted into the bilayer.
• Scramblases randomly and evenly redistribute phospholipids between the monolayers.
• Vesicles deliver lipids from the ER to the Golgi, lysosomes, endosomes, and plasma membrane.
• Flippases in the Golgi and plasma membrane specifically and asymmetrically relocate phospholipids from one monolayer to the other.

Question 23

How and why are newly synthesized lipids transferred to peroxisomes and mitochondria?

Answer 23

Peroxisomes and mitochondria do not participate in vesicular transport, therefore cytosolic lipid carrier proteins transfer lipids to them.