Organisms respond to changes in their internal and external environments

Question 1

What is homeostasis

Answer 1

Maintenance of a stable internal environment within restricted limits by physiological control systems

Question 2

High temperature means..

Answer 2

H bonds in tertiary structure break, enzymes denature, active sites change shape and substrates can’t bind, fewer ES complexes

Question 3

Low temperature means..

Answer 3

Not enough kinetic energy, fewer ES complexes

Question 4

Above/below optimal pH means..

Answer 4

Ionic/Hydrogen bonds in tertiary structure break, enzymes denature, active sites change shape and substrates can’t bind, fewer ES complexes

Question 5

Negative feedback systems

Answer 5

-Receptors detect change from optimum
-Effectors respond to counteract change
-Returning levels to optimum

Question 6

Positive feedback systems

Answer 6

-Receptors detect change from normal
-Effectors respond to amplify change
-Producing a greater deviation from normal

Question 7

Glycogenesis converts

Answer 7

glucose→glycogen

Question 8

Glycogenolysis converts

Answer 8

glycogen→glucose

Question 9

Gluconeogenesis converts

Answer 9

amino acids/glycerol→glucose

Question 10

When is insulin secreted

Answer 10

When beta cells in islets of Langerhans in pancreas detect high blood glucose concentration

Question 11

Action of insulin

Answer 11

Attaches to specific receptors on cell surface membranes of target cells→more glucose channel proteins join cell surface membranes→ increases permeability to glucose→ more glucose enters by facilitated diffusion
-Enzymes involved in glycogenesis→ lowers glucose conc in cells → glucose enters cells by facilitated diffusion. down conc gradient

Question 12

When is glucagon secreted

Answer 12

When alpha cells in islets of Langerhans in pancreas detect blood glucose conc is. too low

Question 13

Action of Glucagon

Answer 13

Attaches to specific receptors on cell surface membrane of target cells→activates enzymes involved in glycogenolysis→activates enzymes involved in gluconeogensis

Question 14

When is adrenaline secreted

Answer 14

Fear, stress, exercise

Question 15

Role of Adrenaline

Answer 15

Attaches to specific receptors on cell surface membrane of target cells→activates enzymes involved in glycogenolysis
conc gradient- glucose leaves cells and enters blood by fd

Question 16

Second messenger model- adrenaline and glucagon

Answer 16

First messenger (adrenaline and glucagon) attach to to specific receptors which:
Activate enzymes adenylate cyclase→converts many ATP to many cyclic AMP→cAMP acts as second messenger → activates protein kinase enzymes→activates enzymes for glycogenolysis

Question 17

Advantage of second messenger model

Answer 17

Amplifies signal from hormone as each hormone can stimulate production of many molecules of a second messenger, which can activate many enzymes for rapid increase in glucose

Question 18

Causes of Type 1 Diabetes

Answer 18

-Beta cells in islets of langerhans in pancreas produce insufficient insulin
-Normally develops in childhood due to an autoimmune response destroying beta cells in islets of langerhans

Question 19

Control by insulin-Type 1

Answer 19

Injections of insulin. (not orally as protein is digested)
Blood glucose concentration monitored with biosensors, dose of insulin matches to glucose intake

Question 20

Control by diet manipulation-Type 1

Answer 20

Eating regularly, control carbohydrate intake to avoid sudden rise in glucose

Question 21

Causes of Type 2 Diabetes

Answer 21

Receptor loses responsiveness to insulin, fewer glucose transport proteins, less uptake of glucose, less conversion of glucose to glycogen

Question 22

Control by insulin-Type 2

Answer 22

Not normally treated this way, uses drugs which target insulin receptors to increase their sensitivity- more glucose uptake

Question 23

Control by diet manipulation-Type 2

Answer 23

-Reduced sugar intake, less absorbed
-Reduced fat intake, less glycerol to glucose
-More exercise, uses glucose by respiration
-Weight loss- More sensitivity of receptors to insulin

Question 24

Effects of hypoglycaemia

Answer 24

Not enough glucose for respiration→ less ATP produced→ active transport can’t occur → cell death

Question 25

Effects of hyperglycaemia

Answer 25

Water potential of blood decreases→ water lost from tissue to blood via osmosis→ kidneys can’t absorb all glucose→ more water lost in urine causing dehydration

Question 26

Function of Bowman’s/ renal capsule

Answer 26

Formation of glomerular filtrate

Question 27

Function of proximal convoluted tubule

Answer 27

Reabsorption of water and glucose

Question 28

Function of Loop of Henle

Answer 28

Maintenance of a gradient of sodium ions in the medulla

Question 29

Function of distal convoluted tubule and collecting duct

Answer 29

Reabsorption of water

Question 30

How is glomerular filtrate formed

Answer 30

-High hydrostatic pressure in glomerulus (as the diameter of the afferent arteriole is wider than the efferent arteriole)
-Small substances are forced into glomerular filtrate
-Filtered by:
→pores between capillary endothelial cells
→capillary basement membrane
→podocytes
-Large proteins/blood cells remain in the blood

Question 31

How is glucose reabsorbed by the proximal convoluted tube

Answer 31

-Sodium ions actively transported out of epithelial cells to capillary→moved by facilitated diffusion into epithelial cells down conc. gradient, bringing glucose against its conc gradient → glucose moves into capillary by facilitated diffusion down its conc. gradient

Question 32

How is water reabsorbed by the proximal convoluted tube

Answer 32

Glucose in capillaries lowers water potential, so water moves by osmosis down a water potential gradient

Question 33

In diabetics, why isn’t all glucose reabsorbed

Answer 33

Blood glucose conc too high→ glucose carrier proteins are working at max rate

Question 34

How is a gradient of sodium ions maintained in the medulla by the loop of Henie

Answer 34

Ascending limb: Sodium ions actively transport out (filtrate conc decreases) → water remains as impermeable to water→increases conc of sodium ions in medulla, lowering water potential
Descending limb: Water moves out by osmosis then reabsorbed by capillaries (filtrate conc increases) → sodium ions recycled→ diffuses back in

Question 35

Importance of maintaining a gradient

Answer 35

Increases concentration of sodium ions further down→so water potential decreases down the medulla→water potential gradient maintained between collecting duct and medulla to maximise reabsorption of water by osmosis from filtrate

Question 36

Why do animals needing to conserve water have long loops of Henie

Answer 36

More sodium ions moved out → sodium ion gradient is maintained for longer in. medulla→water potential gradient is maintained for longer and more water can be reabsorbed from collecting duct by osmosis

Question 37

How is water reabsorbed by the distal convoluted tubule and collecting ducts

Answer 37

Water moves out of the distal convoluted tubule and collecting duct by osmosis down a water potential gradient, controlled by ADH which increases their permeability

Question 38

What is osmoregulation

Answer 38

Control of water potential of the blood

Question 39

Function of the hypothalamus

Answer 39

-Contains osmoreceptors- detects blood water potential
-Produces ADH

Question 40

Function of posterior pituitary gland

Answer 40

-Secrete ADH into blood due to signal from hypothalamus

Question 41

Function of antidiuretic hormone (ADH)

Answer 41

-More secreted when blood water potential is low
-Increases permeability of cells of collecting duct and DCT to water→ increases water reabsorption into blood→ decreases volume and increases conc of urine produced

Question 42

How does the body respond to a decrease in water potential

Answer 42

-In the hypothalamus, osmoreceptors detect a decrease in water potential→ produces more ADH
-Posterior pituitary gland secretes more ADH into blood
-ADH attaches to receptors on collecting duct→ increasing permeability of cells to water (aquaporins join cell surface membrane)→so more water reabsorbed from collecting duct by osmosis
-Urine=smaller volume and more concentrated

Question 43

How do organisms increase their chance of survival

Answer 43

They respond to stimuli

Question 44

What is a stimulus

Answer 44

Change in organisms internal or external environment

Question 45

What is tropism

Answer 45

growth of a plant in response to a directional stimulus

Question 46

What is the role of growth factors in flowering plants

Answer 46

Specific factors move from growing regions (root/shoot tips) to other tissues where they regulate growth in response to directional stimuli

Question 47

How does indoleacetic acid affect cell elongation in roots v shoots

Answer 47

In shoots, high conc of IAA stimulate cell elongation
In roots, high conc. of IAA inhibits cell elongation

Question 48

Gravitropism

Answer 48

-Cells in tip of shoot/ root produce IAA
-IAA diffuses down shoot/ root
-IAA moves to lower side of shoot/ root so conc increases
-Shoots bend away from gravity, roots bends towards gravity

Question 49

Phototropism

Answer 49

-Cells in tip of shoot/root produce IAA
-IAA diffuses down shoot/root so conc increases
-In shoots this stimulates cell elongation whereas in roots this inhibits cell elongation
-Shoots bend towards light, roots bend away from light

Question 50

Taxes response

Answer 50

Directional response.
Movement towards or away from stimulus

Question 51

Kineses response

Answer 51

Non directional response.
Speed of movement changes in response to a non directional stimulus.
Intensity is a factor.
E.G. woodlice move faster when drier to raise chance of moving to higher humidity to prevent drying out

Question 52

Protective effect of simple reflex

Answer 52

Stimulus →receptor →sensory neurone →relay neurone →motor neurone →effector →response

Question 53

Importance of protective effect

Answer 53

-Rapid →only 3 neurones and few synapses (synaptic transmission is slow)
-Autonomic so doesn’t have to be learnt by brain
-Protects from harmful stimuli

Question 54

How does deformation of stretch mediated sodium ion channel cause generator potential

Answer 54

-Mechanical stimulus (e.g.high pressure)
-Sodium ion channels in membrane open and sodium ions diffuse into sensory neurone
-Greater pressure causes more sodium ion channels to open and more sodium ions to enter
-Causing depolarisation, leading to generator potential

Question 55

What does the pacinian corpuscle illustrate?

Answer 55

Receptors respond only to specific stimuli- only responds to mechanical pressure.
Stimulation of a receptor leads to the establishment of a generator potential
When threshold is reached, action potential triggered.

Question 56

What are the features of a myelinated motor neurone

Answer 56

-Dendrite
-Axon [myelin sheath (made of Shwann cells), Node of Ranvier in gaps]
-Cell body (soma)
-Axon terminal

Question 57

Establishment of a resting potential

Answer 57

-Na+/K+ pump actively transports
-3 Na+ out of axon
-2 K+ into axon
-This creates an electrochemical gradient
-Differential membrane permeability:
-More permeable to K+, moves out by fd
-Less permeable to Na+ (closed channels)

Question 58

What happens at resting potential

Answer 58

Inside of axon has a negative charge relative to outside, as there are more positive ions outside compared to inside

Question 59

What do changes in permeability lead to

Answer 59

Depolarisation, and the generation of an action potential

Question 60

Stimulus

Answer 60

-Na+ channels open; membrane permeability to Na+ increases
-Na+ diffuse into axon down electrochemical gradient (causing depolarisation)

Question 61

Depolarisation

Answer 61

-If threshold potential is reached, an action potential is generated:
-As more voltage-gated Na+ channels open (positive feedback effect)
-More Na+ diffuses in rapidly

Question 62

Repolarisation

Answer 62

-Voltage-gated Na+ channels close
-Voltage-gated K+ channels open; K+ diffuses out of axon

Question 63

Hyperpolarisation

Answer 63

K+ channels slow to close so there’s a slight overshoot- too many K+ diffuse out

Question 64

Resting potential

Answer 64

Restored by Na+/K+ pump

Question 65

All or nothing principle explained

Answer 65

Depolarisation has to exceed threshold potential, for action potential production. Action potentials are always the same magnitude at same potential

Question 66

Factor that affects action potential

Answer 66

Bigger stimuli increases frequency of action potentials

Question 67

Passage of action potential along non myelinated axon

Answer 67

-Action potential passes as a wave of depolarisation
-Influx of Na+ in one region increases permeability of adjoining region to Na+ by causing voltage-gated Na+ channels to open so adjoining region depolarises

Question 68

Passage of action potential along myelinated axon

Answer 68

-Myelination provides electrical insulation
-Depolarisation of axon at nodes of Ranvier only
-Results in saltatory conduction (local currents circuits)
-No need for depolarisation along whole length of axon

Question 69

What happens if the myelin sheath is damaged

Answer 69

Slow responses/jerky movement

Question 70

What Is an action potential

Answer 70

When the neuron’s voltage increases beyond a set point from the resting potential (-70mV) , generating nervous impulse

Question 71

What causes increases in voltage aka depolarisation

Answer 71

Neurone membrane becomes more permeable to sodium ions

Question 72

Nature and Importance of the refractory period

Answer 72

Ion channels are recovering and don’t open, so there’s a time delay between action potentials ∴ :
-Actions potentials don’t overlap, but pass along as separate impulses
-There’s a limit to the frequency at which nerve impulses are transmitted
-Action potentials are unidirectional (only travel in one direction)

Question 73

How does axon diameter affect speed of conductance

Answer 73

Bigger diameter so less leakage of ions, less resistance to flow of ions

Question 74

How does temperature affect speed of conductance

Answer 74

-Increases rate of movement of ions as more kinetic energy
-Higher rate of respiration due to faster enzyme activity, ATP produced faster and energy released faster (because active transport is faster)
*PROTEINS CAN DENATURE AT V HIGH TEMPS

Question 75

Where are rods and cones found

Answer 75

retina

Question 76

Rods

Answer 76

More sensitive to light
-Several rods connected to a single neurone
-Spatial summation to reach threshold to generate action potential
Lower visual acuity
-Several rods connected to a single neurone, so they send a single set of impulses to brain (brain can’t distinguish between separate sources of light)
Allow monochromatic vision
-1 rod (1 pigment)

Question 77

Cones

Answer 77

Less sensitive to light
-Each cone is connected to a single neurone
-No spatial summation
Cones give higher visual acuity
-Each cone connected to a single neurone
-Cones send separate sets of impulses to brain so it can distinguish between separate sources of light
Cones allow colour vision
-3 types of cones (red, green, blue) with different optical pigments (so absorb different wavelengths
-Stimulation of different combinations of cones gives a range of colour perception

Question 78

What does myogenic mean (cardiac muscle is myogenic)

Answer 78

Can contract/relax without receiving electrical impulses from nerves

Question 79

Role of the sinoatrial node

Answer 79

Acts as a pacemaker and sends out regular waves of electrical impulses across both atria causing right/left atria to contract simultaneously
Waves of electrical activity reaches atrioventricular node

Question 80

What prevents waves crossing directly to ventricles

Answer 80

Layer of non conductive tissue

Question 81

Where are chemoreceptors and baroreceptors located

Answer 81

In aorta and cartoid arteries

Question 81

Role of atrioventricular node

Answer 81

Delays impulse allowing atria to fully contact and empty
Passes waves of electrical activity to ‘bundle of His’ which conducts wave between ventricles to the apex of the heart, where the bundle branches into smaller fibres of Purkyne tissue

Question 82

How are baroreceptors stimulated by low blood pressure

Answer 82

More frequent impulses to medulla, more frequent impulses sent to SAN along sympathetic neurones, more frequent impulses sent from SAN, cardiac muscle contracts more frequently so heart rate increases

Question 83

How are baroreceptors stimulated by high blood pressure

Answer 83

More frequent impulses to medulla, more frequent impulses sent to SAN along parasympathetic neurones, less frequent impulses sent from SAN, cardiac muscle contracts less frequently so heart rate decreases

Question 84

How are chemoreceptors stimulated by high blood CO2 conc/ low pH

Answer 84

More frequent impulses to medulla, more frequent impulses sent to SAN along sympathetic neurones, more frequent impulses sent from SAN, cardiac muscle contracts more frequently so heart rate increases

Question 85

How are chemoreceptors stimulated by low blood CO2 conc/ high pH

Answer 85

More frequent impulses to medulla, more frequent impulses sent to SAN along parasympathetic neurones, less frequent impulses sent from SAN, cardiac muscle contracts less frequently so heart rate decreases

Question 86

What happens when action potential reaches the end of a neurone

Answer 86

Neurotransmitters (which are contained in synaptic vesicles in the synaptic knob of the presynaptic neurone) are released into the synaptic cleft. They diffuse across to the postsynaptic membrane and bind to specific receptors.
*Neurotransmitters will either be broken down by enzymes or taken back not presynaptic neurone so response doesn’t keep happening.

Question 86

What’s a synapse and synaptic cleft

Answer 86

Synapse- junction between a neurone and another neurone/an effector cell
Synaptic cleft- Tiny gaps between cells at a synapse

Question 86

What happens when neurotransmitters bind to specific receptors

Answer 86

They might trigger an action potential, cause muscles contraction, or cause hormone to be secreted.

Question 87

How is a nerve impulse transmitted across a cholinergic synapse

Answer 87

-An action potential arrives at the synaptic knob of the presynaptic neurone
-This stimulates voltage-gated calcium ion channels in the presynaptic neurone to open
-Calcium ions diffuse into the synaptic knob
-The influx of calcium ions cause the synaptic vesicles to move to the presynaptic membrane, they then fuse with the membrane
-The vesicles release the neurotransmitter acetylcholine into the synaptic cleft (exocytosis)
-Acetylcholine diffuses across the synaptic cleft and binds to specific cholinergic receptors on postsynaptic membrane
-Causes sodium ion channels in the postsynaptic neurone to open
-Influx of sodium ions into the postsynaptic membrane causes depolarisation, action potential
generated if threshold is reached
-Acetylcholine is removed from the synaptic cleft so the response doesn’t keep happening, broken down by acetylcholinesterase and the products are reabsorbed by presynaptic neurone and used to make more acetylcholine

Question 87

Why are the impulses unidirectional

Answer 87

Because the receptors are only on the post synaptic membrane , impulses can only travel in one direction

Question 88

Cholinergic synapses v neuromuscular junctions

Answer 88

-Cholinergic synapses; neurone to neurone whereas neuromuscular; neurone to muscle
-Neuromuscular; acetylcholine is always excitatory and never inhibitory, so always triggers action potential
-Neuromuscular junction; post synaptic membrane has more receptors than other synapses.
-Neuromuscular junction; lots of folds on post synaptic membrane which. forms clefts to store enzyme (acetylcholinerase) to break down neurotransmitter

Question 89

Excitatory neurotransmitters

Answer 89

Depolarise the postsynaptic membrane, making it fire an action potential when threshold is reached

Question 90

Inhibitory neurotransmitters

Answer 90

Hyperpolarise the postsynaptic membrane (making pd more negative), preventing it from fitting an action potential

Question 91

Where are neuromuscular junctions

Answer 91

-Synapse between motor neurone and a muscle cell

Question 92

What is summation

Answer 92

Addition of a number of impulses converging on a single post-synaptic neurone

Question 92

Spatial summation

Answer 92

Many presynaptic neurones share the same synaptic cleft/ post synaptic neurone, and release sufficient neurotransmitters to reach threshold and trigger an action potential

Question 93

Temporal summation

Answer 93

One presynaptic neurone releases neurotransmitter many times over a short period. Sufficient neurotransmitter to reach threshold to trigger an action potential

Question 94

How do muscles work and where are they

Answer 94

In antagonistic pairs:
-One contracts (agonist); pulls on bone produces a force
-One relaxes (antagonist)
e.g. biceps and triceps
-Attached to bones by tendons
-Ligaments attached from one bone to the other to hold them together

Question 95

What are advantages of skeletal muscle being arranged in antagonistic pairs

Answer 95

-Muscles can only contract
-2nd muscles required to reverse movement caused by 1st
-Helps maintain posture

Question 96

Gross structure of skeletal muscle

Answer 96

Muscle made up of bundles of muscle fibres (muscle cells) packages together
Muscle cells contain;
-Cell membrane=sarcolemma
-Cytoplasm=sarcoplasm
-Myofibrils made up of actin and myosin
-Shared nuclei
-Lots of endoplasmic reticulum

Question 97

Ultrastructure of a myofibril

Answer 97

-Made up many sarcomeres which are made up of partly overlapping myosin (thick, dark A bands ) and actin (thin, light I bands) filaments (proteins)
-A sarcomere contains;
-Ends (z line)
-Middle (A band) and overlap
-H zone (only contains myosin), middle (no overlap)
-M line in the middle

Question 98

Muscle contraction- Sliding filament theory

Answer 98

Myosin and actin filaments slide over each other to make sarcomeres contract.
Simultaneous contractions of sarcomeres cause myofibrils and. muscle fibres to contact.
During contraction:
-H zones get shorter
-I (isotropic) bands get shorter
-A (anisotropic) bands stay the same
-Z lines get closer

Question 99

Why can myosin filaments move back and forth and what binding sites do they have

Answer 99

Myosin filament have globular heads and are unhinged
Each myosin head has a binding site for actin and a binding site for ATP

Question 100

Structure of actin filaments

Answer 100

Actin filaments have binding sites for myosin heads, called action-myosin binding sites
Tropomyosin is found between actin filaments, this helps myofilaments move past each other

Question 101

Why cant myofilaments slide pass each other in resting muscles

Answer 101

The actin myosin binding side is blocked by tropomyosin, so the myosin heads can’t bind to the actin myosin binding site on the actin filaments

Question 102

Name 3 types of muscles in the body and where they are located

Answer 102

Cardiac; exclusively found in heart
Smooth; walls of blood vessels and intestines
Skeletal; attached to incompressible skeleton attached by tendons

Question 103

How is muscle contraction stimulated

Answer 103

-Action potential from a motor neurone. stimulates a muscle cell, depolarises sarcomella
-Depolarisation spreads down the T-tubules to the sarcoplasmic reticulum
-Sarcoplasmic reticulum releases Ca2+ into sarcoplasm
-Ca2+ binds to a protein attached to tropomyosin, causing the protein to change shape
-Attached tropomyosin is pulled out of actin-myosin binding site on actin filament
-Exposes binding site, allows myosin head to bind (actin-myosin cross bridge forms)
-Ca2+ activated ATP hydrolase (hydrolyses ATP) to provide energy for contraction
-Energy released from ATP causes myosin head to bend, which pulls the actin filament in a rowing action
-Another ATP. provides energy to break actin-myosin cross bridge, so myosin head detaches from the actin filament after its moved
-Myosin head reattaches to a different binding site further along the actin filament and process is repeated
-Many actin-myosin cross bridges form and break, pulling the actin filament along- shortens sarcomere, contracts muscle
-Cycle continues as long as Ca2+is present.

Question 104

What happens when Ca2+ leave their binding sites

Answer 104

-Ca2+ moved by active transport back into the sarcoplasmic reticulum (need ATP)
-Causes tropomyosin molecules to move back and block actin myosin binding sites
-Muscles don’t contract as no myosin heads are attached to actin filaments ( no cross bridges)
-Actin filaments slide back to relaxed position, sarcomere lengthens

Question 105

How does aerobic respiration produce ATP for muscle reactions

Answer 105

-ATP generated via oxidative phosphorylation in the cells mitochondria
-Aerobic respirations works when there’s oxygen so its good for low intensity exercise

Question 106

How does anaerobic respiration produce ATP for muscle contraction

Answer 106

-ATP made by glycolysis
-Produces pyruvate which is converted to lactate by lactate fermentation
-Lactate quickly builds up causing muscle fatigue
-Anaerobic is good for short intense exercise

Question 107

How does ATP phosphocreatine produce ATP for muscle contraction

Answer 107

-ATP made by phosphorylating ADP
-PCr stored in cells and ATP-PCr system generates ATP rapidly
-PCr runs out after seconds so its used during short intense exercise
-ATP-PCr system is anaerobic and. doesn’t form lactate (alactic)

Question 108

Slow twitch muscle fibres

Answer 108

-Contract slowly
-Used for posture
-Good for endurance activities
-Works for a long time without getting tired
-Energy released slowly through aerobic respiration, lots of mitochondria and blood vessels supply muscles with oxygen
-Reddish in colour as they’re rich in myoglobin (red colour protein that stores oxygen)