unit 2 Cells

Question 1

Eukaryotic (eg human) cells compared with Prokaryotic (bacterium) (7)

Answer 1

1. Bacterial cell is much smaller than a human cell; (or human cell is much larger than a bacterial cell)
2. Bacterial cell has a cell wall but human cell does not;
3. Bacterial cell lacks a nucleus but human cell has a nucleus;
4. Bacterial cell lacks membrane-bound organelles but human cell has membrane-bound organelles;
5. Bacterial ribosomes smaller than human ribosomes / bacteria have 70S ribosomes whereas humans have 80S
6. Bacterial DNA is circular but human DNA is linear
7. Bacterial DNA is ‘naked’ whereas human DNA is bound to histones/proteins

Question 2

Eukaryotic - Describe the structure and function of the nucleus.(4)

Answer 2

Any four from Structure
Nuclear envelope/double membrane
(Nuclear) pores (in the membrane)
Chromosomes/chromatin/(linear) DNA with histones
Nucleolus/nucleoli

Function
Holds/stores genetic information for production of proteins
DNA replication OR interphase
Production of mRNA/tRNA OR transcription
Production of rRNA/ribosomes

Question 3

Eukaryotic - Name the main polymer that forms the following cell walls – plants cells & fungal cells (1)

Answer 3

Cellulose (plant) and

chitin (fungi)

Question 4

Eukaryotic - Describe the role of one named organelle in digesting these bacteria. (3)

Answer 4

1. Lysosomes;
2. Fuse with vesicle;
   Accept phagosome for vesicle
3. (Releases) hydrolytic enzymes;

Question 5

Eukaryotic - Identify two organelles in cells that enable the production of glycoproteins (1)

Answer 5

Rough endoplasmic reticulum/ribosomes and Golgi (apparatus/vesicles)

Question 6

Eukaryotic - Give two structures found in all prokaryotic cells and in all eukaryotic cells. (2)

Answer 6

1. Cell(-surface) membrane;
2. Ribosomes;
   Ignore 70S
3. Cytoplasm;
4. DNA;

Question 7

Eukaryotic – Give one feature of the chloroplast that allows protein to be synthesised inside the chloroplast and describe one difference between this feature in the chloroplast and a eukaryotic cell. (2)

Answer 7

Mark in pairs, 1 and 2 OR 3 and 4
1. DNA;
2. Is not associated with protein/histones but nuclear DNA is
OR
Is circular but nuclear DNA is linear
OR
Is shorter than nuclear DNA;

3. Ribosomes;
4. Are smaller than cytoplasmic ribosomes;

Question 8

Eukaryotic - Eukaryotic cells produce and release proteins.
Outline the role of organelles in the production, transport and release of proteins from eukaryotic cells.(4)

Answer 8

1. DNA in nucleus is code (for protein)
2. Ribosomes/rough endoplasmic reticulum produce (protein);
   Accept rER for ‘rough endoplasmic reticulum’
3. Mitochondria produce ATP (for protein synthesis);
4. Golgi apparatus package/modify;
   OR
   Carbohydrate added/glycoprotein produced by Golgi apparatus;
   Accept body for ‘apparatus’
5. Vesicles transport
   OR
   Rough endoplasmic reticulum transports;
6. (Vesicles) fuse with cell(-surface) membrane;

Question 9

Eukaryotic – state three differences between DNA in the nucleus of a plant cell and DNA in a prokaryotic cell.(3)

Answer 9

Plant v prokaryote
1. (Associated with) histones/proteins v no histones/proteins;
2. Linear v circular;
3. No plasmids v plasmids;
Do not credit if suggestion that prokaryotic DNA only exists as plasmids.
4. Introns v no introns;
5. Long(er) v short(er);

Question 10

Eukaryotic – Name the main biological molecule in the cell membrane (1)

Answer 10

Phospholipids

Question 11

Eukaryotic – Describe the role of mitochondria in secreting a protein (1)

Answer 11

(Many mitochondria) release energy / ATP for movement of vesicles / synthesis of protein / active transport;

Question 12

Eukaryotic – Describe the role of golgi apparatus in secreting a protein (1)

Answer 12

(Many Golgi) vesicles transport protein / glycoprotein / milk to cell membrane / out of cell;

Question 13

Eukaryotic – Descirbe the role of the golgi apparatus in lipid absorption

Answer 13

1. Modifies / processes triglycerides;
2. Combines triglycerides with proteins;
3. Packaged for release / exocytosis
   OR
   Forms vesicles;

Question 14

Prokaryotic - Name the main biological molecule in a bacterial cell wall (1)

Answer 14

Murein / glycoprotein;

Question 15

Prokaryotic - Give two features of all prokaryotic cells that are not features of eukaryotic cells.

Answer 15

Cytoplasm with no membrane-bound organelles
Single, Circular DNA
DNA free in the cytoplasm
DNA that is not associated with proteins/histones
A cell wall that contains murein

Question 16

Viruses – Give 2 features of all viruses (2)

Answer 16

1. attachments proteins
2. capsid
3. nucleic acid

Question 17

Microscopes - How to measure objects using an eyepiece graticule (3)

Answer 17

1. Use eyepiece graticule to measure the object e.g. nucleus or capillary
2. Calibrate eyepiece graticule against stage micrometer
3. Take a number of measurements and calculate the mean

Question 18

Microscopes - Advantages and Limitations of Transmission Electron Microscope (TEM) (6)

Answer 18

Advantages:
1. Small objects can be seen;
2. TEM has high resolution as wavelength of electrons shorter;

Limitations:
1. Cannot look at living cells as cells must be in a vacuum;
2. Must be thin specimen;
3. Preparation may create artefact;
4. Does not produce colour image

Question 19

Microscopes - Comparison of TEM and optical microscope (8)

Answer 19

1. TEM use electrons and optical use light;
2. TEM allows a greater resolution;
3. (So with TEM) smaller organelles/named cell structure can be observed
4. TEM view only dead/dehydrated specimens and optical (can) view live specimens;
5. TEM does not show colour and optical (can);
6. TEM requires thinner specimens;
7. TEM requires a more complex/time consuming preparation;
8. TEM focuses using magnets and optical uses (glass) lenses;

Question 20

Microscopes – Advantage of electron microscope over optical microscope (2)

Answer 20

1. High resolution;
2. Can see internal structure of organelles

Question 21

Microscopes - The resolution of an image obtained using an electron microscope is higher than the resolution of an image obtained using an optical microscope.
Explain why. (2)

Answer 21

Shorter wavelength between electrons;
OR
Longer wavelength in light rays;

Question 22

Microscopes - Describe and explain one difference between TEM and SEM (2)

Answer 22

1. 3D image (with SEM), not 2D image
   OR
   Lower resolution (with SEM)
   OR
   (Only) surface visible with SEM, but internal structures visible with TEM;
2. (Because) electrons deflected/bounce off (using SEM)
   OR
   Electrons transmitted/pass through (using TEM);

Question 23

Homogenisation – Conditions required for cell homogenisation (3)

Answer 23

1. Ice-cold – Slows/stops enzyme activity to prevent digestion of organelles/mitochondria;
2. Buffered – Maintains pH so that enzymes/proteins are not denatured;
3. Same water potential – Prevents osmosis so no lysis/shrinkage of organelles/mitochondria;

Question 24

Homogenisation & Ultracentrifugation – How to separate mitochondria? (4)

Answer 24

1. Break open cells/homogenise/produce homogenate;
2. Remove unbroken cells/larger debris by filtration;
3. Centrifuge highest density organelle nuclei obtained as pellet at slowest speed
4. Mitochondria in 2nd pellet as less dense than nucleus/organelle in first pellet;

Question 25

Suggest why scientists can use detergent to break open cells instead of homogenisation (2)

Answer 25

1. Cell membranes made from phospholipid;
2. (Detergent) dissolves membranes / phospholipid (bilayer);

Question 26

Viruses - Describe viral replication.(4)

Answer 26

1. Attachment proteins attach to receptors;
   For ‘attachment protein’ accept gp41/gp120/ glycoprotein but ignore ‘receptor protein’.
2. Virus injects nucleic acid (into host cell);
   For this mp accept ‘genetic material’ for ‘nucleic acid’?
3. Host cell replicates viral nucleic acid;
   Accept ‘RNA/DNA’ for ‘nucleic acid’.
4. Host cell produces (viral) protein/capsid/enzymes;
5. Virus (particles) assembled and released (from cell);

Question 27

Bacteria - Describe binary fission in bacteria. (3)

Answer 27

1. Replication of (circular) DNA;
   Accept nucleoid
   Reject chromosome
   Reject mitosis
2. Replication of plasmids;
3. Division of cytoplasm (to produce daughter cells);

Question 28

Bacteria -Describe how bacteria divide.(2)

Answer 28

1. Binary fission;
2. Replication of (circular) DNA;
3. Division of cytoplasm to produce 2 daughter cells;
4. Each with single copy of (circular) DNA;

Question 29

Eukaryotic division - What is a tumour? (2)

Answer 29

1. Mass of cells;
   Accept abnormal growth for ‘mass’
2. Many cells in mitosis/dividing cells
   OR
   Uncontrolled cell division;

Question 30

Eukaryotic division - Describe and explain the arrangement of the genetic material in prophase (2)

Answer 30

1. Chromosomes (are) becoming visible/distinct;
2. Because (still) condensing;
   OR
   Accept ‘chromosomes are condensed’ for 2 marks.
   Accept shorten or thicken for ‘condensed’
3. Chromosomes (arranged) at random/not lined up;
4. Because no spindle (activity);
   OR
   Because not attached to spindle fibres;

Question 31

Eukaryotic division - Chromosome Behaviour in all Stages (8)

Answer 31

(During prophase)
1. Chromosomes coil/condense/shorten/thicken/become visible;
2. (Chromosomes) appear as (two sister) chromatids joined at the centromere;

(During metaphase)
3. Chromosomes line up on the equator/centre of the cell;
4. (Chromosomes) attached to spindle fibres;
5. By their centromere;

(During anaphase)
6. The centromere splits/divides;
7. (Sister) chromatids/chromosomes are pulled to opposite poles/ends of the cell/separate;

(During telophase)
8. Chromatids/chromosomes uncoil/unwind/become longer/thinner;

Question 32

Eukaryotic division - Describe the role of the spindle fibres and the behaviour of the chromosomes during mitosis (5)

Answer 32

1. (In) prophase, chromosomes condense;
   Accept chromatin for ‘chromosomes’ and for ‘condense’, shorten and thicken
2. (In) prophase OR metaphase, centromeres attach to spindle fibres;
3. (In) metaphase, chromosomes/pairs of chromatids at equator/centre of spindle/cell;
4. (In) anaphase, centromeres divide;
5. (In) anaphase, chromatids (from each pair) pulled to (opposite) poles/ends (of cell);
   Accept for ‘chromatids’, chromosomes but reject homologous chromosomes
6. (In) prophase/metaphase/anaphase, spindle fibres shorten;

Question 33

Eukaryotic division – state name given to the division of cytoplasm during the cell cycle. (1)

Answer 33

cytokinesis

Question 34

Eukaryotic division - Give two pieces of evidence that the cell was undergoing mitosis (2)

Answer 34

1. The (individual) chromosomes are visible because they have condensed;
2. (Each) chromosome is made up of two chromatids because DNA has replicated;
3. The chromosomes are not arranged in homologous pairs, which they would be if it was meiosis;

Question 35

Eukaryotic division – Evidence for a cell in anaphase (2)

Answer 35

1. Chromosomes / chromatids are (in two groups) at poles of spindle / at ends of spindle;
   Do not accept ‘ends of cell’
2. V-shape shows that (sister) chromatids have been pulled apart at their centromeres / that centromeres of (sister) chromatids have been pulled apart.

Question 36

Eukaryotic division – During the cell cycle, the amount of DNA in a cell changes. Explain how the behaviour of chromosomes causes these changes in the amount of DNA per cell (2)

Answer 36

(Increase)
1. Chromosomes / DNA replicates;
(First decrease)
2. Homologous chromosomes separate;
(Second decrease)
3. Sister chromatids separate.

Question 37

Eukaryotic division - Suggest why preventing the formation of spindle fibres stopped the cell cycle.

Answer 37

1.   Chromosomes/centromeres cannot attach (to spindle)
OR
Chromosomes cannot line up (on spindle);

2.   (So, no) metaphase;
OR
3.   Chromatids cannot separate (on spindle);
Accept description of ‘cannot separate’ e.g cannot move to poles
Ignore ‘split’

4.   (So, no) anaphase;

Question 38

Eukaryotic division – Describe the appearance of chromosomes in anaphase (1)

Answer 38

Chromatids are being pulled to opposite poles/ends (of the cell) by spindles/spindle fibres;

Question 39

Eukaryotic division - Suggest and explain how two environmental variables could be changed to increase the growth rate of cells. (4)

Answer 39

1. Increased (concentration of) glucose;
2. Increased respiration;
3. Increased (concentration of) oxygen;
4. Increased respiration;
5. Increased temperature;
6. Increased enzyme activity;
7. Increased (concentration of) phosphate;
8. Increased ATP/DNA/RNA;
9. Increased (concentration of) nucleotides;
10. Increased DNA synthesis;

Question 40

Eukaryotic division -– Req Prac 2 Suggest why the student soaked the root tips in hydrochloric acid

Answer 40

1. To break down links between/separate cell walls;
2. Allowing the stain to pass/diffuse into the cells
   OR
   Allowing the cells to be (more easily) squashed;

Question 41

Eukaryotic division -– Required Practical 2 Pressing the coverslip downwards enabled the student to observe the stages of mitosis clearly.
Explain why.

Answer 41

1. To break down links between/separate cell walls;
2. Allowing the stain to pass/diffuse into the cells
   OR
   Allowing the cells to be (more easily) squashed;

Question 42

Eukaryotic division -– Required Practical 2 using only the first 5 mm from the tip of an onion root.(1)

Answer 42

Where dividing cells are found / mitosis occurs;
OR
No dividing cells / mitosis in tissue further away / more than 5 mm from tip;
OR
To get (soft) tissue that will squash;
OR
Length that will fit under cover slip;

Question 43

Eukaryotic division – Required Practical 2 - Describe how you would determine a reliable mitotic index (MI) from tissue observed with an optical microscope.
Do not include details of how you would prepare the tissue observed with an optical microscope.

Answer 43

1. Count cells in mitosis in field of view;
2. Divide this by total number of cells in field of view;
3. Repeat many/> 10 times
   OR
   Select (fields of view) at random;

Question 44

Eukaryotic division – Required practical 2 Describe and explain what the student should have done when counting cells to make sure that the mitotic index he obtained for this root tip was accurate.

Answer 44

1. Examine large number of fields of view / many cells;
   Mark as pairs only
   Accept large number / 20 or more for many
2. To ensure representative sample;
   Accept typical / reliable
   OR
3. Repeat count;
4. To ensure figures are correct;
   OR
5. Method to deal with part cells shown at edge /count only whole cells;
6. To standardise counting;

Question 45

Eukaryotic division – Required Practical 2 Suggest why different student may get a different mitotic index using the same methos (assume no errors) (2)

Answer 45

1. (Garlic) grown for different lengths of time
   OR
   (Garlic) grown in different conditions;
   Accept suitable descriptions of conditions, eg in different temperatures
2. The root tips from different (garlic) plants/roots/bulbs/species;
3. Single field of view is not representative of a root tip
   OR
   Different fields of view are different samples;

Question 46

Eukaryotic division -The scientists measured the percentage change in tumour volume.
Suggest why they recorded both percentage change and tumour volume.(2)

Answer 46

Percentage change
1.   To allow comparison as tumours may differ in volume/size (at the start of the investigation);
Tumour volume
2.   (As) tumours may differ in length/width/shape
OR
(As) volume is (best) indication of the number of cells in tumour;

Question 47

Membrane structure – Describe how proteins arrange themselves in the membrane (2)

Answer 47

1. Hydrophobic parts of helix/AP (to the outside) to sit within the (hydrophobic) fatty acid (tails) of the phospholipids;
2. Hydrophilic parts of helix/AP (to the inside) as ions are charged/polar/water soluble;

Question 48

Membrane structure – Describe the role of cholesterol (1)

Answer 48

Cholesterol stabilises the membrane
OR
Cholesterol restricts the movement of molecules/phospholipids (making up the membrane);

Question 49

Transport methods - Name and describe five ways substances can move across the cell-surface membrane into a cell. (5)

Answer 49

1. (Simple) diffusion of small/non-polar molecules down a concentration gradient;
   If no reference to ‘small/ non-polar’ for 1.
   accept this idea from ‘large/charged’ given in description of 2.
2. Facilitated diffusion down a concentration gradient via protein carrier/channel;
   Reject if active rather than passive
3. Osmosis of water down a water potential gradient;
4. Active transport against a concentration gradient via protein carrier using ATP;
5. Co-transport of 2 different substances using a carrier protein;

Question 50

Transport methods - The movement of substances across cell membranes is affected by membrane structure. Describe how. (5)

Answer 50

1.   Phospholipid (bilayer) allows movement/diffusion of non-polar/lipid-soluble substances;
2.   Phospholipid (bilayer) prevents movement/diffusion of polar/ charged/lipid-insoluble substances
OR
(Membrane) proteins allow polar/charged substances to cross the membrane/bilayer;
3.   Carrier proteins allow active transport;
4.   Channel/carrier proteins allow facilitated diffusion/co-transport;
5.   Shape/charge of channel / carrier determines which substances move;
6.   Number of channels/carriers determines how much movement;
7.   Membrane surface area determines how much diffusion/movement;
8.   Cholesterol affects fluidity/rigidity/permeability;

Question 51

Transport methods - Give two similarities in the movement of substances by diffusion and by osmosis. (2)

Answer 51

1. (Movement) down a gradient / from high concentration to low concentration;
2. Passive / not active processes;
   OR
   Do not use energy from respiration / from ATP / from metabolism;
   OR
   Use energy from the solution;

Question 52

Transport methods – What two factors affect the rate of facilitated diffusion (2)

Answer 52

1. (external) concentration
2. number of channel / carrier proteins

Question 53

Transport methods - Suggest and explain two ways the cell-surface membranes of may be adapted to allow rapid transport of nutrients. (2)

Answer 53

1. Membrane folded so increased / large surface area;
   OR
   Membrane has increased / large surface area for (fast) diffusion / facilitated diffusion / active transport / co-transport;
2. Large number of protein channels / carriers (in membrane) for facilitated diffusion;
3. Large number of protein carriers (in membrane) for active transport;
4. Large number of protein (channels / carriers in membrane) for co-transport;

Question 54

Transport methods - Describe how substances move across cell-surface membranes by facilitated diffusion. (3)

Answer 54

1. Carrier / channel protein;
2. (Protein) specific / complementary to substance;
3. Substance moves down concentration gradient;

Question 55

Transport methods - Contrast the processes of facilitated diffusion and active transport. (3)

Answer 55

1. Facilitated diffusion involves channel or carrier proteins whereas active transport only involves carrier proteins;
2. Facilitated diffusion does not use ATP / is passive whereas active transport uses ATP;
3. Facilitated diffusion takes place down a concentration gradient whereas active transport can occur against a concentration gradient.

Question 56

Transport methods - Why does inhibiting
respiration/using cyanide prevent
active transport? (4)

Answer 56

1. Oxygen is required for aerobic respiration which releases ATP
2. ATP is needed to change the shape of the protein carrier
3. Which would cause the release of the transported ion/molecule
4. So no ATP, no Active Transport

Question 57

Required practical 3
How do we find water potential of plant tissue practically? (3)

Answer 57

1. Plot a graph with concentration on the x-axis and percentage change in mass on the y-axis;
2. Find concentration where curve crosses the x-axis/where percentage change is zero;
3. Use (another) resource to find water potential of sucrose concentration (where curve crosses x-axis);

Question 58

Required practical 4
Describe an experiment that you could do to investigate whether the mangrove root cells have a lower water potential than sea water.
You are given:
•   a piece of fresh mangrove root
•   sea water
•   access to laboratory equipment.

Answer 58

1. Record mass/length before and after;
2. Place in sea water for specified/equal time;
3. Remove surface water;
4. Increase in mass/length will show water has been absorbed by osmosis;
5. Repeat minimum of three times;

Question 59

Required practical 4
Give one way in which the student could ensure the first three beetroot cylinders were kept at 25 °C throughout her experiment. (1)

Answer 59

Measure temperature (in tube) at intervals and use appropriate corrective measure (if temperature has fluctuated)

Question 60

Required practical 4
How does a high temperature disrupt membranes (2)

Answer 60

(By) 70°C denaturing/altering membrane protein
OR
(By) 70°C increasing fluidity/permeability of membrane;

Question 61

Required practical 4
How does alcohol disrupt membranes (1)

Answer 61

(By) ethanol dissolving phospholipid bilayer
OR
(By acid) altering membrane protein;

Question 62

Required practical 4
Use your knowledge of membrane structure to explain how high temperature cause an increase in absorbance 1)

Answer 62

Higher absorbance indicates more pigment (released/in solution)
OR
Higher absorbance indicates more membrane damage/permeability

Question 63

Required practical 4 - Explain why it is important to control the volume of water in each test tube (1).

Answer 63

1. (If) too much water the concentration of pigment (in solution) will be lower / solution will appear lighter / more light passes through (than expected);
   OR
   (If) too little water the concentration of pigment (in solution) will be greater / solution will appear darker / less light passes through (than expected);
2. So results (from different temperatures) are comparable;

Question 64

Non-specific - Phagocytosis (3)

Answer 64

1. Phagosome/vesicle fuses with lysosome;
2. (pathogen) destroyed by lysozymes/hydrolytic enzymes;
3. Antigen (from pathogen) displayed on cell membrane (of phagocyte/antigen presenting cell);

Question 65

Non-specific - Describe how a phagocyte destroys a pathogen present in the blood.(3)

Answer 65

1. Engulfs;
   Accept endocytosis
   OR
   Description
   Ignore ‘taken in’
2. Forming vesicle/phagosome and fuses with lysosome;
3. Enzymes digest/hydrolyse;

Question 66

Specific - Describe how presentation of a virus antigen leads to the secretion of an antibody against this virus antigen.

Answer 66

1. Helper T cell / TH cell binds to the antigen (on the antigen-presenting cell / phagocyte);
2. This helper T / TH cell stimulates a specific B cell;
3. B cell clones
   OR
   B cell divides by mitosis;
4. (Forms) plasma cells that release antibodies;

Question 67

Specific - What is antigen? (2)

Answer 67

1. Foreign protein;
2. (that) stimulates an immune response/production of antibody

Question 68

Specific - What is antibody? (2)

Answer 68

1. A protein/immunoglobulin specific to an antigen;
2. Produced by B cells OR Secreted by plasma cells;

Question 69

Specific - Antibody specificity (4)

Answer 69

1. Antibody has (specific) tertiary structure
2. Has binding site/ variable region which only binds to one antigen
3. Antigen is only found on this particular (pathogen/cell/tissue)
4. so antibody (only) binds to / forms antigen/antibody complex with these (pathogen/cell/tissue) destroying them

Question 70

Specific - Antigen-Antibody complex formation (4)

Answer 70

1. Antibody has 4 polypeptide chains and has a quaternary structure
2. Antibody has a variable region which has a specific amino acid sequence/primary structure
3. Shape of the binding site is complementary to the antigen
4. Forming an antigen-antibody complex

Question 71

Specific - Humoral Response (6)

Answer 71

1. Antigen on surface of bacterium binds to surface protein / surface receptor on a (specific/single) B cell;
2. (Activated) B cell divides by mitosis / produces clone;
3. (Division) stimulated by cytokines / by T cells;
4. B cells/plasma cells release antibodies;
5. (Some) B cells become memory cells;
6. Memory cells produce plasma / antibodies faster;

Question 72

Specific - Give two types of cell, other than pathogens, that can stimulate an immune response. (2)

Answer 72

1. (Cells from) other organisms/transplants;
2. Abnormal/cancer/tumour (cells);
3. (Cells) infected by virus;
4. Antigen presenting cells

Question 73

Specific - Draw a labelled diagram of an antibody (3)

Answer 73

1. Y shape showing two long and two short (polypeptide) chains correctly positioned;
2. binding site labelled on the end of the branches of the Y of the antibody;
   Accept one or two being labelled, if two both must be correct.
3. Variable region labelled /Constant region labelled / Disulfide bridge/bond labelled;

Question 74

Specific - Describe and explain the role of antibodies in stimulating phagocytosis.

Do not include details about the process of phagocytosis.

Answer 74

1.   Bind to antigen
OR
Are markers;
Accept opsonin for ‘marker’
Accept form (antibody-antigen) complexes/are complementary to antigen

2.   (Antibodies) cause clumping/agglutination
OR
Attract phagocytes;

Question 75

Vaccines - Immunity – Compare Active and
Passive Immunity (6)

Answer 75

1. Active involves memory cells, passive does not;
2. Active involves production of antibody by plasma cells/memory cells;
3. Passive involves antibody introduced into body from outside/named source;
4. Active long term, because antibody produced in response to antigen;
5. Passive short term, because antibody (given) is broken down;
6. Active (can) take time to develop/work, passive fast acting;

Question 76

Vaccines - Immunity – Compare Primary and Secondary Response (4)

Answer 76

1. Before vaccination no antibody released because patients not yet encountered vaccine/antigen/virus;
2. Primary response/after first dose) activation/clonal selection/expansion of B cells into plasma cells;
3. Plasma cells release antibodies;
4. Secondary response/after second dose) memory cells produce more antibodies/produce antibodies more
   quickly;

Question 77

Vaccines - How a vaccine produces an immune response (7)

Answer 77

1. Vaccine contains antigen from pathogen;
2. Macrophage presents antigen on its surface;
3. T cell with complementary receptor protein binds to antigen;
4. T cell stimulates B cell;
5. (With) complementary antibody on its surface;
6. B cell/plasma cell secretes large amounts of antibody;
7. B cell divides to form clone all secreting/producing same antibody;

Question 78

Vaccines - Explain why giving children more than one vaccination develops good immunity (2)

Answer 78

1. (Production of more) memory cells;
2. (So) higher concentration of (circulating) antibodies in blood
   OR
   (So) rapid production of antibodies (on further infection)

Question 79

Vaccines - Determining the genome of the viruses could allow scientists to develop a vaccine.
Explain how.(2)

Answer 79

1. (The scientists) could identify proteins (that derive from the genetic code)
   OR
   (The scientists) could identify the proteome;
2. (They) could (then) identify potential antigens (to use in the vaccine);

Question 80

Vaccines - Describe how B lymphocytes would respond to vaccination

Answer 80

1. B cell (antibody) binds to (viral) specific/complementary receptor/antigen;
   Accept B cell forms antigen-antibody complex
2. B cell clones
   OR
   B cell divides by mitosis;
3. Plasma cells release/produce (monoclonal) antibodies (against the virus);
4. (B/plasma cells produce/develop) memory cells;

Question 81

HIV - HIV treatment with anti-retroviral drug AZT (6)

Answer 81

1. Person (infected with HIV) has HIV DNA (in their DNA);
2. New HIV (particles) still made;
3. (AZT) inhibits reverse transcriptase;
4. (AZT) stops replication of HIV;
5. Stops destruction of more / newly infected T cells;
6. So immune system continues to work (and AIDS does not develop);

Question 82

HIV - Describe how HIV is replicated (5)

Answer 82

1. Attachment proteins attach to receptors on helper T cell/lymphocyte;
2. Nucleic acid/RNA enters cell;
3. Reverse transcriptase converts RNA to DNA;
4. Viral protein/capsid/enzymes produced;
5. Virus (particles) assembled and released (from cell);

Question 83

HIV - Describe how the human immunodeficiency virus (HIV) is replicated once inside helper T cells (TH cells). (4)

Answer 83

1. RNA converted into DNA using reverse transcriptase;
   Reject ‘messenger’ or ‘m’ before RNA
2. DNA incorporated/inserted into (helper T cell) DNA/chromosome/genome/nucleus;
3. DNA transcribed into (HIV m)RNA;
   Accept descriptions of transcription
4. (HIV mRNA) translated into (new) HIV/viral proteins (for assembly into viral particles);

Question 84

HIV - Explain how HIV affects the production of antibodies when AIDS develops in a person. (3)

Answer 84

1. Less/no antibody produced;
2. (Because HIV) destroys helper T cells;
   Accept ‘reduces number’ for ‘destroys’
3. (So) few/no B cells activated / stimulated
   OR
   (So) few/no B cells undergo mitosis/differentiate/form plasma cells;

Question 85

HIV - Describe the structure of the human immunodeficiency virus (HIV). (4)

Answer 85

1.   RNA (as genetic material);
Reject nucleus/DNA/plasmids.
2.   Reverse transcriptase;
3.   (Protein) capsomeres/capsid;
Reject capsule.
4.   (Phospho)lipid (viral) envelope
OR
Envelope made of membrane;
Reject if HIV has a cell membrane or a cell wall.
5.   Attachment proteins;

Question 86

Monoclonal Antibodies- What is a monoclonal antibody? (3)

Answer 86

1. Antibody specific/complementary to one antigen only
2. Antibodies all the same and from one original plasma cell
3. Derived from a hybridoma cell/fused B lymphocyte and cancer cell

Question 87

Monoclonal antibodies - Suggest monoclonal antibodies help scientists to identify target cells (4)

Answer 87

1. antigen in cell-surface membrane;
2. Antibody is complementary;
3. (So) binds/attaches to the ZO-1/protein;
4. (Cells identified with) dye/stain/fluorescent marker linked to antibody;

Question 88

Monoclonal antibodies – Suggest how one antibody can bind two different molecules (2)

Answer 88

1. have a similar shape/structure;
2. Antibody is complementary to both
   OR
   Antigen-binding site is complementary to both
   OR
   Antibody can form antigen-antibody complex with both

Question 89

Monoclonal antibodies - Explain why antibody will only bind to target cell

Answer 89

1. antibody has a (specific) tertiary structure;
2. Has binding site / variable region that only binds to / complementary to one antigen;
3. Antigen to this antibody (only) found on these nerve cells;
4. So, antibody (only) binds to / forms antigen-antibody complex with these cells

Question 90

Monoclonal antibodies - Describe the role of antibodies in producing a positive result in an ELISA test.(4)

Answer 90

1.   (First) antibody binds/attaches /complementary (in shape) to antigen;

2.   (Second) antibody with enzyme attached is added;

3.   (Second) antibody attaches to antigen;
Accept (second) antibody attaches to (first) antibody (indirect ELISA test).

4.   (Substrate/solution added) and colour changes;

Question 91

Why are viruses classed as non living?

Answer 91

have no metabolism/metabolic reactions;
OR
Cannot (independently) move/respire/replicate/reproduce/excrete
OR
(Have) no nutrition;

Question 92

Why are viruses classes as acellular?

Answer 92

no cell(-surface) membrane
OR
Not made of cells;
Or
Has no cytoplasm/organelles