Chapter 1: Cells and Microscopy

Question 1

how is magnification calculated?

Answer 1

image size / actual size

Question 2

how is total magnification calculated?

Answer 2

eye piece magnification x objective magnification

Question 3

what are the differences between light and electron microscopes?

Answer 3

Radiation source = light v electrons

LM uses living specimen EM electron has vacuum ∴ dead samples

LM can distinguish colour EMelectron can’t

LM has has low mag. and res, EM electron has high mag. and res.

Question 4

what does an electron microscope use to focus?

Answer 4

an electromagnet

Question 5

what is the maximum resolution for a- light microscope- electron microscope?

Answer 5

LM 200nm

EM 0.1nm

Question 6

what is the maximum magnification for a light microscope, scanning electron microscope (SEM), transmission electron microscope (TEM)?

Answer 6

LM 1500x

SEM 100,000x

TEM 500,000x

Question 7

what is the definition of magnification?

Answer 7

the degree of enlargement of an image to reveal further detail

Remember: magnification is limited by reosolution of the microscope

Question 8

what is the definition of resolution?

Answer 8

the ability to distinguish between two different points and to see detail

Question 9

what is the use of a microtome?

Answer 9

to cut extremely thin non-living specimens so that the light rays or beam of electrons can pass through the specimen

Question 10

how does a TEM produce an image?

Answer 10

• e- passed through specimen
• e- are scattered
• magnetic lenses focus image on fluorescent screen / photographic plate

Question 11

how does an SEM produce an image?

Answer 11

e- knock other e- from surface of specimen

Question 12

what is added to TEM specimens?

Answer 12

• heavy metal impregnation
• used to stain specimen as atoms of heavy metals have large positivec nuclei that scatter e- beam

Question 13

what is added to SEM specimens?

Answer 13

coated with carbon/gold

Question 14

outline the process of preparing a temporary slide

Answer 14

• fixation
• staining
• mounting

Question 15

outline the process of prepaing a permanent slide

Answer 15

1. fixation (immersion in gluteraldehyde)
2. dehydration (incr. alcohol content)
3. clearing (xylol removes alcohol)
4. embedding (in epoxy/resin)
5. sectioning
6. staining
7. mounting

Question 16

what is cryosectioning?

Answer 16

• tissue embedded in gel medium
• then rapidly frozen to -20/-30^oC
• cut with cryostat into 5-10 um sections
• then stained

Question 17

what is the purpose of differential staining?

Answer 17

to improve contrast betwen diferent tissues and or strucrtures

i.e. to make certain structures appear darker or different in colour from other structures

to distinguish between

• different types of cells
• living and dead cells
• different chemicals or metabolic processed

Question 18

how is Leishman’s stain applied?

Answer 18

• blood smear prepared
• allow blood smear to air dry
• fixed with methanol for 2 mins
• dilute with distilled with water for 6 mins
• slide washed until pink to naked eye

Question 19

how is Wright’s stain applied?

Answer 19

• blood smear prepared
• allow blood to air dry
• dipped in Wright’s stain for 3-4 minutes
• dilute in distilled water
• leave for 6-8 minutes
• rinse in distilled fresh water for 25s (until pale pink edges are seen)
• air dry vertically
• oil applied

Question 20

what is the purpose of a blood smear?

Answer 20

• to observe the appearance of the blood:-
  
  • presence/absence of cells
  • cell morphology
  • cell health

Question 21

how is a blood smear achieved?

Answer 21

• place a small drop of blood at the end of a clean, sterile, dry slide
• another slide used to spread blood at 30^o angle
• immediately labelled slide left to dry
• fixative used to preserve cells

Question 22

what are the functions of the blood?

Answer 22

• delivery of oxygen to tissues
• delivery of nutrients e.g. glc, fatty acids to tissues
• removal of waste products e.g. carbon dioxide, urea from tissues
• immunological protection e.g. circulation of antibodies, phagocytes and memory cells
• clotting
• transport cell signalling molecules e.g. hormones (insulin, glucagon, ADH etc)
• acting as a buffer to regulate pH of plasma
• distribution of heat to regulate core body temperature

Question 23

what is the function of erythrocytes?

Answer 23

red blood cells, RBCs

• Transport oxygen as oxyhaemoglobin from lungs to tissues
• each Hb carries 4 oxygen moecules (i.e. 8 oxtgen atoms)
• Transport carbon dioxide from tissues to lungs

Question 24

how are erythrocytes produced?

Answer 24

• produced from erythropoietic stem cells in bone marrow
• following stimulation from erythropoietin

Question 25

how is the structure of an erythrocyte related to its function?

Answer 25

• no nucleus
• few organelles (incl. no mitochondria, GA)
• biconcave (incr. SA)
• production of haemoglobin (for oxygen transportation)

Question 26

how is the structure of a neutrophil related to its function?

Answer 26

• lobed nucleus
• granular cytoplasm
• many lysosomes containing hydrolytic enzymes (phagocytosis)

Question 27

what are the requirements of a haemocytometery sample?

Answer 27

• mixed (representative)
• known dilution (accurate counting)

Question 28

how is a cell count performed using a haemocytometer?

Answer 28

count number of cells in 3-line square using NW rule

= ___find volume (0.2 x 0.2 x 0.1 = 0.004 mm3) in 1 mm3

= 1/0.004 x ___ = ~~~ cells account for dilution

= ~~~ x dilution factor = …….. cells

Question 29

what is flow cytometery used for?

Answer 29

analysis of physical and chemical characteristics of cells in heterogenous cell populations

Question 30

what are the components of flow cytometery?

Answer 30

flow cell (liquid stream carrying single file cells)

measuring system

detector

amplification system

computer + relevant analysis software

Question 31

how can cell size and volume be analysed by flow cytometery?

Answer 31

• specific antibodies can be tagged to different fluorochromes –> recognise and target specific antigens inside cells/on CSM
• fluorochromes can be attached to a chemical that binds to a specific of DNA/cell membrane/cells structure
• each fluorochrome has its own peak of excitation and emission wavelengthslaser causes tagged cell to fluoresce so it can be counted
• scattering occurs based on size and density

Question 32

what are the 6 principles of cell theory?

Answer 32

1. cell = basic unit of all life forms
2. organisms can be uni- or multi-cellular
3. metabolic processes take place inside the cell
4. new cells are derived from pre-existing cells
5. cells process genetic material which is passed to daughter cells
6. cell = smallest unit of an organism capable of surviving independently

Question 33

what are the structural components of the cell surface membrane (CSM)?

Answer 33

• phospholipid bilayer - selective permeabilitycholesterol - strength and consistency
• proteins - integral (channels) and peripheral (recognition)
• carbohydrates - glycoproteins (recognition)

Question 34

what is the function of the CSM?

Answer 34

1. maintains physical integrity
2. maintains a chemical environment
3. selective permeability
4. marks and signals cell

Question 35

what is the structure of the nucleus?

Answer 35

• surrounded by double membrane called nuclear envelope
• pores in nuclear envelope (allows exchange of molecules)
• contains at least one nucleolus
• large & spherical structure ~10-20um diameter
• fluid within nucleus = nucleoplasm

Question 36

what is the function of the nucleus?

Answer 36

• contains genetic, hereditary material in form of DNA
• control of hereditary characteristics
• replication of DNA for mitosis in S stage of cell cycle
• controls of expression
• chromosomes carry genes for production of polypeptide chains → and hence proteins

Question 37

what is the structure of the nucleolus?

Answer 37

• granular and fibrillar
• components ill-defined matrix
• found within the nucleoplasm
• small spherical structure

Question 38

what is the function of the nucleolus?

Answer 38

Produces rRNA

Produces ribosomal subunits and assembles them into ribosomes

Question 39

what is the structure of the mitochondria?

Answer 39

• Rod shaped organelles
• Capable of changing shape and replicating
• ~1-10nm length
• Possess their own small loop of DNA (code for production of enzymes used in aerobic respiration)
• Surrounded by mitochondrial envelope (double membrane
• Filled with liquid called matrix
• Matrix contains 70s ribosomes & small plasmids (circular loops of DNA)

Question 40

what is the function of the mitochondria?

Answer 40

ATP production through aerobic respiration

• Main function = site of link reaction, Krebs cycle & oxidative phosphorylation (later stages of aerobic respiration)
• Site of ATP production for the cell

Question 41

what is the structure of the endoplasmic reticulum?

Answer 41

• folding network of cisternae held together by cytoskeleton
• RER also has attached ribosomes

Question 42

what is the function of the endoplasmic reticulum?

Answer 42

• RER: protein production
• SER: production, metabolism and storage of fats and steroid hormones
• sarcoplasmic reticulum: storage and release of Ca²⁺ ions for muscle contraction

Question 43

what is the structure of a lysosome?

Answer 43

• Small, fluid filled membrane bag organelle formed by GA
• Contain different types of hydrolytic enzymes (proteases & lipases)
• ~1.0mm diameter
• Typical internal pH ~5

Question 44

Outline the functions of a lysosome?

Answer 44

• breaking down macromolecules in hydrolysis
• remove unwanted cell structures & organelles and chemicals within cell
• important role in phagocytosis & apoptosis
• enzymes usually formed on RER and then enclosed in vesicles which bud off the Golgi body

Question 45

what is the structure of the golgi apparatus?

Answer 45

• Appear similar to SER but form convex shapes
• Made from fluid-filled flattened sacs of cisternae held together by matrix proteins and cytoplasmic microtubules
• Typically 40-100 stacks per GA & 3-6 cisternae per stack

Question 46

what is the function of the golgi apparatus?

Answer 46

• Assemble polypeptides into proteins
• Package proteins and lipids made by RER and SER
• Modify proteins and lipids
  
  • addition of glycocalyces (glycocalyx = singular) which are oligosaccharides → glycoproteins & glycolipids
  • addition of phosphate groups → phospholipids
• Sort proteins into vesicles → ensures proteins/lipids are transported to correct place in cell
• ost modification (glyco)proteins, (glyco)lipids and phospholipids packaged into golgi vesicles

Question 47

what is the structure of a ribosome?

Answer 47

• NOT membrane bound i.e. not true organelles
• Actually cytoplasmic granules made from rRNA and protein
• Found free in cytosol or bound to ER to form RER
• Each ribosome contains 2 subunits: large & small subunit
• Two types:
  
  • 80s
    
    • only found in eukaryotes (free or on RER)
    • 25-30 nm diameter
    • 1:1 ratio of rRNA:protein
    • Large subunit = 60s, small = 40s
  • 70s
    
    • found in cytosol of prokaryotes
    • 65%:35% ratio of rRNA:protein in prok.
    • also found in mitochondria & chloroplasts
    • Large subunit = 50s, small = 30s

Question 48

what is the function of a ribosome?

Answer 48

synthesis of a polypeptide chain through translation of mRNA

Question 49

what is the structure of a centriole?

Answer 49

• Cylindrical structure found in membrane bound vesicle → centrosome
• Membrane of centrosome is continuous with nuclear envelope during interphase
• Found in pairs
• Composed mainly of protein called tubulin in structures called microtubules (see later)
• Short cylinders of 9+0 arrangement (i.e. 9 microtubules arranged in circle around the circumference but none in the centre)

Question 50

what is the function of a centriole?

Answer 50

• Organise spindle fibres in nuclear division (mitosis & meiosis)
• Centriole within centrosome duplicates itself during G2 phase of cell cycle: they are arranged at right angles to each other
• Centrosomes migrate to poles during prophase
• Impotant in increasing effectiveness of mitosis
• Involved in the movement of cilia and flagella

Question 51

what is the structure of a vacuole?

Answer 51

• membrane-bound sacs
• surrounded by a sinlge membrane called a tonoplast (selectively permeable membrane)

Question 52

what is the function of a vacuole?

Answer 52

• Acts as reservoir for water (main content)
• Also contain dissolved salts, sugars, organic acids
• Provide support to the plant cell
• Contributes to cell turgidity i.e. provides whole plant support
• Surrounded by tonoplast

Question 53

how do organelles work together to produce a protein?

Answer 53

• nucleus contains gene for transcription of protein
• nucleolus = site of ribosomal subunit production & assmebly
• ribosomes = site of translation of mRNA to form ppc
• RER is continuous with nuclear envelope
• vesicles transport protein to golgi apparatus, which processes it (e.g. quaternary structure by adding prosthetic groups)
• golgi vesicles transport protein to CSM

Question 54

what are the features of a prokaryotic cell?

Answer 54

• no nucleus
• no embrane-bound organelles
• 70 Svedberg ribosomes
• peptidoglycan cell wall
• flagella
• polysaccharide capsule
• plasmid DNA

Question 55

what are the three main types of unicellular cells?

Answer 55

• amoeba
• chlamydomonas
• paramecium

Question 56

what is the role of the cytoskeleton?

Answer 56

• cell stability
• support
• movement of cilia and flagella
• changing shape of cell during cytokinesis
• phagocytosis
• exocytosis
• movement of organelles/vesicles

Question 57

what are the three components of the cytoskeleton?

Answer 57

1. microfilaments
2. intermediate filaments (10nm)
3. microtubules (23nm)

Question 58

outline the process by which motor proteins move along the cytoskeleton

Answer 58

• binding conformational change
• filament release
• conformational relaxation
• filament rebinding

Question 59

what is the purpose of colourimetery?

Answer 59

quantitative analysis of a solution to determine its quantity/quality

Question 60

what is simple diffusion?

Answer 60

passive movement of molecules down the concentration gradient (until an equilibrium is reached) across a partially permeable membrane

Question 61

what are the factors affecting the rate of diffusion?

Answer 61

• Concentration gradient
• Size of molecule
• Amount of kinetic energy the molecules posses (i.e. directly related to temperature)
• Polarity of the molecule
• Surface area
• Diffusion distance

Question 62

what is facilitated diffusion?

Answer 62

Passive movement of molecules down the concentration gradient through specialised proteins (until an equilibrium is reached) across a partially permeable membrane

Question 63

what is function of

• channel proteins
• carrier proteins?

Answer 63

Channel proteins

• Form pores form aqueous channels which allows ions to cross
• Can be gated which enables the channels to be open or closed depending on
  
  • A potential differences across the membrane
  • The presence of a specific molecule (a ligand)
• Used to transport water soluble molecules and ions
• Different channels are specific to specific ions i.e. some channels allow Na⁺ to cross whereas others allow Cl^- ions to cross etc

Carrier proteins

• each carrier protein has a complementary binding site to a specific molecule
• carrier protein undergoes allostery i.e. a conformational change
• The carrier protein changes between a ‘ping’ and ‘pong’ state
  
  • Ping state = binding site exposed to outside of the cell
  • Pong state = binding site exposed to inside of the cell
• Used to transport larger molecules e.g. glucose, amino acids uptake in small intestine

Question 64

what is active transport?

Answer 64

• the movement of molecules against their concentration gradient
• requires ATP
• requires a carrier protein:-
  
  • with a specific binding site
  • to undergo a conformational change
  • have a binding site for ATP- ∴ can carry out hydrolysis

Question 65

outline the process of active transport across a membrane

Answer 65

• carrier protein takes up molecule from outside
• molecule binds to carrier protein
• ATP attaches to membrane protein on inside
• molecule causes conformational change to structure –> access for molecule opened
• molecules released to inside of membrane using E from hydrolysis of ATP
• release of molecule causes carrier protein to revert to binding configuration

Question 66

what are the two forms of endocytosis?

Answer 66

• intake of small quantitites of liquid by pinocytosis
• intake of olid material by phagocytosis

Question 67

what is the function of endocytosis?

Answer 67

• uptake of nutrients
• engulfing bacteria

Question 68

State the function of exocytosis and give 2 exmpales

Answer 68

• insoluble waste material excreted from cell
• e.g.
  
  • the removal of waste products or secretion of useful products (e.g. secretion of pancreatic enzymes, secretion of insulin from -cells of the pancreas)
  • plant cells use it to develop the cell wall which is outside of the cell surface membrane

Question 69

Describe the how to test for lipids in

a) a liquid sample and
b) a solid sample

Answer 69

Testing liquid smaples:

• add ethanol
• add equal volume of distilled water
• shake gently
• mixture turns cloudy/milky

Testing solid samples

• Place a small piece of each solid into test tube
• Add 2 cm³ ethanol to test tube and shake thoroughly
• Using the glass rod gently mash each sample: ensure rod is cleaned between samples to avoid cross-contamination
• Shake each tube thoroughly
• Allow the solid to settle to the bottom of the tube
• Carefully pipette the ethanol from each sample into a fresh, labelled tube, leaving the solid sediment behind
• Add 2 cm³ distilled water and shake gently to mix
• Observe the appearance of each sample

Question 70

what are the similarities between a triglyceride and a phospholipid?

Answer 70

Both

• contain glycerol
• contain fatty acids
• contain choline
• contain ester bonds
• contain C, H and O
• formed by condensation reactions

Question 71

what are the differences between a triglyceride and a phospholipid?

Answer 71

• T: 3 fatty acids; P: 2 fatty acids
• T: 3 ester bonds; P: 2 ester bonds
• T: absence of phosphate group; P: presence of phosphate group

Question 72

Whay do we preserve specimens?

Answer 72

• To enable them to be cut into secrions to observe under a microscope
• To enable them to be treated with different stains

Question 73

Describe how to prepare a temporary slide for observing under an LM

Answer 73

1. Fixation: use 70% alcohol
2. Staining: use few drops of appropriate differential stain
3. Mounting: cover with coverslip to exclude dust and air

Question 74

State 2 advanatges of preparing temporary slides for use under an LM

Answer 74

1. Rapid & simple procedure (no complex apparatus or skill required)
2. Can mount specimen in glycerine to prolong examination period

Question 75

Explain why specimens need to be fixed before observing under a LM

Answer 75

• specimen in life like condition
• minimises distortion
• chemicals such as or are added to make proteins and nucleic acids insoluble à fixing them in position

Question 76

Explain why specimens need to be dehydrated before observing under an LM

Answer 76

• traces of water from fixed material
• Achieved by placing the specimen in increasing e.g. up to 70% ethanol

Question 77

Explain why specimens need to be dehydrated before observing under an LM

Answer 77

• Addition of xylol
• Ensures material is made

Question 78

Explain why a specimen needs to be embedded as part of the preparation methd for preparin a temporary slide

Answer 78

• material so it is firm enough for sectioning
• can be resin, plastic or wax

Question 79

State 3 advantages of using differential stains

Answer 79

1. General adv = most biological specimens are colourless & almost transparent → easier to observe tissues/cells/chemicals
2. when observing animal tissue = allows observer to distinguish xylem vessels from other tissues etc
3. when observing plant tissue = allows observer to distinguish between different types of WBC

Question 80

State 4 advanatages of using a LM

Answer 80

1. Low skill set needed by user
2. Can be transported to use in field work
3. Can observe living organisms
4. Relatively inexpensive so available for schools & colleges

Question 81

State 3 disadvantages of using a LM

Answer 81

1. Low resolution
2. Hence limited magnification
3. Many internal cellular structures can’t be seen e.g. ribosomes, cristae,

Question 82

Discuss advanatges and disadvantages of using EM

Answer 82

Advantages of EM

• greater resolution (~0.1nm)
• higher magnifications can be used
• finer detail seen e.g. ribosomes

Disadvantages of EM

• specimen has to be placed in vacuum therefore must be dead (as essential specimen is completely dehydrated)
• highly expensive so prohibits use in schools
• high skill set required à need for training before use
• must be used in specialist room due to electromagnets within the EM
• more complex process to prepare specimen e.g. must be mounted on copper grid rather than glass slide
• more prone to artefacts due to complex preparation procedure

Question 83

Compare TEM and SEM

Answer 83

Both

• use e- beam
• place specimen in vacuum
• can only be used to observe dead specimens
• produce images that can be colour enhanced
• have higher resolution than LM
• obtain higher magnifications than LM

Differences

• TEM = 2D image, SEM = 3D image
• TEM higher resolution than SEM
• TEM max mag = 100 000x, SEM 10 000x
• TEM shows internal detail, SEM shows surface detail and contours
  *

Question 84

State 6 advanatges of using Confocal Scanning Laser Microscope

Answer 84

1. ability to eliminate or reduce background information away from the focal plane to reduce to image degradation
2. capability to collect a series of optical sections from thick specimens ay various depths by optical sectioning
3. ability to obtain high resolution images
4. ability to obtain 3D reconstructions
5. ability to image living cells and tissues
6. any out-of-focus light is blocked à clearer image than standard LM

Question 85

Outline how CSLM works

Answer 85

1. point source of light is detected on to the object plane
2. point of emitted fluorescence light or reflected light from the specimen is directed through detector pinhole
3. fluorescent/reflected light is enhanced using photomultiplier
4. fluorescent/reflected light displayed on computer screen as a pixel
5. specimen is scanned point by point & line by line à very thin, blur-free optical sections are recorded one pixel at a time
6. series of images then combined à image stack → 3D image

Question 86

Outline how fluorescent markers can be used to detect biological chemicals/structures using a CLSM

Answer 86

• fluorochromes attached to antibody that is specific for one antigen on or in the cell
• fluorochromes can also be tagged to a chemical that binds specifically to a component of the csm, DNA or other structure
• each fluorochrome has its own peak excitation & emission l
• lasers with different l are used depending on which fluorochromes are used
• laser excites the fluorochrome causing the tagged cells to fluoresce
• this fluorescence is counted by the detector
• the specific light scattering and fluorescent characteristics of each cell as they pass the laser beam is used for counting and sorting

Question 87

Describe how to calculate the field of view

Answer 87

Calculating field of view:

Field of view = area that can be seen when looking down through eyepiece

Hence FOV = area of circle i.e. π​r² (units = mm² assuming radius measured in mm)

Question 88

Describe the role of a thrombocyte

Answer 88

• Role in blood clotting
• Role in clot formation

Question 89

Describe the role of a neutrophil

Answer 89

• Defend against bacterial and fungal infections
• Engulf bacteria by phagocytosis

Question 90

State the main role of B-lymphoctyes

Answer 90

Produce immunoglobulins (antibodies)

Question 91

State the different types of T-lymphocytes and outline thier roles

Answer 91

• Several types:
  
  • T helper cell – produces cytokines to coordinate the immune response
  • Cyotoxic T cell – binds to antigens on viral infected cells/tumour cells & destroys them
  • Natural killer cells – roles vary

Question 92

Outline the role of a monocyte

Answer 92

• Carry out phagocytosis
• Longer living than neutrophils
• Can leave the blood stream by amoeboid movement & differentiate into macrophages in the liver, spleen & lungs

Question 93

State which cells can move out of the bloodstrem to become macrophages

Answer 93

1. Neutrophils
2. Monocytes

Question 94

State the 3 key points to the North-West rule when counting cells using a haemocytometer

Answer 94

• count all cells that lie completely within the triple lined 5x5 grid
• also include any cell that lies on the middle line of the north triple boundary and the middle line of the west triple boundary
• if a cell lies on the middle triple line on the south or east boundary do not count them

Question 95

State 4 uses for flow cytometry

Answer 95

• analysing the activity of molecules found in the cell surface membrane and within the cell
• characterising and defining different cell types in heterogeneous (mixed) cell populations
• assessing the purity of samples
• analysing cell size and volume

Question 96

Describe how different cells can be identified using flow cytometry

Answer 96

Larger and more granular granulocyte cells produce a large population with high SS and FS

Monocytes are large cells, but not so granular, so these produce a separate population with high FS but lower SS

Smaller lymphocytes and lymphoblasts produce a separate population with less FS. They are agranular cells so also have low SS.

Question 97

describe the structure and role of the nuclear envelope

Answer 97

• double membrane
• that surrounds nucleus
• outer membrane of NE is continuous with RER

Question 98

Describe the structure and role of the nuclear pore

Answer 98

• Gaps within the NE (usually ~3000 pores)
• Each pore~40-100nm diamete
• Enables cell to control what enters and exits the nucleoplasm from cytosol e.g. allows exit of mRNA after transcription to enable translation to occur in cytosol

Question 99

Describe the structure of the SER

Answer 99

• Series of flattened membrane sacks (cisternae) that form sheets in the cytosol
• Tubular appearance

Question 100

Outline the functions of the SER

Answer 100

• Site of lipid synthesis, storage and transport
• Site of carbohydrate synthesis, storage and transport
• Site of steroid hormone synthesis, storage and transport

Question 101

Describe the structure of the RER

Answer 101

• Series of flattened membrane sacks (cisternae) that form sheets in the cytosol
• Has ribosomes attached to outer surface of cisternae
• Continuous with outer membrane of nuclear envelope

Question 102

Outline the function of the RER

Answer 102

• Site of protein & glycoprotein synthesis
• Site of folding of ppc into 20, 30 structure
• Provides pathway to transport proteins & other materials through the cell

Question 103

Outline the functions of golgi vesicles

Answer 103

• Used in various processes
  
  • secretion e.g. release of insulin from β-cell in pancreas, secretion of antibodies from B-lymphocyte by exocytosis
  • phagocytosis
  • endocytosis
  • transports phospholipids to csm for cell growth
• Also used in cell metabolism and enzyme storage

Question 104

Outline the role of plasmodesmata

Answer 104

• Cell to cell connections between adjacent plant cells
• Enables materials and chemicals to be transferred between cells

Question 105

OUtline the structure and role of a plasmid

Answer 105

Structure:

• Very small circular pieces of DNA
• Separate from main DNA within cytosol
• Capable of replicating independently of main DNA

Role:

• Carry genes that increase survival chances of prokaryote e.g. genes to produce enzymes that breakdown antibiotics (i.e. antibiotic resistance genes)

Question 106

Explain how bacteria carry out respiration int he absnece of any mitochondria

Answer 106

• Formed by invaginations of cell surface membrane (csm)
• Site of aerobic respiration

Question 107

Outline the structure and role of pili

Answer 107

• Hair-like structures
• Extend through cell wall
• Enable bacteria to adhere to each other (important in sexual reproduction in bacteria) or other surfaces
• NB Not found in all species of bacteria

Question 108

Outline the structure and role of a flagellum

Answer 108

Structure

• Specialist extension of csm and cytosol

Role

• Enables motility and movement of bacteria
• Rotation unit at base of flagellum (motor protein)
• Some bacteria have multiple flagella

Question 109

Describe the structure of microfilaments

Answer 109

• made from a specialised protein = actin
• thinnest cytoskeletal filaments
• consist of 2 intertwined strands
• 7nm width

Question 110

Outline the role of microfilaments

Answer 110

• maintain the cell shape
• enable motility e.g. pseudopodia
• enable muscle contraction e.g. skeletal muscle
• enable cytokinesis of cell division

Question 111

Describe the structure of intermediate cytoskeleton filaments

Answer 111

• ~10nm diameter
• more stable than microfilaments
• made specialised protein called keratin
• consist of fibres wound together

Question 112

Outline the role of intermediate cytoskeleton filaments

Answer 112

• maintain the cell shape
• anchor the nucleus & organelles in the cytosol

Question 113

Describe the structure of microtubules

Answer 113

• ~23 nm diameter
• made of specialised protein called tubulin
• arranged in hollow cylinders

Question 114

State 4 functions of microtubules

Answer 114

• maintain the cell shape
• enable motility e.g. cilia & flagella
• enable movement of chromosomes
• enable movement of organelles

Question 115

State 4 functions that all cell cytokeleton fibres have in common

Answer 115

• help to maintain the cell’s shape & structure
• enable the movement of organelles within the cytosol
• enable the intracellular transport of molecules & materials
• enable the movement of chromosomes to occur during mitosis & meiosis

Question 116

Outline how motor proteins can move cell structures within the cell

Answer 116

1. Motor protein binds strongly to a cytoskeleton filament
2. Motor protein undergoes a conformational change (allostery)
3. Motor protein is released from the filament (unbound)
4. Motor protein undergoes conformational relaxation (i.e. returns to original shape)
5. Motor protein rebinds to the cytoskeletal filament i.e. process repeats
6. This cyclical process à motor protein & associated organelle/molecule moves few nm at a time along filament

Question 117

State 8 roles of cell membranes

Hint: remember cell membranes include both the cell surface membrane (plamsa membrane) and internal cell membranes

Answer 117

1. control entry & exist of molecules within organelles
2. isolate organelles to enable specialisation of chemical reactions
3. provide internal transport system
4. concentrate enzymes & substrates to increase efficiency and productivity of organelle
5. isolate enzymes to prevent cellular damage
6. maintain internal specific conditions at optimal level
7. can be moved within cell to where they are needed
8. provide surfaces for chemical reactions

Question 118

State the 3 main components of cell membranes

Answer 118

1. phospholipids
2. proteins
3. cholesterol

Question 119

State 5 key features/characteristics of cell membranes

Answer 119

• 7nm wide
• Allow lipid soluble molecules to cross bilayer
• Prevent water soluble molecules from crossing bilayer
• Allows membrane to be flexible
• Allows membrane to be stable

Question 120

Define an integral/intrinsic protein

Answer 120

• span across both monolayers

Question 121

State 6 functions of integral/intrinsic proteins

Answer 121

1. Carrier proteins for specific molecules
2. Channel proteins for water-soluble molecules & ions
3. Electron carriers
4. Structural role
5. Receptor proteins
6. Membrane-bound enzymes

Question 122

Define a extrinsic/peripheral protein

Answer 122

Proteins that only exist within one monolayer

Question 123

Describe the roles/functions on extrinsic proteins

Answer 123

• Glycoproteins receptors
• Membrane-bound organelles
• Electron carriers
• Structural role
• Cell to cell recognition
• Antigens that trigger an immune response
• Cell to cell adhesion

Question 124

Describe the properties and arrangement of phospholipids in cell membranes

Answer 124

• Have a polar head
  
  • Which consists of glycerol, choline & phosphate group
  • Is hydrophilic
• And a non-polar tail
  
  • which consists of 2 fatty acid tails
  • is hydrophobic
• PPL molecules are arranged as a bilayer (upper & lower monolayer)
• PPL bilayer acts as a barrier to water-soluble molecules

Question 125

Describe the role of cholesterol in cell membranes

Answer 125

• Provide mechanical strength to the cell membrane
• Regulate fluidity of the membrane
• Prevent water & water-soluble ions leaking out
• Reduce lateral movement of PPL within the monolayer

Question 126

Describe the properties of cholesterol

Answer 126

• It is a specialised lipid (steroid)
• It is mostly hydrophobic but one part is hydrophilic (this area is attracted to the phosphate head of the PPL molecules)
• The amount of cholesterol within different membranes varies

Question 127

State what a glycoclayx is and its function

Answer 127

State:

• carbohydrate chain which can be added to a protein or a PPL

Function

• Act as antigens
• Act as recognition sites for the attachment of other molecules

Question 128

Outline the difference between glycolipids and glycoproteins and thier functions

Answer 128

Glycolipid = lipid + glycocalyx

• Acts as recognition sites
• E.g. cholera toxin

Glycoprotein = protein + glycocalyx

• Acts as recognition site for molecules
• E.g. Hormones & neurotransmitters

Question 129

Describe the properties of the phospholipid head

Answer 129

• polar
• hydrophilic
• because it can form hydrogen bonds with water
• this property stabilises the membrane

Question 130

Describe the propetries of the phosphlipid tails

Answer 130

• non-polar
• hydrophobic
• unsaturated fatty acids contribute to fluidity of the membrane
• fatty acid core forms barrier to hydrophilic substances and ions
• fatty acid core allows movement of non-polar substances & fat-soluble molecules

Question 131

State the main components of a single phosphlipid

Answer 131

1 glycerol + 1 choline + 1 phosphate group + 2 fatty acids

Question 132

Outline how a triglyceride is formed

Answer 132

• Requires 3 condensation reactions (one between each FA and glycerol)
• 3 water molecules removed (and released as waste product)
• 3 ester bonds formed (one between each FA & glycerol)

Question 133

OUtline how a phospholipid is formed

Answer 133

• Formed by 2 condensation reactions
• One condensation reaction between 1 FA and glycerol molecule

Question 134

Outline how cholesterol regulates the fluidty of cell membranes

Answer 134

• at low*** temp it ***increases fluidity
• at high*** temp it *****dec**_r_eases fluidity

Question 135

State 5 roles of glycoproteins in cell membranes

Answer 135

1. Antigens and cell markers
2. Cell adhesion
3. Satabilises the membrane by interacting with water
4. Acts as a receptor molecule for cell signalling
5. Cell recognition

Question 136

Describe how carrier proteins involved in facilitated diffusion and active transport are similar

Answer 136

both

• use intrinsic proteins
• posses a binding site
• have a binding site which is specific for a particular molecule
• have a bindings site which is complementary to the molecule to be transported
• undergo a conformational change (i.e. allostery) to move the molecules

Question 137

Describe how carrier proteins involved in facilitated diffusion and active transport are different

Answer 137

Carrier proteins involves in AT also

• Have an additional binding site for ATP
• Requires the hydrolysis of ATP to release the molecule form the binding site
• Only work in one direction
• Allow the accumulation of molecules within the cell (i.e. do not stop at the point of equilibrium)
• Work against the concentration gradient

Question 138

Outline the process of phagocytosis

Answer 138

• This is when cells take in solid material in large quantities
• The cells are called phagocytes
• They produce phagocytic vesicles
• E.g. bacteria being engulfed by a phagocyte

Question 139

Outline the process of pinocytosis

Answer 139

• This is when cells take in liquid material in large quantities
• Very small vesicles are formed in a process called micropinocytosis
• E.g. the uptake of nutrients by an ovum from follicle cells

Question 140

Explain the difference betwen a qualitative, semi-quantitiative and quantitative test

Answer 140

Qualitative test

• Only tells of presence or absence of substance

Semi-quantitative test

• Gives an indication of the relative amounts of a substance
• Resulting positive result should be scaled low/medium/high

Quantitative test

• provides information on absolute quantity of substance present

Question 141

Describe how testing for lipids can be produce qualitative, semi-quantitative or quantitative results depending on the method used

Answer 141

Qulaitative:

• Emulsion test: cloudy /colurless = lipids present/absent

Semi-quantitative:

• Emulsion test - degree of cloudines can indicate relative amounts of lipid present (more cloudy = mpre lipid present)

Quantitative :

• Emulsion test: use colorimeter to measure transmission and then use a calibration curve to determine an absolute concentration of lipid

Question 142

Explain how temperature affactes membrane permeability

Answer 142

• Higher temperatures (for example, from 55 °C) increased the permeability of the tonoplast and plasma membrane, which have the same structure.
• Membrane (cell surface membrane and tonoplast) proteins become denatured.
• Both these create spaces for pigment leakage by diffusion.
• This occurs faster i.e. more pigment leaks out at higher temperatures.
• Non linear trend

Question 143

Explain how alcohol affects membrane permeability

Answer 143

• Ethanol will cause membrane disintegration as it forms temporary bonds with the phospholipid heads in the membrane.
• Causes the phospholipids to move out of place so large gaps form in the membrane allowing pigment to leak out.
• Ethanol also affects bonding in the membrane proteins leading to denaturation causing further gaps in the membrane.
• Cholesterol, important in membrane structure, is soluble in ethanol, and so once it is removed, larger gaps allow increased permeability of molecules such as betalin.

Question 144

Suggest 3 limitations that can occur when investigating the effect of temperature/alcohol on membrane permeability

Answer 144

• Cutting cylinders will damage some cell walls and tonoplasts → this will potentially vary between different cylinders
• Differences between blotting techniques (more blotting → removes more pigment)
• Cylinders sit on top of each other /next to each other in some tubes →decreases SA exposed to water (i.e. varies between tubes)
• Degree of swirling will vary between tubes
• Some beetroot loose tissue may be transferred to the cuvette
• Fluctuations in waterbaths → temperature not fully stable & takes longer for cells in centre of cylinder to reach higher temperatures
• Use of forceps to remove cylinder may squeeze tissue and damage cell walls & tonoplasts releasing more pigment
• Insufficient intermediate temperatures → unable to see data between temperatures tested
• No replicates → unable to determine if result is anomalous → can’t calculate SD to determine reliability
• Lack of stirring of solution after removal of cylinder → more densely coloured liquid may not be poured into cuvette

Question 145

Suggest 2 errors that can occur when investigating the effect of temperature/alcohol on membrane permeability

Answer 145

1. Accuracy of cutting cylinders → differences in SA
2. Accuracy of timing period

Question 146

Suggest 3 improvements that could be carried out investigating the effect of temperature/alcohol on membrane permeability

Answer 146

• Carry out at least 3 replicates at each temperature
• Ensure all cylinders cut from same area of the same beetroot
• Standardise blotting mechanism e.g. place on towel and roll once
• Stir coloured liquid after removing cylinder before decanting
• Decant coloured liquid through sieve into cuvette to remove any tissue debris

Question 147

Explain the effect of increasing temperature on the PPL molecules in a cell membrane

Answer 147

• The kinetic energy of the PPL molecules increases
  
  • Causing the PPL molecules to move more within their monolayer
  • This causes the PPL molecules to become more spaced out
  • This causes spaces to occur between the PPL molecules within the cell membranes
  • This causes the cell surface membrane and the tonoplast to become disrupted

Question 148

Explain the effect of increasing temperature on the PPL molecules in a cell membrane

Answer 148

• The kinetic energy of the protein molecules increases
  
  • Causing the protein molecules to move more within their monolayer
  • This causes the protein molecules to become denatured
  • This causes spaces to occur between the protein and PPL molecules within the cell membranes
  • This causes the cell surface membrane and the tonoplast to become more disrupted