Part 3

Question 1

Cardiovascular disease

Answer 1

Main cause of death in UK and world wide, over 1 in 4

Question 2

Myocardial infarction

Answer 2

Heart attack

Leading cause of death in developing countries, one person has a heart attack every 3 min in uk

Question 3

Congenital heart diease

Answer 3

800 deaths per year

1/3 babies

Question 4

Health care cost

Answer 4

around £11 billion per year in UK

Question 5

Why do we study Drosophilla (lower organisms)?

Answer 5

Help understand human organogenesis
Drosophilla genome sequenced- March 2000
929 genes in humans- 548 have homologues in drosophila
Discovered- Hh, Notch, Wg, Dpp

Question 6

Timings of cardiac development in different organisms

Answer 6

Drosophila (24h), mouse (19.5 dpc) and human (40 hrs) all have same steps different timings
Straight after gastrulation:
- fusion and formation of heart tube/looping
- Chamber form
- Heart functions

Question 7

Where do cardiac cells originate from?

Answer 7

Ventral latera mesoderm called splanchnopleura

Somatopleura= Splanchic mesoderm and ectoderm 
Splancnopleura= Splanchnic mesoderm and foregut endoderm (lateral)

Question 8

Heart precursor cells have 2 origins

Answer 8

First heart field
second heart field

Fate cells- identify in early development and follow to late to see what they make

Question 9

What does the first heart field consist of?

Answer 9

• left ventricle
• right ventricle
• atrio-ventricular canal

Question 10

What does the second heart field consist of?

Answer 10

• right ventricle
• outflow tract
• inflow tract

Question 11

Cardiac specification

Answer 11

Production of angiognetic cell clusters
Above neural plate

• Arise immediately after gastrulation
• Crescent mannor is the anterior part of the embryo

Question 12

Steps in heart formation for vertebrate and drosophila

Step 1

Answer 12

Precursor to cardioblast
(specification)

Drosophila- Tinman
Vertebrate- Nkx2.5

Question 13

Heart formation

Step 2

Answer 13

Cardioblast to cardiomyocyte
(Differentiation)

Drosophila- Dmef2
Vertebrate- Mef2

Question 14

Heart formation

Step 3

Answer 14

Cardiomyocyte to linear heart tube

Drosophila- Pannier
Vertebrate- GATA4

Question 15

Heart formation

Step 4

Answer 15

This stage is where there is a difference between drosophila and vertebrate

Drosophila is linear heart tube to dorsal vessel
Vertebrate is linear heart tube to looping heart tube (InV)

Question 16

Heart formation

Step 5

Answer 16

Only in vertebrates
Looped heart tube to multichambered heat

dhand and ehand

Question 17

What drives the specification of cells in heart formation?

Answer 17

Drosophila

• Uses expression of tinman using dpp
• Tinmnan= protein code for TF homeobox
• Expressed through mesoderm however it becomes restricted as the embryo develops only being expressed in the dorsal vessel

Trunk mesoderm - dorsal mesoderm - dorsal vessel

Vertebrate

• Homologues of tinman= Nkx-2
• Nkx2.5 is the earliest to be expressed and specifically in cardiac crescent- restricted to angiogenetic cells

Question 18

What happens when you have a mutant mice of Nkx 2.5?

Answer 18

Do not form a heart and show cardiac defects at looping stage- compensatory mechanism

Mutant humans- congenital heart defects

Question 19

What regulates the expression of a gene?

Answer 19

1. Onset

2. spatial mannor

Question 20

What induces Nkx2.5 expression?

Answer 20

BMP

Express ectopically in gain or loss of function approach
1- electrooporate the BMP genes in the chick timing either immediately prior or same time as you would expect the genes to be expressed.
2-grafting cells expressing Bmp
3- adding beads (BMP bead soaked and control bead), allow chick embryo to develop, carry out in-situ hybridisation,
-Bmp bead expresses Nkx2.5 but at the paraxial mesoderm
-control expresses Nkx2.5 where it would normally be expressed

Question 21

What signal is produced in the anterior mesoderm and neural plate?

Answer 21

Wnt 
so block BMP
-Create an evironment which is favourable for induction 
-Block inhibitory factors 
- array of genes +proteins required

Question 22

Endocardium

Answer 22

Contains precursors of endothelial lining of the heart and cushions cells that form valves

Question 23

Myocardium

Answer 23

Contains myocytes of atria and ventricles and purkinjie fibres

Question 24

What is used for cardiac muscle differentiation on drosophila and vertebrate?

Answer 24

Drosophila- Dmef2

• Induced by Tinman
• Protein expressed in all muscles of developing embryo
• Mutant= lose differentiation of muscle function but still see tinman expression

Vertebrates- Mef2A, Mef2B, Mef2C

• Earliest gene expressed in heart mef2C
• Mutant- no heart looping and no right ventricle up-regulation of ef2B

Question 25

Cardiomyocyte to linear heart tube in vertebrate and drosophila

Answer 25

GATA- Vertebrates

• GATA1-3=Hematopoiesis
• GATA4-6= cardiogenesis with gata4 the earliest gene expressed

Gene 4 KO- failure to form heart tube
+/1- form endocardial tube and migrated to centre and fused to single tube by this point
-/- Instead of seeing single tube fused in ventral part, see 2 tubes remaining in bilateral position

Question 26

Cardiac bilatera

Answer 26

Failure to form and join single tube- form but dont migrate

Gata involved migration (directed- opposite foregut)

Question 27

Heart looping

Answer 27

First break in embryos symmetry
Heart loops to the right
Assymetic- cell division, death and shape

Question 28

How does establishment of left and right asymmetry in the chick embryo occur?

Answer 28

Lefty and nodal two TGFbeta molecules are specifically expressed on the left side, lefty activates Shh
Activin expressed on the right, inhibits Shh

Question 29

Linear heart tube to looping heart

Answer 29

IV and INV
Mutations in InV or IV cause random or complete reversal of heart looping (meant to be to right)
Lefty and nodal expressed on right not left

Question 30

What do IV and InV do?

Answer 30

IV encodes a dynein, protein involved in the movement of cilia
InV encodes for inversion, a protein containing ankyrin repeats found in cilia
Both required for cilia movement/ rotation, useful as cilia establishes a professional flow of nodal and lefty molecules to the left
(mutation= dont flow)

Question 31

How are the chambers formed?

Answer 31

dHand and eHand- bHLH TF with specific expression in right and left venticle

Conditional -/- eHand= Left ventricle defect but mice survive til birth

• /- eHand= placental defects (mice die E8.5)
• /- dHand in mice = RV hypoplasia (mice die at E10.5)

Question 32

What is an organ?

Answer 32

Single functional unit in your body made up from different functional tissue types

Question 33

What happens when the optic vesicle infolds?

Answer 33

Forms a bilayered optic cup
Inner wall of the optic cup= neural retina
Outer wall of the optic cup= pigment epithelium- produce melanin

Question 34

What is the optic cup derived from?

Answer 34

Neuroepithelium
Inner part contains SC like populationwhich can either self renew or differentiate into progenitors that diff into ganglion, interneurons, photoreceptors

Question 35

Where does the lens come from?

Answer 35

Derived from epiderm also containing sc like population which can either self-renew or differentiate to crystallin- producing fibre like cells

Question 36

What type of cells behaviours underlie eye development?

Answer 36

• Changes in fate- neural to optic vesicle, epiderm to lens placode
• Proliferation
• Involution- Optic vesicle to optic cup
• Pinching off- lens placode to lens vesicle
• Migration- differentiation of retinal neuronal types

Question 37

How do different tissues that form the eye assemble?

Answer 37

Changes in fate - neural to optic vesicle induces epiderm to lens placode
Involution- signal from lens placode induces optic vesicle to optic cup
Pinching off- optic cup induces lens placode to lens vesicle

Question 38

Parts of the kidney

Answer 38

• papilla- tip of each pyramidal where urine drains from
• major/minor calyces- empty into renal pelvis
• Renal pelvis- transmits urine to bladder via ureter
• urether- empties into bladder
• cortex- peripheral layer
• medulla- inner layer ( arranged in multiple pyramidal structures that together overlying cortex comprise the renal lobe)
• Renal capsule- fibrous outer layer

Question 39

What is the ureter?

Answer 39

Runs form the kidney to urinary bladder

Ends in renal pelvis a region characterised by major calyces

Question 40

What are major calyces?

Answer 40

Divided into minor calyces

receive fluid outflow from many microscopic collecting tubes

Question 41

What is the function of calyces, ureter and collecting tubules?

Answer 41

To collect urine and void it into the bladder

colllecting urine from large surface area

Question 42

Where are nephrons found and what are their structures?

Answer 42

Within the cortex and medulla
Structure includes glomerular blood filtrate containing podocytes and a tubular epithelium that loops down into the medulla- Divided into proximal, intermediate and distal segment

Question 43

What events do we need to understand to appreciate the kidney development?

Answer 43

Induce different cell types
induce these in certain place of the body
Proliferation
Form branches- branching morphogenesis
Form many nephrons-2 ends need to be different
Attract blood capillaries to one end of the nephron
Form and connect tubes

Question 44

How is the definitive kidney formed?

Answer 44

Arises as results of reciprocal interactions between 2 structures, a small out-pocketing of an intermediate mesodermal structure, called the ureteric duct and adjacent mesenchyme called metanephric mesenchyme

Question 45

What does the metanephric mesenchyme form?

Answer 45

The definitve nephric tubules
Interaction between ureteric bud epithelium and nephrogenic mesenchyme is an inductive interaction
Ureteric bud induces nephrogenic mesenchyme to CONDENSE around the bud and undergo a mesenchymal to epithelial cell transition and form renal epithelium, then renal vesicles

Question 46

What do renal vesicles proliferate and differentiate to form?

Answer 46

Nephron

Proximally they fuse with bud, distally they will attract endothelial capillaries

Question 47

Facts about the nephron

Answer 47

You have 10^4 in each kidney
This is because the ureteric bud undergoes branching morphogenesis forming 10^6 renal vesicle inducing buds in each kidney

Question 48

Branching morphogenesis of the ureteric bud is governed by signals from the metanephric mesenchyme- the key steps are:

Answer 48

1. Proliferation and outgrowth of the bud ‘tip cells’
2. Arrest in proliferation of leading- edge tip cells, resulting in flattening
3. Continued proliferation of lateral tip cells,resulting in formation of cleft and 2 tips

Question 49

What is clefting in the ureteric bud of the kidney?

Answer 49

GDNF (neurotrophic factor, acts to promote proliferation, migration and outgrowth) signal required by mesenchyme
Luminal mitosis and dispersion to sides causes flattening of basement membrane
Clefting occurs as basement membrane accumulates and basment membrane holes move to the sides

Repeat again and again to form branches

Question 50

What is the receptor of the bud?

Answer 50

A receptor tyrosine kinase called Ret

Question 51

What is the sequence of events?

Answer 51

Signal from mesenchyme and epithelium - signalling pathways - gene expression - cellular response - bifurcation (reshaping)

Question 52

When the mesenchymal condensation around the bud causes a mesenchymal to epithelial cell transition

Answer 52

Ureteric tips - pretubular aggregate - renal vesicle - comma-shaped body - s shaped body - distal collecting tube/loop of henle

Question 53

How do we study this process?

Answer 53

In real time, using transgenic animals, organ cultures and sophisticated imaging
Branching morphogenesis of the ureteric bud underlies future calyces

Question 54

What happens in different weeks of embryogenesis in humans?

Answer 54

Week 6- 16 branches
Week 7- minor calyces formed
Week 32- 10^6 branches formed

Question 55

What gene is expressed in nephron stem cells?

Answer 55

TF six2
Six2 cells form the nephron and all cells within
Loss of function of Six2 depletes SC pool
Overexpression of Six2 prevents differentiation

Suggests six2 is not JUST a marker but regulates the events that keep the nephron stem cells in a self renewing state

Question 56

How do you get the nephric duct and the metanephric mesenchyme

Answer 56

Build structures called pronephrons, mesonephros and metanephros
Give clues anout evolutionary development of segmented vertebrates and evolution kidneys

Question 57

Which mesodermal line of cells do the kidneys form from?

Answer 57

Intermediate mesoderm

• line extends along the whole posterior body
• undergoes a mesenchymal to epithelial cell transition to form two structures the nephric duct and the nephric cord

Question 58

How does the nephric duct and cord develop?

Answer 58

It develops in the lumen
Duct will eventually give rise to the ureteric bud and cord will give rise to metanephric mesenchyme
Recognise them through expression of different genes
ND and NC communicate
Attempt to build new components

Question 59

What happens as the pronephric tubules degenerate?

Answer 59

1. The middle portion of the nephric duct induces a new set of kidney tubules in the mesenchyme constituting the mesenchyme or mesonephric kidney
2. Each meseonephric tubule attracts a blood supply from a branch near the aorta, ending at the capillary tuft
3. Mesonephric tubule forms a capsule around this tuft, allowing for blood filtration
4. mesenphros then largely degenerate but by then the mesenephric (definitive) kidney has been induced

Question 60

What happens in the end to the mesonephric duct?

Answer 60

Attaches to the cloaca
Helps trigger change in the local metanephric duct, causing the formation of the bud, grows into mass adjacent- intermediate mesoderm/ metanephric blastema

Question 61

Why are we keen to look at details of molecules?

Answer 61

• Provides understanding of kidney diseases
• Wnt1 was identified as a gene involved in wilms tumour (pediatric cancer) where kidney elements are incompletely differentiated instead proliferates to form tumours
• Polycystic kidney diseases

Question 62

Which 2 tissues is the lung derived from?

Answer 62

1. Ectoderm- gives rise to epithelial lining of the trachea, larynx and bronchi, alveoli through branching morphogenesis
2. Mesoderm- gives rise to cartilage, muscle and connective tissue

Question 63

What do the trachea, bronchi, broncioles and alveoli all arise from?

Answer 63

Respiratory diverticulum= for this the foregut splits into the oesophagus and trachea and the tip then begins to undergo branching morphogenesis

Question 64

Wen does the lung bud form in humans?

Answer 64

Week 4

Question 65

The respiratory diverticulum is a ventral outgrowth of the foregut endoderm, what is it composed of and what is it dependent on?

Answer 65

It is composed of endothelial, epithelial cells

The outgrowth is dependent on signals from adjacent mesoderm and mesenchyme

Question 66

What is the sac of mesoderm that surrounds each limb bud?

Answer 66

Medial edge- Viscera pleura

outer edge- parietal pleura

Question 67

Development of the human lung- day 41-44

Answer 67

• Trachea
• Right and left main bronchus
• Right middle, superior and inferior primordium
• Left superior and inferior primordium

Question 68

Development of the human lung week 9

Answer 68

Trachea
Lobes
Left main bronchioles

Question 69

Development of the human lung week 10

Answer 69

Lobes

Question 70

What drives branching? step 1

Answer 70

Endothelial, epithelial cells expressing FGF receptor respond to secreted FGF from mesenchyme nearby bud formation and extension
Exposure of tip cells to high concs of FGF induce expression of secondary genes in the tip (including genes that code for BMP, Shh and sprouty)
Turns tip of bronchial branches into signalling centres

Question 71

What drives branching? Step 2

Answer 71

• BMP4 is expressed at highest levels in the ‘leading edge’ tip cells and autonomously inhibits epithelial cells proliferation limitiing branching extension
• Shh expressed by the tip cells diffuses to the mesenchyme and inhibits FGF10 expression in the mesenchyme nearest the tip. Splits FGF10 expression promoting the next round of branching
  Sprouty limits the action of FGF10 so that branching is restricted to the tip of the branch

Question 72

Sprouty as a negative feeback loop

Answer 72

1. FGF10 induces expression of genes that direct growth and proliferation
2. Over slightly linger time-frame, FGF induces expression of another gene, sprouty
3. Sprouty inhibits FGF signalling
4. Negative feedback loop as a signal induces its own inhibitor, to limit the time of its own action

Question 73

How is branching morphogenesis an interactive process?

Answer 73

Elongation

Terminal bifurcation

Question 74

Total number of branching events

Answer 74

17 by the end of 6 months (gestation)
6 more formed during postnatal life

Step that goes on throughout development and into postnatal life

• late disruption= minor effects
• early disruption= results in hypoplasia or agenesis

Question 75

Development of tissue involved in air exchange

Answer 75

1. canicular period- 16th-20th week
2. terminal sac period- 24th weeks to birth
3. avleolar periods-late fetal thru childhood, type 2 sufactant producing cells
   Alveoli are generated they attract endothelial blood cells, which come into close contact and provide expensive capillary network required for gas exchange

Question 76

How much of your alveoli is present at birth?

Answer 76

1/6

Question 77

How do we study complex cell behaviours in 3-D?

Answer 77

1. In vivo approaches- investigate using conditional KO eg. Rac1KO phenotype in mammary gland
   - specific ablation of Rac1 in vivo results in baobob tree with massive enlarged ducts
   - Investigate how Rac1 and integrins regulate SC fate into luminal or basal compartments, through tracing of genetically mark sc using GFP reporter genes
2. Investigate in a 3-D dissected embryonic mouse lung
   - right side cultured unpertubed after dissection
   - left bronchial tip- mesenchyme removed (no braching occurs at tip as lack of FGF10)

Question 78

Apicobasal polarity

Answer 78

If a cell loses apico-basal polarity it no longer recognises the need to be an epithelium and can leave

Question 79

Branching morphogenesis happens to many tissues:

Answer 79

Lung, ureteric bud, salivary gland, prostate, mammary gland and pancreas

Question 80

What are gonadal germ cells?

Answer 80

Cells put aside in an undifferentiated state for next generation

Question 81

Which organisms can readily form new organisms?

Answer 81

Chidarians, flatworm and tunicates

Insects and vertebrates there is an early division between somatic and germ cells

Question 82

Germ cells and the next generation- 2 step process

Answer 82

1. Primordal germ cells (PGCs) are determined in a specific location just ‘in the edge’ or ‘outside’ of the developing embryo
2. PGCs migrate to the gonad and become the progenitor population for eggs and sperm

Question 83

What do you need for germ cell detemination?

Answer 83

Plastic cell type (totipotent)

A cell capable of undergoing meiosis

Question 84

How have C.elegans helped us with stem cells?

Answer 84

In early cleavage and gastrulation
asymmetical division produce a specialised cell- the p lineage cell
P cell is different to others
Depends on plane of division- determining factor
-2 daughters both identical to mother cells
- two different cells. One a progenitor and one has different determinants

Question 85

What does the P cell act as?

Answer 85

Pre-germ cell
Asymmetric division p cells inherit specialised ‘p-granules’ ( mixture of proteins and RNAs ) that are in the cytoplasm but can get into the nucleus

Question 86

What can the p- granuales do?

Answer 86

1, bind to DNA of P-cell and block almost all transcription, thus all differentiation

2. And in cytoplasm block transcription
3. Promote stem cell fate, and cause cells to undergo meiosis (rather than mitosis)

Question 87

Where does the P cell lie in vertebrates?

Answer 87

It ALWAYS lies at the posterior part of the developing embryo germ cells(= - equivalent to p cells) in all species express the transcriptional blocker

Question 88

In all vertebrates in the very earliest stages of development, a germ cell is established - this shows:

Answer 88

• no transcription or translation
  -therefore no differentiation
  These cells therefore have a ‘plastic/multipotent’ identity, also they undergo meiosis

Question 89

How do you control widespread transcriptional decision?

Answer 89

PGCs are ‘shut’ down transcriptionally/translationally
Epigenetic silencing= mechanism that governs widespread shutdown
-DNA methylation- methyl marks added to certain DNA bases to repress gene activity
-Histone modification- a combination of a different molecules can attach to tails of proteins

Question 90

Where do PGCs (progenitor germ cells) form?

Answer 90

At the posterior end in extra embryonic epiblast and initially stay there

Question 91

What is a stem cell?

Answer 91

Divides into a stem cell and a differentiated cell that becomes specialised (eg.muscle or nerve)

Question 92

What is a progenitor?

Answer 92

Like a stem cell but has a tendency to differentiate into a specific cell type
Already more specific then a stem cell

Question 93

Why does a stem cell self renew and differentiate?

Answer 93

1. self renew- maintains stem cell pool
2. specialised cell- differentiation replaces dead or damaged cells throughout your life, adds new cells through life to increase organ size or generate specific cells required

Question 94

Where is a stem cell found?

Answer 94

Embryonic SC- blastocyst at early stage

Adult SC- fetus, baby and throughout life

Question 95

How do you make specific cells from ES cells?

Answer 95

ES cells taken from inner mass inside blastocyst
Culture is lead to grow more cells (fluid with nutrients)
ES cells differentiate into all possible types of specialized cells, directed to produce one type by growing under specific conditions

Question 96

Most body (somatic) cells differentiated and not mitotic but there are stem cells or tissue specific cells

Answer 96

These are multipotent or pluripotent
Recognised first in- Bone marrow, liver, gut + skin
Now recognised in brain/muscle

Question 97

What is an adult stem cell?

Answer 97

Undifferentiated cell found in tissue and organs

Can self renew and differentiate to become most of all specialised cells types within their specific tissue lineages

Question 98

What do adult stem cells do?

Answer 98

Maintain cell population
Help you heal
play a role in ageing

Question 99

What is cellular homeostasis?

Answer 99

The ability to regulate internal conditions usually by a system of feedback controls
Constant or periodic generation of new cells to replace old damaged and dying cells
Example- pregnant females produce more RBC, continuously made throughout life in bone marrow

Question 100

What is innate regeneration capability?

Answer 100

Tissues that regenerate more readily= more prone to cancer (gut, skin)

Question 101

What are the types of adult stem cells?

Answer 101

• Hematopoietic- Blood and immune
• Mesenchymal- bone, cartilage, fat, muscle, tendon/ligament
• Epithelial- skin, gut, other lining
• Muscle
• Neural- neurons, glial, retinal

Question 102

What are specialised niches that stem cells reside in?

Answer 102

Complex micro-environments around the stem cells, made up of many cells, that interact with environment and SC to decide whether to activate

Question 103

What do hematopoietic stem cells give rise to?

Answer 103

Blood cell types:
- Myeloid= Monocytes, macrophages, neutrophils, blastopils, eosinphils, erythrocytes, megakaryoytes/platlelets

• Lymphoid=T cells, B cells, Nk cells

Found in bone marrow from early as in development, as well as in umbilical cord and blood and placental tissue

Question 104

HPCs in the complex niche- that stem cells cycle between a quiescent and an active form. How do they decide?

Answer 104

Many adjacent cells in niche provide factors to regulate stem cell activity then divide to HSC or differentiate
Sc respond to physiological signals like hormones

Question 105

What do mesenchmyal stem cells differentiate into?

Answer 105

Cartilage
Muscle 
Fat 
tendons, ligaments, connective tissues 
Located throughout body- bone marrow, fat and cord blood

Question 106

What is in a muscle stem cell niche?

Answer 106

Includes- post-mitotic, multi-nucleated muscle fibres, ensheathed by basement membrane

Complexity of SC niche increase by presence of other non-muscle, cell types including endothielial and blood cell in vasculature– motor neurons, apidocytes, fibroblasts

Question 107

What happens when ligand is presented on the muscle fibre?

Answer 107

interact with transmembrane receptors displayed by muscle stem cells to regulate stem fate

Question 108

Epithelial stem cells

Answer 108

Give rise to 60% of differentiated cells in the body
responsible for covering internal (intestinal) and external (skin)surfaces of body (including lining of vessels and glands)
found in buldge region of hair follicle cells

Question 109

What are neural stem cells?

Answer 109

Located in sub-ventricular, subgranular and hypothalamus

Neural sc give rise to neural progenitors and then neurons, oligodendrocytes and astrocytes

Question 110

How does regeneration work?

Answer 110

Adult SC remain quiescent (non-dividing) for long periods
Then they are activated by signals to maintain tissue
When activated divide symmetrical and asymmetric
through this maintain sc pool and differentiate to desired tissue