Devlopmental Flashcards

Question 1

Q

What are the two opposing theories for development?

Answer

A

Epigenesis: Progressive process where new structures are added slowly leading to the development of the whole organism.
Preformationism: organisms develop from miniature versions of themselves.

Question 2

Q

What is the germ plasm determinants theory?

Answer

A

Weismann: theory that ‘determinants’ get split up into cells unevenly as they divide. it is only the germ cels that contain all of the genome, and these self differentiate and give rise to somatic cells.

Roux experiment initially supported this mosaic determining of cell fate at cleavage, when ablate one of the two cells of the xenopus with a hot needle and still developed into a well formed half larva.

Question 3

Q

What is the induction theory?

Answer

A

One cell or tissue directs the development of another. Dreisch if divide blastomas at the two cell stage, and even 4 both will form a full sea urchin, just smaller.

Also Spemann and Mangold, grafting the dorsal lip of blastopore and inducing a second axis=organiser.

Question 4

Q

When cells are close vs when far apart?

Answer

A

Condensed vs dispersed

Question 5

Q

What does factor x do?

Answer

A

Negative feedback to inhibit proliferation.

Question 6

Q

Balance of stem cells is important why?

Answer

A

Too few: ageing and degeneration

Too much uncontrolled growth=cancer

Question 7

Q

Cell changes that cause morphogenesis?

Answer

A

Cell adhesion
Cell migration
Cell death e.g digits
Cell shape

Question 8

Q

Steps (single words) from Egg/stem cell to its final fate?

Answer

A

Specification- early comittment, if transplant will likely change fate.
Determination-more stable comittment, now if transplant will likely keep same fate.
Differentiation
Maturation- e.g. muscle fibres fast or slow depends on level of innervation they recieve.

Question 9

Q

Two opposing theories for embryo development between animals?

Answer

A

Haeckel’s Funnel theory: wrong- early all develop very simialrly then gives variety.
Von Baer’s hourglass model: Early v different e.g. gastrulation, then similar in middle section, before differentiating a lot more.

Question 10

Q

Instructive vs permissive?

Answer

A

Instructive: Instructs the fate e.g. tells the cell what action to do.
Permissive: Allows something to happen, e.g. already had some info e.g. a HOX gene, that is turned on to alter fate. (gives permission)

Question 11

Q

What is a morphogen?

Answer

A

Soluble secreted molecule acting at long distances to specify the fates of cells. Can form a concentration gradient.

Question 12

Q

Is a morphogen instructive or permissive?

Answer

A

Instructive.

Question 13

Q

How can test if the signal is a morphogen or not by working out if its instructive or permissive? (2)

Answer

A

Ectopic expression: Provide a second source of signal. If permissive the same patterning, if morphogen different fate, creating a mirror image for example.
e.g. Shh in chick wing, mirror digits.

Or make expression uniformly high, see if changes fates.

Question 14

Q

How can test if the signal is a morphogen or not by working out if it acts directly at distance? (2)

Answer

A

Genetically engineer the signal to ahve a TMD so can only work juxtacrine signalling to the next cell. If put the morphogen in the first cell in a line, if bucket brigade this will work as normal, however if morphogen cant diffuse to other cells, no patterning of further down cells.
Make one cell in the centre lack a receptor for the signal. If morphogen this one cell will not be patterned, if bucket brigade then won’t matter.

Question 15

Q

What is meant by a morphogen working directly at distance?

Answer

A

A gradient is created away from the source, which impacts the cells. If not may work in a Bucket brigade (chinese whispers) like way, signalling to the next cell.

Question 16

Q

As well as passive diffusion what else helps to establish the gradient of morphogens?

Answer

A

Binding to molecules in the ECM e.g. heparin sulfate proteoglycan, and if want a steep gradient, degradation over distance, and high conc of receptors to amplify the signal.

Question 17

Q

How can heparin sulfate proteoglycan regulate morphogen diffusion? (2)

Answer

A

Binds many ligands e.g. Sequestering and slowing BMP, or facillitating the diffusion of Hedgehog.

Question 18

Q

How can morphogens travel through cells?

Answer

A

Planar transcytosis.

Cell can endocytose into a pit coated vesicle

Question 19

Q

Evidence that morphogens travel through cells?

Answer

A

If block vesicle formation caused Dpp to ask juxtacrinely.

Question 20

Q

How does timing play a part in morphogen induction?

Answer

A

Poorly understood, but likely the receptors respond to the signal when it gets to a steady state.

Question 21

Q

Transcriptional read out model?

Answer

A

Higher conc of morphogen, leads to higher conc of activated transcription factor (moving it into the nucleus).

Question 22

Q

How else is the expression of genes controlled as well as concentration of morphogen (transcriptional read out model) lead to differential differentiation intrinsically and autonomously?

Answer

A

Affinity of enhancers
e.g. if receptors see only low levels of transcription factors and the enhancers have a low affinity definitely no transcription will happen, whereas if both high lots of transcription will occur. So two cells could see the same concentration of transcription factor but one could have the genes expressed if high affinity, whereas other not if has low affinity enhancers.

Question 23

Q

Name an example of a signal that is both a morphogen and a transcription factor?

Answer

A

Bicoid mRNA is localised at the anterior of the egg and is translated into protein during early embryogenesis. Bicoid protein then diffuses through the cytoplasm and accumulates in nuclei of the syncytial blastoderm generating a concentration gradient.

Question 24

Q

How else is the expression of genes controlled as well as concentration of morphogen (transcriptional read out model) lead to differential differentiation non-autonomously?

Answer

A

Negative feedback crosstalk
if one cells genes are activated, it can also code for a repressor and repress neighbouring cells, to create differences.

Question 25

Q

How are strict thresholds achieved when the gradient is not steep?

Answer

A

Positive feedback, once weakly activated the gene may code for a transcription factor which feeds back to activate its own expression, thus amplifying it.

Question 26

Q

Epiblast and hypoblast equivalent to … and .. in the xenopus

Answer

A

Epiblast: Animal
Hypoblast: Vegetal

Question 27

Q

How is the egg already polarised in xenopus before fertilisation?

Answer

A

due to gravity, heavy yolk sinks down, whereas the pigment cortex is more animal.

Question 28

Q

First cleavage in the xenopus?

Answer

A

Asymmetric. All of the cytoplasmic components sink to the vegetal (bottom) cell.

Question 29

Q

hypoblast or epiblast goes on to form the ICM?

Question 30

Q

What do the vegetal cytoplasmic components of the xenopus cell do?

Answer

A

Act on the DNA to regulate gene expression e.g. some are DNA binding proteins. As a result certain transcription factors are turned on in vegetal hemisphere cells.

Question 31

Q

In the xenopus what causes the formation of the blastocoel?

Answer

A

Changes in the osmolality cause an influx of water creating the fluid filled blastocoel.

Question 32

Q

After the sperm enters what is the next event to happen?

Answer

A

30degree cortical rotation.
Sperm entry into ventral cortex causes the cortex to become loose from the cytoplasm so it can move. Dorsalising factors are activated and through the actin filaments in the microtubules causes relocation of maternal proteins.

Question 33

Q

What are the dorsalising factors in the xenopus during cortical rotation?

Answer

A

wnt and dishevelled, Wnt binds to frizzled receptors in cells, which leads to activated Beta Catenin, leading to upregulation of these genes.

Question 34

Q

What forms opposite the sperm entry of the xenopus embyro?

Answer

A

differentiation of the organiser.

Question 35

Q

From the dorsal part of the xenopus embryo what factor is secreted? leading to?

Answer

A

Wnt, which binds to Frizzled, and eventually causes the accumulation of Beta-catenin turnin gon Wnt genes in the dorsal quadrant.

Question 36

Q

The dorsal of the embryo will become future…

Answer

A

posterior

Question 37

Q

Relevence of the dorsal region in development stage?

Answer

A

The dorsal lip/ blastopore folds inwards in gastrulation.

Question 38

Q

How do transcription factors work?

Answer

A

gene is transcribed as mRNA in the cytoplasm and then translated into a protein which can be secreted or autonomously migrated back to the cells nucleus to bind to promoters and enhancers of genes to alter transcription.

Question 39

Q

…….. accumulates dorsally in the xenopus embryo, whereas ….. vegetally

Answer

A

Beta- catenin

TGF B signal (Nodal or Vg1)

Question 40

Q

Vegetally ……. located in vegetal nuclei transcriptionally activates …….. in the xenopus.

Answer

A

VegT (to Veg1)

Nodal

Question 41

Q

Nodal is a what? Function?

Answer

A

secretory Morphogen, which sets a gradient across the animal hemisphere for gastrulation.

Question 42

Q

What is Nodal’s mode of action?

Answer

A

Cells that contain receptors for Nodal respond by the Receptor Serine Threonine Kinase Type 1 and 2’s dimerizing and phosphorylating Smad 2/4, which translocates into the nucleus and leads to the induction of target genes such as Nodal, Lefty, the antagonist of nodal Cerberus, to cause differentiation of the 3 germ layers.

Question 43

Q

Cells that see high Nodal will become….
Low Nodal….
No Nodal…

Answer

A

In a gradient Vegetal to animal, so those most vegetal in the animal hemisphere (or epiblast) become Endoderm. Low levels become Mesoderm and no Nodal cells become Ectoderm.

Question 44

Q

Why is the hypoblast so important in gastrulation?

Answer

A

It is the hypoblast that signals to the epiblast via morphogens such as Nodal, to differentiate into the 3 germ layers.

Question 45

Q

From a coronal view of the epiblast what is happening during gastrulation?

Answer

A

The cells of the mesoderm undergo an epithelial to mesenchymal transition and invaginate and drop down into the middle layer causing the formation of the primitive streak.

Question 46

Q

As well as low levels of Nodal what other transcription factor is expressed in mesoderm that can show its mesoderm?

Answer

A

Brachyury

Question 47

Q

Where both ….. dorsally and ……vegetally overlap what develops?

Answer

A

Beta- catenin
Nodal
The Nieuwkoop centre.

Question 48

Q

How is the Nieuwkoop centre induced?

Answer

A

Where both high Nodal signalling (P Smad 2/4 effector) and B-catenin (Wnt effector) vindn to the promoter elements, zygotic genes such as Siamois and later Goosecoid are activated. These are characteristic of the Nieuwkoop centre.

Question 49

Q

What does Siamois do in the Nieuwkoop centre?

Answer

A

T.F. which causes the upregulation of the gene goosecoid (Gse) by binding to the promoter region, not only in the Nieuwkoop centre itself but also just animal to in the dorsal mesoderm. Causing the formation of the organiser.

Question 50

Q

The high Nodal and Wnt signals the organiser to express what transcription factors?

Answer

A

Siamois, Goosecoid, Chordin, Xlim, Xnot etc.

Question 51

Q

What does the organiser/node do?

Answer

A

secretes BMP inhibitors e.g. Chordin, Noggin to Dorsallises the neighbouring mesoderm and neuralise the overlaying ectoderm.

Question 52

Q

Under the transcription factors of …. and ….., the node self-differentiates into? How?

Answer

A

Siamoid and Goosecoid
Axial mesoderm
These TF go back into the nucleus, binding to promoters causing the differentiation. Under slightly different concentrations of, the A/P axis is established.

Question 53

Q

What movements does the node do when self-differentiating?

Answer

A

Migration by convergent extension into a long thin rod underlaying the midline of the ectoderm. The Pre-cordal mesoderm migrates first anteriorly, and then the notocord posteriorly.

Question 54

Q

What transcription factors are expressed in a gradient along the A/P axis of the axial mesoderm?

Answer

A

Wnt and Retonoic acid are highest posteriorly, giving the posterior characteristics of the hindbrain, as differrent HOX genes are turned on.

Question 55

Q

intermediate mesoderm (in terms of dorsal to ventral), induced by BMP inhibition from node, goes on to form..?

Answer

A

somites and heart

Question 56

Q

Ventral mesoderm forms?

Answer

A

Blood and kidney

Question 57

Q

Dorsal mesoderm forms?

Answer

A

Notocord (self differentiated node)

Question 58

Q

What is the structure that runs anterior to posterior thats formed during gastrulation?

Answer

A

The primitive streak, with hensons node which progreses posteriorly.

Question 59

Q

What happens along the primitive streak during gastrulation?

Answer

A

The mesoderm undergoes an epithelial to mesenchymal transition and migrates down (ventrally) and laterally under the overlaying ectoderm.

Question 60

Q

After gastrulation what happens to the node?

Answer

A

It self differentiates into axial mesoderm, made of notocord and precordal mesoderm.

Question 61

Q

what are the three types of mesoderm found in a coronal cross section through the primitive streak?

Answer

A

Paraxial mesoderm, most medial, either side of the neural tube.
Intermediate mesoderm, ventral to and slightly lateral
Lateral mesoderm, furthest lateral in a C shape.

Question 62

Q

What does paraxial mesoderm go on to form?

Answer

A

Head and somites from.

Question 63

Q

what does the intermediate mesoderm go on to form?

Answer

A

Urogenital system- kidney nd gonads.

Question 64

Q

What does the lateral mesoderm go on to form?

Answer

A

Circulatory system e.g lungs and somatic cells. and extraembryonic tissues.

Answer 64

A

Sclerotome (cartilage) 
Syndotome (tendons) (people with a syndrome tend to..)
Myotome (skeletal muscles)
Endothelial cells
Dermatome (Dermis)

Answer 65

A

The anterior and posterior ahve different fates, the posterior segments into somites, whereas the anterior is unsegmented.

Answer 66

A

Segmented paraxial mesoderm.

Answer 67

A

Engrailed1

Answer 68

A

vertebrae.

In humans some vertebrae fuse- from 33 at birth to 24 in adulthood.

Answer 69

A

Yes, but not individuals. 
Humans: 38-44
chicks: 55
Mouse: 65
Zebrafish:33

Answer 70

A

Pairs
Anterior
Posterior
Node

Answer 71

A

90minutes,

2 hours.

Answer 72

A

Clock Wave- front model. A molecular oscillator, where cells hit the travelling wavefront and have an abrupt chnage in property and become somites.

Answer 73

A

The periodicity of C-Hairy every 90mins, correlated with the addition of a new somite in chicks. Cooke et al 1976

Answer 74

A

Negative feedback mechanisms

Short half life

Answer 75

A

Retinoic acid from the anterior anatagonises so the presomatic region continously getting longer.

Answer 76

A

Between the node and the last formed somites cells, before the paraxial meso is converted to somites

Answer 77

A

Position of the last somite-2

Answer 78

A

Notch family genes are expressed and at a somite boundary these are inhibited by lunatic fringe Glycosyltransferase enzyme.

Answer 79

A

Mesenchymal to epithelilal transition.

Answer 80

A

Anterior: Retinoic acid gradient
Posterior: FGF/wnt

Answer 81

A

when FGF/Wnt levels drop below a threshold level, then gene expression is turned on, to cause somatogenesis

Answer 82

A

Glycosylation affects the ability for the extracellular domain of Notch to bind to the ligand delta, so creates a negative feedback loop.
Therefore causes the formation of a boundary between somites.

Answer 83

A

Stem cell, myoblast, myotube, myofibre

Stem cell- specification/determination, loss of pluripotency-> Muscle progenitor cell myoblast- differentiation-> Myotubes-maturation->myofibres

Answer 84

A

Specification/determination, muscle specific genes turned on such as MyoD, Myf5, MRF4.

Answer 85

A

A demethylating agent that can drive stem cells to differentiate into myoblasts.
By removing the methylation of histones, which repress the muscle specific genes being expressed.

Answer 86

A

Treat a fibroblast (already differentiated cell) with 5Aza.
extract the mRNA, and reverse transcriptase into cDNA.
Screen the cDNA for muscle specific genes using myoblast specific probes.
compare results with a control.

Answer 87

A

If treat already differentiated cells such as nerve cells, fat, fibroblasts etc, with MyoD along with an active viral promoter, they get a myotube fate.
With muscle specific receptors and proteins, and become multinucleate.

Answer 88

A

They are basic helix- loop helix proteins.
They have a basic domain- which binds DNA to, and a helix-loop-helix domain which causes dimerisation with E12 or E47 proteins, whcih act as a co-factor for transcription activation.

Answer 89

A

Nothing, it is compensated by Myf5 and Mrf4, in which it acts redunantly with.

Answer 90

A

it is a transcription activator which binds to the E-box sequence of enhancers to drive transcription of genes e.g. muscle specific genes have this specific e-box in.
Forms dimer with E12 or E47 too.
CANNTG sequence.

Answer 91

A

skeletal muscles

Pax3

Answer 92

A

Signals from adjacent tissues,
e.g. Wnts from the doral enural tube and ectoderm and BMP4 from the lateral mesoderm cause formation of the dermomyotome.
Whereas Shh from the notocord and floorplate cause the formation of the sclerotome.

Answer 93

A

Shh Signals from the notocord and floorplate, which causes the sclerotome to express PAX1 and undergo a mesenchymal to epithelial transition and migrate laterally.

Answer 94

A

Sclerotome

Answer 95

A

BMP4 from lateral mesoderm signals and Wnts from the dorsal neural tube and ectoderm.
Dermomyotome forms a flat sheet- dermis, while other cells migrate away MET to become the myotome.

Answer 96

A

Epaxial- more medial, higher Shh and Wnt

Hypaxial- more lateral, high Wnt and BMP4.

Answer 97

A

Abdominal and limbs
Splotch mutant lacks Pax3 and lacks limb muscles.
(normally high in Pax3, which induces c-Met expression

Answer 98

A

Dermomyotome.

Answer 99

A

Myogenic regulatory factors- can tell by doing a blue insitu hybridisaion ane expression correlates to skeletal muscle.

Answer 100

A

deep back muscles (more dorsal)

Answer 101

A

Pax3

Pax1 present

Answer 102

A

Redundancy with MyoD so little difference, just delay in myotome formation.

Answer 103

A

No skeletal muscle present, and no myoblasts.

Answer 104

A

Mice unable to take their first breath so die shortly after birth, as there is no diaphragm.

Answer 105

A

Wnt and Shh

myf5

Answer 106

A

Wnt and BMP4
MyoD and Myf5
BMP4 induces Pax3, and represses Myf5 and MyoD in cells fated to migrate
in the limb bud.

Answer 107

A

It expresses Pax3, which drives C-met receptor expression, which is a RTK to Scatter factor (or hepatocyte growth factor HGF) in the limb mesenchyme, which acts as a chemoattractant for the somite cells to the limb.

Answer 108

A

Fusion requires integrin B on the cell membrane, and structural reorganisation of Multinucleate myotubules.
Myogenin also expressed.
Growth factors inhibit, as promote myoblast proliferation, and not differentiation.
Without, it withdraws from the cell cycle under P21 (myogenin and MyoD activate transcription of)

Answer 109

A

it then differentiates, Myf5 and MyoD determination.

Answer 110

A

Lose ability to repair muscles in adulthood.

Answer 111

A

Delamination, Migration, Proliferation, determination, differentiation

Answer 112

A

under basal lamina in the extracellular matrix of all muscle fibres.

Answer 113

A

Myf4
Maturation decides whether short or fast fibres, and the muscle expresses proteins such as actin, tropomyosin, creatine phosphate etc.

Answer 114

A

Where the retinoic acid gradient from the anterior meets the FGF and Wnt gradient from the posterior = the level of the determination front.
This is when there is an arrest in oscillations of Wnt and FGF8.

Answer 115

A

By Mesp2, RA activates expression of, which inhibits FGF8. But also are morphogens which just gradually diminish over distance.

Answer 116

A

Absense of Notch signalling.Spondylocostal dysplasia, ossificaion centres of vertebrae dont align due to the misalignment of somite formation.

Answer 117

A

C-Hairy1 -> Lunatic fringe -> Notch1 -> ephrins -> cell adhesion changes

Genes that encoding C-Hairy are periodicially activated then inactivated in the posterior mesoderm. When high levels are detected this activates Lunatic fringe, which works to inhibit Notch
(mesenchymal to epithelial cells condense together)

Answer 118

A

Oscillation slows down as cells mature
Acquisition of anterior and posterior identity:
Notch1 and Dl1 in post.
Notch2 and Dl3 in ant

Answer 119

A

bHLH transription factor

Answer 120

A

It creates a boundary between RA anterior and Wnt and FGF8 posterior which initiates somite formation. Cells posterior to the determination front are maintained in a non-determined state by FGF activity, whereas those anterior initiate the formation.

Answer 121

A

Theory holds that the size of each somite is defined by the number of mesodermal cells that pass the determination front between these two opposing signalling domains during one cycle of the segmentation clock.

Answer 122

A

Mesp2 is only expressed in the anterior half of the somite,anterior to the determination front, as Notch from the anterior activates Mesp2 via TbX-6.
Whereas Mesp2 is low posterior to the determination front, as Mesp2 is inhibited by FGF and Ripply2.

Answer 123

A

Induces boundary formation, by activating Ephrin and E cadherin signalling, causing epithelialisation and the formation of a furrow.

Answer 124

A

Proximal near shoulder, distal at phalanges, anterior thumb, posterior little finger. Dorsal back of hand, whereas palm is ventral

Answer 125

A

A limb bud.

Answer 126

A

T-box
Tbx5 specifies the forelimb in mouse, or wing the case of drosophila (induced by Pitx1)
Tbx4- hind limb- leg

Answer 127

A

If force transcription factor expression of other limb, that limb will form- sufficient.

Answer 128

A

Differential HOX genes along the anterior to posterior axis, which cause differential gradient of Retinoic acid (highest anteriorly) which leads to the different T-box genes being activated.

Answer 129

A

If ectopically put an FGF bead in a flank region not destined for limb formation early, an ectopic limb appears.
Depending on proximity to which limb, this could be either a forelimb or a hindlimb.

Answer 130

A

expressed in the hindlimb, and is thought to determine the differences in hindlimb and forelimb

Answer 131

A

TBX5- mutation in humans causes Holt-Oram syndrome defects in upper limbs and heart
PITX1- mutation associated with lower limbs required for TBX4 expression

Answer 132

A

control local production of FGFs that initiate limb developement, FGF10 is the ligand.

Answer 133

A

Mice lack limbs

Answer 134

A

Apical Ectodermal Ridge- essential for limb bud formation (FGF8)
Zone of polarizing activity-determines pattern along the anterior posterior of the limb.

Answer 135

A

FGF10
FGF8 in the overlying ectoderm
FGF10 in the proximal mesoderm

Answer 136

A

Truncation in growth of the limbs, the earlier its removed the bigger the impact. Reduced proliferation in this area and more cell death.
3days- develop only the proximal bones
3.5days- proximal and distal but no digits
4days- only truncated digits

Answer 137

A

Distal

the progress zone moves ditally as the limb grows

Answer 138

A

Progress zone model- amount of time in determines fate
Two-signal model- Proximal signal from paraxial meso antagonises the distal gradient from AER giving differential expression,

Answer 139

A

Progress zone model- amount of time in determines fate
Two-signal model- Proximal signal from paraxial meso antagonises the distal gradient from AER giving differential expression, (correct)

Answer 140

A

Retinoic acid from the proximal paraxial mesoderm, and FGF and Wnt from the AER.
Retinoic acid drives expression of Meis homodomain genes which is required for proximal fate.
And FGFs drive expression of HOX11 and 13 (most distal), which give distal fate.

Answer 141

A

Limb abnormalilites as normally in proximal

Answer 142

A

By the Zone of polarising activity which acts as a source of the Shh morphogen gradient from the posterior.

Answer 143

A

Mirror image duplications of digits forms e.g. in chick 4,3,2 -> 4,3,2,2,3,4

Answer 144

A

Complete loss of distal skeletal elements and single bone of ulna and radius(zeugopods), as this sets the anterior to posterior axis.

Answer 145

A

Humerus: stylopod
Ulna and radius: zeugopods
Digits: autopod

Answer 146

A

1/4 of UK deaths a year, 1 person has a myocardial infarction every 3 mins in UK.
Costs NHS £11billion a year

Answer 147

A

800

1/3 of babies deaths before 1

Answer 148

A

Over half, 548/929 - 550/930

Answer 149

A

Vertebrates it happens immediately after gastrulation e.g. human and mouse at around 6-12 hours.
Drosophila later, delay for mesoderm to form.

Answer 150

A

The Ventro-lateral mesoderm, called the Splanchnopleura (the Ventral bottom part of the lateral C shaped mesoderm) or Splanchnic lateral plate mesoder,

Answer 151

A

First heart field (cardiac crescent)

Answer 152

A

Makes the open cuved tube heart scaffold, low proliferative capactiy,
Forms two layers of cells: the inner endocardium and the outer myocardium.

Answer 153

A

The tube elongates and becomes divided transversely nto the atrial and ventricular chamber. Epicardium forms to surround the myocardium.

Answer 154

A

Looping into a multichambered heart.

Answer 155

A

first heart field earlier: cardiac muscle cells of the primitive left ventricle, and myocardial cells of the outflow tract.
Second heart field: elongation of the early heart tube causing looping, and formation of the separate chambers later.

Answer 156

A

The second heart field myocardial cells lie medially and posterior to the first heart field cells.

Answer 157

A

Develops slightly later but has a high proliferative capacity.

Answer 158

A

Angiogenic cell clusters- on the heart plate.
These angiogenic cell clusters coalesce to form right and left endocardial tubes at around day 21.
Heart formation

Answer 159

A

Mesodermal precursor (splanchnic mesoderm) specification by Dpp-> causing expression of the transcription factor Tinman.
Cardioblast differentiates under DMef2 into a cardiomyocyte.
Expression of Pannier is upregulated creating a linear heart tube as the two endocardial tubes fuse together
Linear heart tube further differentiates into the dorsa;l vessel.

Answer 160

A

Mesodermal precursor (splanchnic mesoderm)is specified as BMP induces the NKX2.5 transcription factor
A cardioblast is formed, which under MEF2C, which causes muscle differentiation, differentiates into a cardiomyocyte
Under GATA4 the cardiomyocyte (endocardial tubes) migrate ventrally and fuse into a linear heart tube.
inv and iv expression causes the looping of the heart tube.
dHand and eHand causes the final multichambered heart formation

Answer 161

A

mesoderm

Dorsal vessel heart tube.

Answer 162

A

NK-2 family, with Nkx2.5 specifically found in the cardiac crescent.

Answer 163

A

Do form a heart (compensatory mechanism?) but the looping is often defected.
(human congenital heart malformations

Answer 164

A

Electroporate BMP genes ectopically in Chick, or bead soaked in BMP2 anterior to the primitive streak.
Nkx2.5 induced in the paraxial mesoderm,

Answer 165

A

The tissue posterior isnt permissive to the signal, and posteriorly BMP inhibitors are secreted from the posterior notocord. Also anterior neural plate secretes Wnt inhibitors (dkk and Ceberus) which stops the Wnt inhibiting the BMP like in the posterior.

Answer 166

A

Angiogenic cell clusters go on to form bilateral endocardial tubes and dorsal aortas with epimyocardial cells around

Answer 167

A

As they migrate medially epimyocardium surrounds them. They then migrate ventrally below the foregut, and fuse into a single endocardium, surrounded by epimyocardium.

Answer 168

A

DMef2 (drosophila Mef2)

Is required, as no tinman no Mef2

Answer 169

A

Endocardium contains precursors of endothelial lining of heart and cushion cells that form valves.

Answer 170

A

Myocardium contains myocytes of atria and ventricles, and Purkinje fibers

Answer 171

A

Mef2 proteins contain both MADS-box and Mef2 DNA-binding domains. DNA binding causes the dimerisation

Answer 172

A

It causes muscle differentiation, so a mutation causes the loss of differentiation,

Answer 173

A

Mef2c

-/- no heart looping, no right ventricle, upregulation of Mef2B as compensation.

Answer 174

A

Zinc finger domain.
GATA1-3 role in hematopoiesis
GATA 4-6- Cardiogenesis (GATA 4 earliest expressed)

Answer 175

A

Fail to form the heart tube, as the endocardial tubes dont fuse. PLays a role in driving ventral migration CARDIA BIFIDA

Answer 176

A

Growth factor. Bone morphogenetic protein.

Answer 177

A

a morphogen.

Answer 178

A

BMP Dorsal (roofplate and ectoderm), and Shh ventrally (floorplate and axial mesoderm). This is converted into GliR dorsally and GliA ventrally.

Answer 179

A

Pax3,6 and especially important Pax7 and Lim1 which lead to formation of Dorsal progenitors fate of dorsal cells.

Answer 180

A

Pharyngeal

Answer 181

A

Previously thought the BMP acted as a morphogen but now evidence suggests that many different types of BP’s diffuse varying differences giving different transcriptional profiles.

Answer 182

A

It is made in the notocord and floor plate and secreted in a gradient away MORPHOGEN. -> GliA

Answer 183

A

Covergent extension following a fibronectin rich pathway that binds to integrins expressed by organiser cells.

Answer 184

A

GliR represses Nkx 6.2, NKX2.2 and Nkx 6.1, but ventrally this is converted to GliA, so these are disinhibited immediately dorsal to the floorplate
FoxA2 is expressed in the floorpalte.

Answer 185

A

RX, srx3, Pax6.

Answer 186

A

A Shh expressing flooplate like structure, which is induced by Shh from the precordal mesoderm.

Answer 187

A

Division of the eyefield in two. The Shh supresses Pax6, RX expression in the centre of the embryo eyefield.

Answer 188

A

Cyclopia or holoprosencephaly- failure for the ventral tube to close

Answer 189

A

In Anterior neural plate

Answer 190

A

Eyefield grows sideways and contacts surface ectoderm laterally forming a T like shape with two optic vesicles from the neural ectoderm diencephalon.
Optic vesicle induces the lens placode in the surface ecoderm overlaying.
Ectoderm thickens (e.g. optic placode) and the membrane starts to invaginate in.
The optic vesicle invaginates around the optic placode which is also invaginating inwards.
Eyefield forms a double layered cup, with the inner forming the neural retina, and outer the pigmented epithelium.
Lens vesicle dettatches from the surface ectoderm as it invaginates in making a tube with the cornea over.

Answer 191

A

5 vesicle stage- e.g telencephalon, diencephalon, mesencephalon, metencephalon, myelincephalon
22 days.

Answer 192

A

By the optic stalk which will become the optic nerve.

Answer 193

A

Neural ectoderm/ Neuroepithelium: Retina and Retinal pigment epithelium
Surface ectoderm: lens, Cornea
Migrating cells: Sclera, A. chamber (fluid filled space between the iris and cornea)

Answer 194

A

As optic vesicle grows out it contacts the surface ectoderm and induces thickening.into the optic placode.

Answer 195

A

Neural to optic vesicle-> epidermis to lens placode/optic-> induces involution and invagination of optic vesicle into 2 layer cup -> signals to lens placode to pinch off into lens and diffentiate -> Optic vesicle becomes neural and pigmented retina -> lens vesicle induces overlaying ecto to become the cornea.

Answer 196

A

Pinches off to form a hollow ball of cells that is stem-like, capable of self renewal anteriorly or fibre-like cells that elongate from the posterior.
They make lots of transparent crystallin and get rid of their nucleus

Answer 197

A

outer: Retinal pigment epitheliium- produce melanin give colour
inner: neural epithelium, stem like pop, ganglion cells, bipolar, photoreceptors etc

Answer 198

A

astrocyte cells, bt turns into the optic nerve.

Answer 199

A

Necessary for eyeformation, can cause ectopic eye growth

Answer 200

A

Insert PAX6 from mouse in Drosophila and normal drosophila eye forms.

Answer 201

A

Early: in eyefield

Maintained in forming retina and play a role in stem cell maintainance and differentiation

Answer 202

A

1 cell wide neuroepithelium, when these proliferate they migrate away from the ventricle.

Answer 203

A

1 cell wide initially. Initially these are symmetrical division, then radial glial like. Asymmetric divison, the neuron uses the radial glial cell to migrate away from the ventricle.

Answer 204

A

From 5 weeks the outer neuroblastic layer signals to the inner neuroblastic layer to form at 6-7 , then to innermost at 7-8weeks.

Outer neuroblastic- rods and cones
Inner- bipolar
Innermost- ganglion
with synapses between

Answer 205

A

Virus containing a functional Bgalactosidase gene injected intothe back of a newborn rat to infect some of the retinal precursor cells.
After a month-6weeks, the eye is removed and retina stained for B-galactosidase and found.

Answer 206

A

bHLH TF’s:

Chx10 promotes bipolar cells( inner neuroblastic layer), whereas Prox1 is involved in horizontal cell fates.

Answer 207

A

Age-related macula degeneration.

Neuones in the eye can degenerate and stem cel numbers decline over age

Answer 208

A

transplant stem cells into patients and see if regenerate.

Answer 209

A

A stem- cell like population, which can either self renew or differentiate into ganglion, interneurons, photoreceptors etc

Answer 210

A

Changes in cell fate: neural to optic vesicle
Invagination- of the optic cup, cells need to change shape to go from a columnar rectangular shape to a triangular.
Involution- optic vesicle to optic cup, growing larger than area to take up.
Pinching off- lens vesicle from epithelium placode. ETM
Migration- lens moving inwards

Answer 211

A

ureter to renal pelvis, to major calyces to minor- nephrons

Increasing surface area

Answer 212

A

Nephric duct- bud

Nephric cord- mesenchyme

Answer 213

A

Intermediate mesoderm running bilaterally down the posterior of the body

Answer 214

A

Pronephros-24days near heart
Mesenephros-25days midway down
Metanephros-26 days

Answer 215

A

Intermediate mesoderm undergo a MET to form bilateral nephric Ducts (Anterior) and cord (posteriorly)
The duct forms a lumen and expresses PAX2.
The duct Tries to bud at 24days (pronephros), 25days (mesenephros) and 26 days (metanephros) =uroteric bud.
A uroteric bud grows towards and induces the nephrogenic mesenchyme to condense (was cord earlier)
Mesenchymal to epithelial transition to renal epithelium then renal vesicle, then proliferates into S-Shaped body towards to uroteric bud (collecting duct)
Defined apoptosis and enables the two to fuse, as the S-shaped body elongates into a long tube (by proliferation and differentiation)
Local signals for angiogenesis via chemoattractants and angiogenic factors, so capillaries form around, making the glomerulus
The nephron then folds to make the final PCT, loop of henle DCT and BC

Answer 216

A

10^6.
Branching morphogenesis- uroteric bud braches off.
e.g. week 6: 16 branches, week 7- minor calyces formed, week 32: 10^6

Answer 217

A

Initially proliferation and outgrowth of the uroteric bud ‘tip cells’ under GDNF (to Ret RTK) from the metanephric mesenchyme.
Arrest in proliferation of the tip cells creating a flatterned cleft
Continuing growth of lower down cells which create T shape which keeps extending laterally.
This makes new tip cells of two separate buds, which can either bud again or join to nephrons.

Answer 218

A

Transgenic animals e.g. GFP transgene to HOXB7 can visuallise the uroteric bud and can see branching.

Answer 219

A

Six2, which regualtes stem cells in self-renewing state.

Answer 220

A

Gain: Prevents differentiation in kidney stem cells
Loss: depletes stem cell pool

Answer 221

A

Pronephros- apoptosis and broken down

Mesonephros- some blood vessels form near etc but differentiate into other strucutres.

Answer 222

A

Endoderm: epithelial lining of the trachea, laynx, bronchi
Mesoderm: cartilage, muscle and connective tissue

Answer 223

A

Respiritory diverticulum off the ventral foregut

Answer 224

A

Respiritory diverticulum buds off the ventral foregut.

This then forms the trachea and inferiorly undergoes branching morphogenesis to form the lung buds

Answer 225

A

outgrowth from the foregut endoderm induced by adjacent mesodermal mesenchymal cells

Answer 226

A

A sack of mesoderm, inner will become the visceral pleura and the outer the parietal.

Answer 227

A

day 41-44: first two bronchi
week 10: miniature but all formed, got all 5 lobes
6months: 17 branching events
and 6 more post natally until 23 total 2^23 =8million

Answer 228

A

Overlaying mesoderm secretes FGF10 which the endothelial epithelial cells respond to bud towards.
In the tip cells high FGF induces signalling cascade, resulting in MAP Kinases.
Secondary genes are turned on such as Shh, BMP4, Sprouty and genes encoding signals, making this now a signalling centre.
BMP4 levels are highest in the leading tip, and these act autonomously to inhibit thier proliferation, causing the flatterning of the bud.
At the same time Shh diffuses to the mesenchyme and inhibits FGF10 expression in the mesenchyme nearest to the tip.
Sprouty limits the action of FGF signalling so there is only branching at the tip.
Where there is still high levels of FGF10 either side, new tips are made either side causing the T shaped branching.

Answer 229

A

There is a lag between the tip cells proliferating under FGF10 (induces expression of cyclins) and it inducing expression of the genes Shh and Sprouty to inhibit it.
Negative feedback loop

Answer 230

A

induces the expression of cyclins which promote the cell cycle

Answer 231

A

Canonical Wnt signalling reinforces FGFR2B (FGF10 R) expression in the epithelium, whereas non-canonical WNT5 signalling inhibits FGF10 expression.

Answer 232

A

BMP4 signalling by the tip epithelium restrict FGF signal transduction and branching, whereas mesenchymal BMP4 enhances local branching

Answer 233

A

Canalicular period- 16-26weeks
Terminal sac period- 24 weeks
Alveolar period- late fetal to childhood

Answer 234

A

FGF acts as angiogenesis factor, attracting endothelilal blood cells to form the capillary network. Surfactant producing cells added. also.

Answer 235

A

Rac1

Conditional K/O- baobab duct phenotype with massively enlarged ducts.

Answer 236

A

Ras-related GTPase that regulates many cell movements and differentiation etc.

Answer 237

A

Found raised levels linked to carcinomas, formation of lamellae as a result of which can use to migrate and metastasis-ise. Therapeutic drug target?

Answer 238

A

If remove the mesenchyme from lung tissue in vitro no branching happens here due to a lack of FGF10.

Answer 239

A

Key places for cancer where there is branching e.g. lungs, mammary glands, pancreas, prostate etc

Answer 240

A

set of undifferentiated cells set aside in the embryo that give rise to the reproductive gametes enabling the next generation

Answer 241

A

Primordial germ cells are determined in a specific location in extra-embryonic structures posteriorly but later migrate to the gonads.

Answer 242

A

totipotent

- capable of meiosis

Answer 243

A

P lineage cells in the c elegans-P granules in. posteriorly accumulate.

Answer 244

A

Block transcription by binding to the P-cell DNA e.g. epigenetic (no proteins no differentiation)
Block translation in the cytoplasm
Promote a stem cell fate- cause cells to undergo meiosis

Answer 245

A

Vertebrates posterior between the epiblast and hypoblast, in the extra-embyonic tissue where they are protected from differentiation signals.

Answer 246

A

Passively travel in the endoderm moving up the gut (as forms by convergent extension) until chemoattractive/repulsive signals cause movement into the gonadal niche laterally along with the gonad precursor cells.

Answer 247

A

Microenvironment that protects the stem cells in an undifferentiated state.

Answer 248

A

in ovaries the cells attatch to the stromal cap, whereas in testes the hub cells.

Answer 249

A

Teratoma forms- chaotic development of lots of different cell types, can be coming out of bottom or mouth

Answer 250

A

In the travelling stem cell niche, with support cells.

Secretes stem cell factor (SCF)

Answer 251

A

Following a fibronectin trail with chemoattractants (Sdf-1) required.

Answer 252

A

Inner cell mass of an embryo(of blastocyst 50-100cells big), then cultured in a lab under conditions to maintain stem cell-ness

Answer 253

A

Progenitors are not totipotent, rather multi as they have a limited number of cell types can become e.g. satellite only muscle.
Also, progenitors have a limited number of times it can self renew, whereas stem cell endless

Answer 254

A

4, 1
so 1/5 self renew
Either make two stem cells when divide or two specialised cells now think- so 1/5 divisions make two stem cells.

Answer 255

A

Replaces damage/dead cells
or adds cells e.g organ growth
or generate cells needed at specific time in development in life e.g. puberty

Answer 256

A

Bone marrow,gut, skin also brain, liver , muscles

Answer 257

A

Can’t: RBC’s, skin, gut lining (nearly all differentiated cells)
Can: stem cells, T-cells, liver cells (rare- stem cells therefore v important for repair, replacement etc, ften from progenitors)

Answer 258

A

100,000 million.

From hematopoietic stem cells in the bone marrow (make blood and immune cells)

Answer 259

A

The constant repairing of old or damaged cells,or addition of new cells as needed

Answer 260

A

Bone, cartilage, fat, muscle

Found in bone marrow, fat, blood

Answer 261

A

Skin, gut, other linings
60% of differentiated cells in the body
Found in the bulge region of hair follicles

Answer 262

A

Neurons, retinal, glial

Answer 263

A

Progenitors can feedback to stem cells to signal about how many progenitors there are, and if more are needed etc (v vascularised so get info)
Change in microenvironment in niche causes the differentiation.

Answer 264

A

In bone marrow from v early in development
Myeloid (Monocytes, macrophages, neutrophils)
Lymphoid (T cells, B cells, NK cells)

Answer 265

A

Subventricular zone lining the lateral ventricles
Subgranular zone of hippocampus
Hypothalamus, lining the 3rd ventricle
Neural S.C

Answer 266

A

stem cells in a cycle between quiencent and active, first decision is whether to enter cell cycle to be active. Adjacent cells in the niche provide factors to determine this.
When divides, give rise to a differentiated daughter cell or self renew as a HSC.
Hormones and signals in the blood will determine this, so niches have endothelial capillary cells.
(e.g. Stem cell factor)

Answer 267

A

Quiescent hematopoietic stem cells (HSCs) are localizated in a zone called the endosteal zone close to osteoblastic lining cells, called the Osteoblastic Niche. When activated (by signals coming from eg endothelial capillary cells/CAR cells), they divide to give rise to active HSCs that move to the central marrow region, in the Vascular Niche.
These can move into the sinusoid blood around body.

Answer 268

A

Sees lots of oestrogen and makes lots more RBCs frp, progenitors of Hemapoietic stem cells as more are used up.

Answer 269

A

Nanos shuts down translation epigenetically, so cant differentiate.

Answer 270

A

By epithelial to mesenchymal transition.

Answer 271

A

Stoke, baldness, blindness, deafness, myocardial infarction, diabetes, cancers, crohns, arthiritis, SC injury, alzheimers, parkinsons, MS, bone marrow transplantation etc.

Answer 272

A

2018, Royal hallamshire hospital for MS

Answer 273

A

Bone marrow relatively easy, gut showing promise

Epithelia much harder

Answer 274

A

Crypt of the gut villi. The crypt is a tube of cells with stem-like cells at the bottom (distal) and as they move up they differentiate into Transient amplifying progenitor cells

Answer 275

A

Crypt base columnar cells see high Wnt (from the neighbouring paneth cells) which induces stem-ness, along with Notch and Noggin.

Answer 276

A

BMP, PTEN

Answer 277

A

Genetically label by EGFP (enhanced GFP)
Use Fluorescent activated cell sorting (FACS) to separate the setm cells.
Culture.
A single stem cell can form a new vill crypt and go onto bud into an organoid

Answer 278

A

Initially synchronous cell cycles symmetric only have S and M phases.
Later, after 14 cell cycles: asyncronous, G2 starts and nuclei migrate to the periphery

Answer 279

A

Syncronous cleavages
Asynchronous after 14 rounds
Migration of nuclei to periphery
Cellularisation as the membrane involutes.

Answer 280

A

Protein String, a phosphatase that activates cyclin dependent kinases

Answer 281

A

Mesoderm is one of the first domains to express string (activates the cdks) but one of the last to divide, so although present the cells don’t divide
Meso inducing genes induce Tribble to inhibiit String.

Answer 282

A

Same strucutres but different growth times, e.g. giraffe’s will grow for longer than humans.
More proliferation is the main cause,
also individual cells may grow larger e.g. cardiac hypertrophy
or Accretion (gradual accumulation of layers of bone)

Answer 283

A

Graft a limb which is fated to be very large in size, onto another animal which is fated to have smaller limbs, becomes the original large size, showing that it is controlled intrinsically. Not all are.

Answer 284

A

If add additional thalamus, all organs maintain same size just have a lrger number, intrinsic control.
Whereas, if add another spleen both will only grow to haf the size, giving correct total tissue- show extrinsic control also.

Answer 285

A

Head initially v big in babies, but stops growing so comparitively shrinks.
Or puberty- both boys and girls initially grow at the same rate (grils bit earlier) but boys keep growing for longer so end up taller.
In Pygmies- this second growth spurt doesnt happen so remain small.

Answer 286

A

14

After is zygotic String

Answer 287

A

Experiment with Ploidy (no. of chromosomes)

If haploid- half number of cells, but overall tissue size is the same, same if triploid- smaller cells as more.

Answer 288

A

Until 13th cycle: maternally supplied string is induced by the maternal genes -> induces the syncronous divisions
After 14th: Zygotic string induced by zyotic genes e.g. pair rule gap etc -> induces the asyncronous divisions

Answer 289

A

By String phosphatase, then cyclins binding

Answer 290

A

To inhibit String, as the mesoderm needs to invaginate , creating the primitive streak, and proliferation will inibit this so until after, it is inhibited.

Answer 291

A

Because more chance of error as dividing, through replication etc e.g. epithelia

Answer 292

A

Cancer cells able to give to give rise to all 3 germ layers. If tranplant these cells into a developing mouse embryo, act normally so are not perminantly altered

Answer 293

A

Loss of function of a tumour supressor gene
e.g. Ras, Raf, Myc

gain of function of a proto-oncogene going to an active oncogene.
e.g. Rb- tumour supressor- retinoblastoma
P53- tumour supressor gene-inhibits cell cycle
Patched- Hh- basil cell carcinoma
APC- Wnt- Adenomatous polyposis coli

Answer 294

A

TOR Pathway- Regulates Cell size (e.g. Tour stops ur cells growing)
Hippo pathway- Regulates Organ size (e.g. a hippos organ is bigger than ours)

Answer 295

A

When it is inactive: The T.F Yki/Yap/Taz is in the nucleus stimulaitng growth and survival
When it is activated these are excluded from nucleus by Phosphorylating them. This inhibits growth.

Answer 296

A

Yki- Drosophila

Yap/Ta- vertebrate

Answer 297

A

When cells are v crowded, making lots of cell-cell contacts they tend to inibit growth.
If however cells feel stretched they turn it off- so proliferate more.

Wnt/BMP may block

Answer 298

A

It is a kinase, that phosphorylates Yki/Yap/Taz if active, keeping the nuclear factors out of the nucleus.

Answer 299

A

Loss of control of growth restriction, tissue keeps growing e.g. wing

Answer 300

A

Determined by the size of the larvae.

Larval rate and duration of growth is influenced by insulin

Answer 301

A

Small cells and fewer.

Answer 302

A

It grows through Ecdysis -moults its shell, secretes another shell to grow into etc progressively. These intermoults are called instars and there are 3 instars in drosophila before pupation.
It grows through Ecdysis -moults its shell, secretes another shell to grow into etc progressively. These intermoults are called instars and there are 3 instars in drosophila before pupation.

Answer 303

A

Stretch receptors in the epidermis or cuticle control the molting.

When the larva has grown too much the receptors will activate and send signals to the brain.
Protothoracicotrophic hormone released from corpus alatum
Acts on the Protothoracic gland to release Ecdyson
The cuticle is released from the epidermis which starts making the new cuticle. Ecdyson causes molting and the old cuticle is broken down by molting enzymes.

Answer 304

A

In imaginal discs

Answer 305

A

intrinic

Extrinsically controlled e.g. CNS interprets the environment.

Answer 306

A

Environmental signals, which the CNS interprets, and secretes PTTH if favourable.
This causes the release of Ecdyson.
If unfavourable Juvenile hormone is released- which prevents metamorphis.
Balance of these two hormones.

Answer 307

A

Balance between Thyroxin and prolactin, causes metamorphis.
Controlled by environment-> hypothalamus causes the secretion of Corticotrophin releasing hormone->pituitary secretes Thyroid stimulating hormone-> thyroid releases thyroxin.
Positive feedback, if enough is reached then metamorphis is irreversible.

Answer 308

A

Different effects on different tissues, growth in limbs but tail regeneration.

Answer 309

A

Insulin like growth factors 1&2, IGF1 and IGF2 important for both embryo and adult growth
Growth Hormone (IGF’s may monitor) from the pituitary, .
GH stimulated by GH releasing hormone, but inhibited by Somatostatin from hypothalamus.
(GH negatively feeds back on itself)

Answer 310

A

GH releasing hormone activates GH, whereas Somatostatin inhibits.
GH then activates Insulin like growth factor 1.
GH feeds back on itself to decrease GHRH levels and upregulate somatostatin levels.

Answer 311

A

Coronal heart disease CHD

Answer 312

A

If cross shetland with shire horse, and the mother grows in is a Shetland the birth weight will be small, whereas if a Shire, will be much higher. Both will grow to end up the same size eventuall however.

Answer 313

A

Dutch famine WWII winter 1944-45, babies mid-late gestation compensatedbirth size but increased risk in obesity, diabetes, CHD later in life.

Answer 314

A

Epithelial tissue-85%

most active tissue continuously being replaced

Answer 315

A

Wnt- loss of APC- Adenomatous polyposis coli
Hh- basal cell carcinoma and Medulloblastoma
Nodal- melinoma formation
Notch-leukemia
EGF (epidermal GF)- breast cancers and lung

Answer 316

A

Frequency of mutations in cell replication etc- lead to cancer.

Answer 317

A

uncontrolled proliferation without differentiation.

Answer 318

A

Morphallaxis: regeneration without growth- dedifferentiation and rearrangement of existing tissues

Epimorphis: New cells formed to replace

Answer 319

A

Morphallaxis: Cells grow continuously, constantly changing their positional value and repatterning after cells are lost at the budding region or basal disc.

Answer 320

A

1- head region
6-basal disc
(Budding region between 4 and 5)

Answer 321

A

1- Highest tendancy to become head as it has the highest resistance to the inhibitor, but has highest levels of inhibitor when a head is present.

6- Lowest tendancy, lowest resitance but low conc of inihibtior

Answer 322

A

Take PV 1 tissue and transplant into another hydra- head inhibitor sufficiently strong that it doesnt become head.
However if remove the head, now two heads form, one from this grafted tissue and the existing PV 1 cell.

Answer 323

A

Low inhibitor levels and high resistance to so another ehad will form near basal tip.

Answer 324

A

PV1- 6hrs
PV5- 30 hours
Longer for the inhibitor gradient to drop to sufficient levels to overcome, and lower resitance to the inibitor than PV1,

Answer 325

A

GSK3 B is inhibition in the head region, which causes an increase in nuclear B catenin causing the head fate.

Answer 326

A

Urodele amphibians

Can regenerate limbs, tail, jaw retina, lens (from iris)

Answer 327

A

Muscle, given multinucleate.

Revert back to mononucleate under Thrombin.

Answer 328

A

Epidermal migration after amputation

2. Cells below epithelium dedifferentiate- pluripotent Blastema.

Answer 329

A

Much larger scale so morphogens need to work at a much greater distance.

Answer 330

A

Thrombin, Msx1

and Phosphorylation needed of Rb to ihibit the inactivation of the cell cycle- so induces proliferation

Answer 331

A

GFP reporter, show muscle will form muscle etc

Answer 332

A

Distal

If distal limb of a newt is amputated and the stump

Answer 333

A

Differential adhesion properties.
Proximal blastema will engulf distal, as distal cells stick together more (stronger adhesion) whereas proximal cells stick to distal.

Answer 334

A

Prod1 is expressed higher levels in proximal, induced by Retinoic acid which can proximalises a blastema via Prod1 upregulation (GPI Linked protein), or Rard2, Meis homeobox gene upregulation.

Answer 335

A

If denervated limb won’t regenerate, however if aneurogenic- never seen nerve cells before, can.

Answer 336

A

nAG- expressed in the nerve sheet after cut normally to damage, and induces regeneration.
In development nAG is expressed in epidermis, and then as nerves develop it stops and is expressed in the nerves. However if aneurogenic, still persists in the epidermis, so can still drive regeneration.

=newt Antior Gradient- binds to Prod1 supporting outgrowth

Answer 337

A

Senses patterning discontinuities in positional vaues, and if there are missing ones it will regenerate those by looking at the patterning before and after to fill in the gaps, irrespective of the overall structure.

Answer 338

A

P1- proximal
P5- Distal
If graft together PV1 to PV5, will regenerate 2,3,4 to fill in the gap.
If graft other way round a PV4 to PV2 will then fill in gaps but keeping a continuum so adding 4,3,2, making it 1,2,3,4,4,3,2,2 etc. as well as the 3,4,5 on the end to finish on the most distal

Answer 339

A

Mice or young children, can regenerate finger tips if beyond nail bed.
Can regrow axons but not whole neurons in PNS.
can’t in CNS- Oligos inhibit with Nogo.

Answer 340

A

Although cardiomyocytes are present they don’t divide.

instead maladaptive hypertrophy and scar tissue is formed.

Answer 341

A

msxB and C expressed, dependent on dedifferentiation of muscle cells, no progenitors or stem cells are used.
Endocardium and epicardium are involved.
Neuregulin may be a signal from the epicardium.

Answer 342

A

Mps1 mutants show scarring, rather than regeneration.

Answer 343

A

Clot forms where there is damage (prevents circulation coming to complete standstill)
Epicardial activation (raldh2 mRNA throughout)
7 days peak in proliferation of cardimyocytes. Epicardium expands to cover the wound- expressing FGF-like Neurogenin which stimulates cardiomyocyte cell division.
Vascularisation of regenerating tissue. New muscle expresses FGF, causes reformation of blood vessels.

Answer 344

A

Neonatal mice can regenerate.

Loss of this ability later, correlates with the loss of Erbb2 a neurogenin co-receptor.

Answer 345

A

Transgenic mice made to have a dominant active form of Erbb2 and were able to induce cardiomyocyte proliferation with limited scar tissue.

Answer 346

A

Induced pluripotent stem cells iPS
Previously taken out from the ICM and cultured=ESC’s, now can take an eunucleated egg and insert nucleus of a fibroblast for example.

Answer 347

A

1962 Gurdon: Found that if add a fibroblast to an enucleated egg cell- it will now have diploid status and form a normal embryo. (dediffferentiation)

2006 Yamanaka: Estimated the 4 factors that induced pluripotency.

Answer 348

A

2006 Yamanaka:
Took a fibroblast of mouse, but instead of inserting into an enucleated egg cell injected these 4 TF’s.
This fibroblast was then inserted into a surrogte mother into a blastocyst with female hormones.
Born a normal embryo.
Dedifferentiate into pluripotent stem cells.

Answer 349

A

vastly renewable
easily acessible
individual specific so no immune reaction
can differentiate into many cell types

Answer 350

A

More complex e.g. overcoming senescence, epigenesis
Safety, no FDA approval
Use of harmful oncogenes when inserting and viral vectors- insertional mutagenesis?
Low efficiency of insertion.

Answer 351

A

Organoids

Culture them, well oxygenated and nutrients

Answer 352

A

Wear and tear: Elephants die because they can no longer eat as their teeth degrade over time. C elegans decline in muscle function
Genetic programme: Suddenly die after laying their eggs

Answer 353

A

Natural selection keeps organism alive until can reproduce and care for young, after there is no natural selection against the animal.

Answer 354

A

High metabolism, short life span- large animals live longer. (smaller have higher)

Answer 355

A

Temperature: Flies 18degrees, 180days, 29degrees 40days- slow metabolism?

Answer 356

A

Metabolism
Reactive oxygen species
DNA damage

Answer 357

A

By product of metabolism of oxygen, which can cause damage to cell structures ‘oxidative stress’ can be in response to stress factors too.
e.g. superoxidide radical
Link to aging not completely clear though

Answer 358

A

High metabolism leads to the formation of ractive oxygen species.

Answer 359

A

Against: C elegans- treat with Paraquat or Juglone (compound created by ROS) caused lifespan increase.

If prevent superoxide radicals by adding another antioxidant, shorter life also

Answer 360

A

Glucose resitriction ends C elegans life by inducing mitochondrial respiration and increasing oxidative stress

Resistance to oxidative stress induced by ‘longevity genes’ increases life.

Answer 361

A

Aging to do with DNA?
e.g
Werner: RecQ DNA helicase mutation, chromosome replication problems
Ehlers Danos- Bgalactosyltransferase mutation

Answer 362

A

When DNA becomes damaged upregulate PARP enzyme, which uses NAD to mark damaged cells, but needed for redox reactions e.g. glycolysis

Answer 363

A

NAD depletion
Senescent cell removal
Superoxide radicals

Answer 364

A

Dietry restriction
environmental stresses
Signals from gonads

Answer 365

A

If restrict calories- life 40% longer- lower metabolism

Answer 366

A

A disproportionate response to small stressors, may activate protective mechanisms in which then conveys an advantage

Answer 367

A

Mutations- see which genes affect lifespan- difficult as could just a be a mutation which causes early death, so longlife mutants more sucessful.

Found IGF pathway, TOR, Sirtuins

Answer 368

A

If c elegans crowded or in adverse conditions can enter this stage, can survive 60days under insulin/IGF1 control (insulin growth factor 1)

Answer 369

A

For life: Dauer stage, survives under insulin IGF1 control.

Answer 370

A

IGF1 to IGF R (DAF2) which inhibits DAF16 (FOXO). FOXO regulates genes that respond increase resistance to stressors

Mutations in Insulin/IGF1 pathway double lifespan (flies are in reproductive diapause) linked to resistance to oxidative stress
Female mice with a mutation in IGF1R (IGF1&2 receptor) live 33% longer

Answer 371

A

FOXO1 and 3A, IGF1 varients have been linked with longevity

Answer 372

A

Dietry restriction decreases insulin signalling in mice, and when mice are made to have a GH receptor mutant (which downregulates IGF) dietry restriction makes no impact as already downregulated; shows defintiely IG pathway.

Answer 373

A

ANITI AGING BY: 
Inhibits IGF (IGF inhibits FOXO also)
Increases anti-oxidant genes
Decreases Metabolic genes
Increases chaperones
Increases antibacterial genes

Answer 374

A

When TOR is active (when lots of nutrients and protein synthesis no stress) PRO-LIFE

Answer 375

A

Stress-> TSC1/2 -I TOR so activates 4E-BP1 (blocks S6 salvage pathway)

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