Model systems Flashcards

1
Q

Why do we need model systems in developmental biology?

A

To understand how humans develop and to understand why sometimes it goes wrong.

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2
Q

What did thalidomide cause and what was it used for?

A

It was used as a morning sickness drug for pregnant women that cause limb development disruption- phocomelia.

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3
Q

What is the difference between development malformations and developmental disruptions?

A

Malformations are genetic mutations and disruptions are environmental factors.

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4
Q

What is cleft palate caused by?

A

Genetic and environmental defects.

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5
Q

What is club foot caused by?

A

Genetic defects.

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6
Q

What is spina bifida?

A

When the neural tubes fail to close.

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7
Q

What are the three approaches in which animal models are used to study development?

A

Anatomical approaches, experimental approaches and genetic approaches.

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8
Q

What are the pros and cons of animal models to consider?

A

The number of embryos, accessibility, cost, embryo manipulation, genetics, gene inventory/genome sequencing, similarity to humans.

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9
Q

In terms of the embryo, what makes sea urchins good model organisms?

A

Embryos are transparent and develop in the external environment - easier to study and manipulate,

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10
Q

In terms of development, what makes sea urchins good model organisms?

A

Development is fast - 5 days after fertilisation, the embryo hatches to become a pluteus larva capable of still feeding.

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11
Q

What are features of drosophila that makes them useful models?

A

The eggs are fertilised when they pass from the oviduct on their way to being laid, females can store male sperm for up to two weeks after mating, eggs are fertilised and immediately laid and the whole process from egg to sexually mature fly only takes 9 days.

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12
Q

How are drosophila stored?

A

They are kept in jars with fluid at the bottom and a stopper at the top. Hundreds can be maintained at one time.

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13
Q

What are the benefits of using nematodes as animal models?

A

They have fast development, they are small, transparent, developing embryos can be removed from the adult female and grown in the lab, hermaphrodite (male and female sex organs).

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14
Q

What are the practical benefits of using nematodes?

A

They are easy and cheap to maintain, the mutant lines can be frozen down to maintain stocks, they are simple (only 959 cells), and by following cell divisions with a microscope the complete cell lineage has been made.

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15
Q

What does it mean that nematodes are hermaphrodites?

A

They are females that make their own sperm for a short time and then switch to making oocytes and they are capable of self fertilisation - however some males do also exist.

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16
Q

What are the benefits of using the xenopus (frog) as an animal model?

A

It has large eggs and embryos and develops outside of the maternal environment. The development of embryos and tadpoles is rapid.

17
Q

What is the disadvantage of using the xenopus as an animal model?

A

The complete life cycle is relatively long, despite the development of embryos and tadpoles being rapid.

18
Q

What are the practical benefits of using the xenopus as an animal model?

A

It is easy and cheap to maintain - it can be kept in small tanks of tap water.

19
Q

What work was John Gurdon involved in with xenopus embryos?

A

He took unfertilised eggs and treated them with UV to destroy the genetic material in them, and then isolated skin cells from adult frogs, removed the nuclei and let the enucleated cells grow into clones.

20
Q

What are the benefits of using mice as animal models?

A

They are mammals - can be used to study human development and disease closely, they have a relatively short life cycle for a mammal, development is internal, they have well characterised genetics, they have embryonic stem cells and then can be easily genetically manipulated.

21
Q

What is the problem practically with using mice as animal models?

A

They are kept in racks of cages in a designated facility with trained staff - high cost.

22
Q

What is the progeny size of mice?

A

6-15 pups per litter.

23
Q

What significance did Martin Evans have with mice animal models?

A

He was the first person to isolate mouse embryonic stem cells and culture them.

24
Q

What are the benefits of using chickens as animal models?

A

You can see most stages of development by cutting a hole in the egg shell. Many aspects of development are similar to humans.

25
Q

What are the practical benefits of using chickens as animal models?

A

They are easy to incubate on a large scale without high cost.

26
Q

What are the downsides of using chickens as animal models?

A

It is tricky to generate transgenic chicks and they have a relatively long life cycle (20 weeks).

27
Q

What are the benefits of using zebrafish as animal models?

A

There is rapid embryogenesis, they have external development and are transparent until just after hatching, they can be genetically manipulated and they have a duplicated genome.

28
Q

What are the practical benefits of using the zebrafish as an animal model?

A

They are easy to produce transgenics/morpholinos and they are cheaper to keep than the mouse (but still expensive).

29
Q

What is an example experiment for the zebrafish being used as an animal model?

A

Large scale mutagenesis screen by Christiane Nusslein-VOlhard to screen for developmental defects.

30
Q

Why is development time after fertilisation important as an animal model?

A

Experimental turnover will be much faster.

31
Q

What determines whether a species is suitable for genetic studies?

A

The duration of the life cycle - if the life cycle is long then the animal is less useful as the turnover is slower so you have to wait for the animal to reach maturity to breed and produce more animals to study.

32
Q

What was an early experiment with the sea urchins in developmental biology?

A

Hans Driesch - 1885 - took a two celled sea urchin embroy and shook it so the cells parted. The cells were separated and found that each cell produced a fully formed normal sea urchin.

33
Q

What was an early developmental biology experiment with drosophila?

A

Thomas Morgan noticed a drosophila had white eyes instead of red and cross bred these to see how the genes were passed on. He linked genes with chromosomes.

34
Q

What was an early experiment involving nematodes?

A

Sydney Brenner lineage traced somatic cells from a zygote and identified genes in cell death, and carried out research that led to the mapping of the worms nervous system.

35
Q

What was an early experiment done with the frog xenopus?

A

John Gurdon treated eggs with UV to destroy genetic material and isolated skin cells from an adult frog and removed the nuclei and put them in the empty eggs and let them develop. Clones were formed.

36
Q

What was an early experiment with mice?

A

Martin Evans and Gail Martin discovered mouse embryonic cells. Knockout mice by injection of genetically modified ES cells into mouse blastocysts.

37
Q

What was an early experiment with chicken?

A

Nicole Le Douarin developed an embryo manipulation technique to produce chimeric embryos. Determined that the precursors in the neural crest were multipotent.

38
Q

What was an early experiment with the Zebrafish?

A

Christiane Nusslein-VOlhard set up a large scale mutagenesis screen of zebrafish embryos and screened for developmental defects. There was phenotype rescue of the alb b4 mutant zebrafish line using genome editing technology.