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Transcript of WELCOME BACK! Chapter 14 Biotechnology:Chapter 14 Biotechnology: New Terms Today:New Terms Today:...
![Page 1: WELCOME BACK! Chapter 14 Biotechnology:Chapter 14 Biotechnology: New Terms Today:New Terms Today: –Genome –Genetic engineering, transgenic organisms, GM.](https://reader035.fdocuments.net/reader035/viewer/2022062423/56649e705503460f94b6db5f/html5/thumbnails/1.jpg)
WELCOME BACK!WELCOME BACK!
• Chapter 14 Biotechnology: Chapter 14 Biotechnology: • New Terms Today:New Terms Today:
– GenomeGenome– Genetic engineering, transgenic Genetic engineering, transgenic
organisms, GM food,organisms, GM food,– Reproductive and therapeutic cloningReproductive and therapeutic cloning– Stem cells, plouripotent, totipotentStem cells, plouripotent, totipotent– Gene therapyGene therapy
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14.1 Genomics
• field that compares the entire DNA content of different organisms– the genome: the full complement of
genetic information of an organism (i.e., all of its genes and other DNA)
– DNA sequencing: a process that allows scientists to read each nucleotide in a strand of DNA
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Table 14.1
Some Eukaryotic Genomes
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What’s going on in DNA sequencing?
• Identifying a chain of nucleotides so the order of their nitrogenous bases is documented.
• DNA fingerprinting
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14.2 The Human Genome
• The publication of the sequence of the entire human genome occurred on June 26, 2000– the human genome contains more than 3
billion base pairs– it is estimated that there are between 20K
and 30K protein-encoding genes
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14.3 A Scientific Revolution• Genetic engineering: moving genes from one organism to another
– 1st: chop up the source DNA and obtain a copy of the gene you want to transfer
– restriction enzymes bind to specific short sequences on the DNA and make a specific cut• the sequence is symmetrical
• the cut generates DNA fragments that are “sticky”
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14.3 A Scientific Revolution
• DNA from another source that is cut with the same restriction enzyme will have the same sticky ends– these ends can be joined together by the
enzyme ligase
• Restriction enzymes are the basic tools of genetic engineering
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Figure 14.4 How restriction
enzymes produce DNA fragments with sticky ends
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14.3 A Scientific Revolution
• The source of DNA to be transferred
– DNA library: collection of DNA fragments representing all of the DNA from an organism
• How do you get the DNA into the host cell?
– You need a vehicle to carry the source DNA into the host cell
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A gene transfer experiment occurs in 4 stages– Cleaving DNA: cut the source & vector
DNA
q Producing recombinant DNA: place DNA fragments into vectors and then transferring the DNA into the target cells
q Cloning: introduce DNA-bearing vectors into target cells. Then allow target cells to reproduce
q Screening: select the particular infected cells that have received the gene of interest
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Fig 14.5 How a genetic
engineering
experiment works
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14.4 Genetic Engineering and Medicine
• potential to improve medicine, to aid in curing and preventing illness
• Advances have been made in the following areas– the production of proteins used to treat illness– the creation of new vaccines to combat
infection– the replacement of defective genes (i.e., gene
therapy)
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14.4 Genetic Engineering and Medicine
• Many genetic defects occur because our cells fail to make critical proteins– Ie: diabetes
• Insulin (protein) transports glucose from blood across cell membranes.
insulin blood glucose level.• A diabetic can receive a donation of protein
made by another body• genes encoding insulin have been introduced in
bacteria, which can cheaply produce lg quantities of protein
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Table 14.3
Genetically
Engineered Drugs
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Subunit Vaccines• a vaccine produced from specific protein subunits of a
virus and thus having less risk of adverse reactions than whole virus vaccines.
• Used to treat herpes and hepatitis– engineers splice genes from the coat of the virus into a
fragment of cowpox (vaccinia) virus genome– the smallpox virus is the vector – carry the viral coat genes into cultured mammalian cells– where the immune system can develop an immunity to the
virus prior to being exposed to a fully active virus
– piggyback vaccines: Inserting a gene encoding a pathogenic microbe's surface protein into a harmless virus produces
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Figure 14.7 Constructing a subunit, or piggyback, vaccine for the herpes simplex virus
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14.5 Genetic Engineering and Agriculture
• Genetic engineering of crop plants has successfully– made plants more resistant to disease– improved nutritional content (?) and yield– made crops hardier and better able to
resist environmental stresses
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Engineering crops to be resistant to insect pests
• reduces the need to add insecticides to the environment– There is a soil bacteria: Bacillus thuringiensis
(Bt), – It contains a gene that produces a protein that is
toxic when eaten by crop pests – This gene has been inserted into the
chromosomes of tomatoes• because the plants can synthesis Bt protein, they are
toxic to pests, such as the tomato hornworm
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Herbicide resistance has also been genetically engineered
– Glyphosphate: powerful herbicide that kills most actively growing plants and is used to control weeds
– using a gene gun, engineers inserted an isolated gene from a bacterium that is resistant to glyphosphate into crop plants
• the glyphosphate can now be widely applied to fields and orchards where it retards weed growth but not crop growth
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Gold particles coated w/ DNA fired into plant
cells where it is
incorporated into cells
DNA
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Figure 14.9 Genetically engineered herbicide resistance
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How do you feel about this?
• The real promise of genetically modified (GM) plants is to produce crops with desirable traits that directly benefit the consumer– Ie: to combat iron and vitamin A micronutrient
deficiencies among the world’s rice eaters, genetic engineers created GM “golden” rice
• this transgenic rice contains genes from a bean, a fungus, wild rice, and a daffodil to increase its nutritional value
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Figure 14.10 Transgenic “golden” rice
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14.5 Genetic Engineering and Agriculture
• Much controversy and protest
• Bioengineers modify crops in two major ways– makes the crop easier to grow– ? improves the food itself
• Is eating GM food dangerous?– does adding genes introduce novel proteins that maybe
potentially harmful when consumed?– could introduced proteins become allergens?
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Those concerned about the widespread use of GM crops
raise 3 concerns
– Poss of unintentional harm to other organisms• Are weeds important source of food and shelter for
non-pest insects?
– potential for new resistance• pests might become resistant to engineered
proteins. • farmers required to plant some non-GM crop
alongside GM crop to slow the selection pressure for resistance
– gene flow: modified genes may spread to non-GM species due to interbreeding
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14.6 Reproductive Cloning
• Theory of irreversible determination: – animal cells become irreversibly committed after
the first cell divisions of the developing embryo
– nuclear transplants: transplanting a nucleus from an animal cell into the an enucleated egg and seeing if it develops
• only cells extracted from early embryos (no further than the 16-cell stage) will develop into an adult
• we now know that this theory is WRONG
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14.6 Reproductive Cloning
• Keith Campbell, a geneticist, proposed that, in order for a successful nuclear transplant to take place, both the egg and the donated nucleus need to be in the same stage of the cell cycle– Starve the cells so that they pause at the
G1 checkpoint– the nuclear transfers succeed in producing
cloned farm animals
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14.6 Reproductive Cloning
• Reproductive biologist Ian Wilmut worked with Campbell to clone a sheep using the mammary cells of an adult
Figure 14.12 Wilmut’s animal cloning experiment.
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14.6 Reproductive Cloning
Figure 14.12 Wilmut’s animal cloning experiment.
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Figure 14.13 A parade of cloned critters
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14.6 Reproductive Cloning
• Despite the success of “Dolly the Sheep,” only a small fraction of transplanted embryos survive to term– most embryos will die late in pregnancy– many exhibit large offspring syndrome or
lateral developmental problems as they become adults
– almost none survive to a normal lifespan
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14.7 Embryonic Stem Cells
• Embryonic stem cells: form early in development and each has the capacity to develop into a healthy individual
• Totipotent is the ability of cells, such as stem cells, to have the ability to form any body tissue, and even an adult animal
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14.7 Embryonic Stem Cells
• As development proceeds, some of the embryonic stem cells begin to become committed to forming a certain type of tissue only– every major tissue is formed from its own tissue-
specific adult stem cell
• possibility of restoring damaged tissues
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Figure 14.16 Using embryonic stem cells to restored damaged tissue
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14.8 Therapeutic Cloning• also called somatic cell nuclear transfer address the
issue of immune acceptance of a transplanted cell used for therapy
– therapeutic cloning: cloned embryo is destroyed to harvest embryonic stem cells, which will be automatically tolerated by the recipient of the therapy
– Reproductive cloning, the cloned embryo is allowed to develop into adults
– many ethical issues
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Figure 14.18 How human
embryos might be used for therapeutic
cloning
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14.9 Gene Therapy
• Gene transfer therapy involves introducing “healthy” genes into cells that lack them– early work with a cold virus vector, called
an adenovirus, was unsuccessful in humans because of immune attack
– a new vector, adeno-associated virus (AAV) does not elicit a strong immune response and seems promising
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Figure 14.19 Using gene therapy to cure a retinal degenerative disease in dogs
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Next Lecture: Evolution/ Ch. 15• Extra Credit Lottery
– Name & explain 4 scientific evidences of Evolution
– What is a fossil? How does an organism become a fossil? Do most organisms fossilize?
– What does the term Hardy Weinberg balance mean? What are the 5 assumptions necessary for a population to be in Hardy Weinberg balance?