17.3 Whole-Genome Sequencing

17.3 Whole-Genome Sequencing

  • Researchers are trying to make the information more accessible to the public.
    • The NCBI has created a tool to simplify the data-mining process by using global positioning systems instead of paper maps.
  • There is a hypothesis.
  • To test the hypothesis, go to this website.
  • There is a comparison of the genes of organisms to the human genes on the web page.
    • Pick the groups of organisms needed for testing the hypothesis from the top portion of the data.
    • The needed information can be found in which columns.
  • Not all of the options are necessary for the task, however it might give more insight to the value of genome/gene comparisons.
  • There is an online catalog of human genes and genetic disorders.
    • The history and research of each trait and disorder can be found on this website.
  • Although there have been advances in the medical sciences in recent years, doctors are still confused by some diseases and are using whole-genome sequencing to find the root of the problem.
    • When there is a genetic basis at the core of a disease, whole-genome sequencing is a brute-force approach to problem solving.
    • Several laboratories offer services to sequence, analyze, and interpret genomes.
  • Whole-exome is a lower-cost alternative to whole genome.
    • The doctor uses exome sequencing to sequence only the genes that produce exons.
    • In 2010, doctors used whole-exome sequencing to save a young boy.
    • The child had a lot of operations.
    • Whole-exome sequencing revealed a defect in a pathway that controls cell death.
    • The doctors used a bone-marrow transplant to cure the boy.
    • He was the first person to receive successful treatment.
    • Results from human genome sequencing can be found within two days for about $1,000.
  • The dideoxy method, which was developed in the 1970s, is the basic sequence technique used in modern day projects.
    • The ddNTPs are missing a hydroxyl group at the site where another nucleotide usually attach to form a chain.
    • Each ddNTP has a different color.
  • When the reaction mixture is separated into single strands, multiple newly replicated DNA strands form a ladder because of the different sizes.
    • Each band on the gel reflects the size of the DNA strand and the ddNTP that ended the reaction.
    • The different colors of the ddNTPs help identify them.
    • The template strand's sequence is produced by reading the gel on the basis of each band's color on the ladder.
  • The dideoxynucleotide is missing the 3' hydroxyl group, but it is similar in structure to a deoxynucleotide.
  • When a dideoxynucleotide is incorporated into a strand of DNA, it stops the synthesis of the strand.
  • The dideoxy chain terminated method is shown in this figure.
    • The DNA fragment can end at different points.
    • We can read the bands based on the size of the fragments.
  • The chain-sequencing method was used for all of the segments.
    • Scientists can analyze the fragments with sequence computer assistance.
  • Scientists can reform the entire DNA sequence by matching overlaps at each fragment's end.
    • Consider that someone has four copies of a landscape photograph that you have never seen before and don't know how it should look.
    • The person takes a photograph with their hands and puts different size pieces in each copy.
    • The person mixes all of the pieces together and asks you to reconstruct the picture.
    • You can see a mountain in one of the smaller pieces.
    • You can see the mountain behind the lake in a larger piece.
    • There is a cabin on the shore of the lake in a third fragment.
    • The picture contains a mountain behind a lake that has a cabin on its shore.
    • This principle is used to reconstruct entire DNA.
  • shotgun sequencing only looked at one end of each fragment for overlaps.
    • It was enough for small genomes.
    • Scientists analyze each fragment's end for overlap.
  • It is easier to reconstruct the sequence when there is more information available.
  • In a single day, these automated low-cost sequencers can generate hundreds of thousands or millions of short fragments.
    • The process of putting all the fragments in order is very time consuming.
  • A sequence alignment is an arrangement of genes.
    • It can be used to identify similar regions between cell types or species.
    • Sequence alignments can be used to build trees.
    • The website uses a software program.
  • The "species" field can be found below the box.
    • Click "BLAST" to compare the inputted sequence against the known sequence of the human genome.
    • The human genome contains over a hundred places where this sequence occurs.
    • A description of each of the matching hits can be found below the graphic with the horizontal bars.
    • You can see the location of the sequence on the page.
    • You can see the sequence immediately around the selected gene by moving the green flag-inspired sliders.
    • You can return to your selected sequence by clicking the "ATG" button.
  • The first genome was completely sequence by Fred Sanger with the help of a bacterial virus.
    • Several other scientists were able to sequence the organelle and viral genomes.
    • Craig Venter, an American geneticist and businessman, was the first to sequence the bacterium.
    • The yeast Saccharomyces cerevisiae, which began in 1989 and was completed in 1996, was 60 times bigger than any other genome sequencing.
    • The genomes of the yeast Saccharomyces cerevisiae and the bacterium Escherichia coli K12 were available in 1997.
    • The genomes of other model organisms, such as the mouse Mus musculus, the fruit fly Drosophila melanogaster, and the nematode Caenorhabditis, are now known.
    • Basic research in model organisms can be applied to similar organisms.
    • The research efforts in these model organisms can be improved by having the entire genomes mapped.
    • Basic experiments in molecular biology can be done with annotating genes.
  • You can click through the steps at this site.