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in every cell of a living thing, a DNA is needed to replicate to build a better body of an organism. learn my short notes on DNA replication from the definition, how DNA replicates, and so on from the lecturer taught in my lecture. i really hope that you can correct the shortcomings of my notes.
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The process of DNA replication occurs before cell division or mitosis and also meiosis. This process is in the S (Synthesis) cycle. The first stage before the cell performs mitosis itself is DNA replication first. In this replication process, in stages:
DNA Polymerase performs reverse nucleotide elongation with the helicase enzyme cutting the template DNA which causes there to be empty nucleotide bases as in the picture below. As long as DNA Polymerase performs nucleotide elongation based on the rules of the road (where as it is known that the synthesis path of DNA Polymerase is 5'-3') as long as the helicase enzyme cuts hydrogen bonds on nucleotide base bonds, there are conditions where the helicase enzyme will not cut in the twisted state of the DNA strand or referred to as the positive supercoil state (Supercoil stable) as in the figure below. With the positive twists or supercoils that are useful for folding DNA to fit the cell nucleus (because it is known that the DNA chain is very long. Therefore, this supercoil is needed), then in the replication process it is very necessary to have a gyrase enzyme or known as a topoisomerase enzyme. The mechanism of action of this enzyme is that the first hand of the enzyme known as nuclease acts as a DNA chain breaker, breaking the entangled DNA chain. At this stage, logically by breaking the coiled rope, the coiled form of the rope can be lost. Then, the other arm of the enzyme is known as ligase. So the other hand of the topoisomerase enzyme acts to glue the twists that are broken by the other hand of topoisomerase, the nuclease. So that after the DNA strand becomes a negative supercoil, the helicase enzyme can work again.
It can be seen that there are repeated and discontinuous primers and nucleotide chains. To overcome this, the primers, which are RNA, are replaced with DNA and also add separate chains and nucleotide base pairs to the new DNA that has been made by DNA Polymerase type 2. After the DNA Polymerase type 2 enzyme attaches a nucleotide chain to another new nucleotide DNA chain, there is an enzyme involved, namely the ligase enzyme (adhesive enzyme) to glue the two nucleotide chains together. However, there is one very crucial case in the process of replacing the Primary RNA at the end of the new strand DNA chain. When DNA Polymerase type 1 terminates the RNA Primer at the very end of the Lagging Strand, there is an overhang (void) because keep in mind that the carbon 5 sequence of the DNA Polymerase part of the Lagging Strand is a carbon atom that binds a phosphate group. So DNA Polymerase type 1 cannot connect the new strand (because for a nucleotide to bind to another nucleotide, a hydroxyl group is needed). (see the picture above in the 5'-3' direction at the top of the double strand. At the end there is an overhang or vacant pair from the top DNA strand to the bottom). With this problem, an enzyme appeared that could solve the problem. The enzyme involved is Telomerase, where the work of the enzyme is to lengthen the parent DNA strands that are overhang by Telomerase with the characteristics of the repeating base sequence (the base sequence in eukaryotic cells, especially humans is TTAGGG) called telomeres and the installation of nucleotide bases from telomeres is in the form of RNA chains. Why RNA? As is known, that the DNA of the new strand that has an overhang is a phosphate group, and to form a nucleotide chain there is a phosphodiester bond that requires an OH group (because of the name DNA which means Deoxyribonucleotide). So by adding RNA to the DNA strands is to attach phosphodiester bonds that require OH groups. After all the RNA chains are attached to the parent DNA chain, the RNA chains are replaced by DNA Polymerase type 2 to become all DNA strands. In addition to the role of telomeres extending short strands of DNA, it can also maintain the integrity of the genome such as from the genome does not stick with other genomes.