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123.txt
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123.txt
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Mitochondrial DNA became an area of research in phylogenetics in the late 1970s. Unlike genomic DNA, it offered advantages in that it did not undergo recombination. The process of recombination, if frequent enough, corrupts the ability to create parsimonious trees because of stretches of amino acid subsititions (SNPs).[clarification needed] When looking between distantly related species, recombination is less of a problem since recombination between branches from common ancestors is prevented after true speciation occurs. When examining closely related species, or branching within species, recombination creates a large number of 'irrelevant SNPs' for cladistic analysis. MtDNA, through the process of organelle division, became clonal over time; very little, or often none, of that paternal mtDNA is passed. While recombination may occur in mtDNA, there is little risk that it will be passed to the next generation. As a result, mtDNA become clonal copies of each other, except when a new mutation arises. As a result, mtDNA does not have pitfalls of autosomal loci when studied in interbreeding groups. Another advantage of mtDNA is that the hyper-variable regions evolve very quickly; this shows that certain regions of mitochondrial DNA approach neutrality. This allowed the use of mitochondrial DNA to determine that the relative age of the human population was small, having gone through a recent constriction at about 150,000 years ago (see #Causes of errors).
Mitochondrial DNA has also been used to verify the proximity of chimpanzees to humans relative to gorillas, and to verify the relationship of these three species relative to the orangutan.
A population bottleneck, as illustrated was detected by intrahuman mtDNA phylogenetic studies; the length of the bottleneck itself is indeterminate per mtDNA.
More recently,[when?] the mtDNA genome has been used to estimate branching patterns in peoples around the world, such as when the new world was settled and how. The problem with these studies have been that they rely heavily on mutations in the coding region. Researchers have increasingly discovered that as humans moved from Africa's south-eastern regions, that more mutations accumulated in the coding region than expected, and in passage to the new world some groups are believed[citation needed] to have passed from the Asian tropics to Siberia to an ancient land region called Beringia and quickly migrated to South America. Many of the mtDNA have far more mutations and at rarely mutated coding sites relative to expectations of neutral mutations.
Mitochondrial DNA offers another advantage over autosomal DNA. There are generally 2 to 4 copies of each chromosome in each cell (1 to 2 from each parent chromosome). For mtDNA there can be dozens to hundreds in each cell. This increases the amount of each mtDNA loci by at least a magnitude. For ancient DNA, in which the DNA is highly degraded, the number of copies of DNA is helpful in extending and bridging short fragments together, and decreases the amount of bone extracted from highly valuable fossil/ancient remains. Unlike Y chromosome, both male and female remains carry mtDNA in roughly equal quantities.