Maximum likelihood estimation of the evolutionary distance of complete genomes of mitochondrial DNA between human and 16 animals

Omar Esmaill Hamadd, I. Akyol, M. S. Ekinci, Emin Özköse
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Abstract

Mitochondrial DNA (mtDNA) is a masterpiece of polynucleotide intelligence provided as a double stranded circular DNA, to be the spirit and manager of molecular activities in eukaryotic cells. The nucleic DNA activity and regulation depend on the signals and the levels of the tRNA and rRNA which mtDNA produced in the cell. The foremost attention-grabbing issue, mtDNA has the ability to adapt with each individual cell by modifying the sequence by slightly the initiation and termination points, likewise, the direction of transcription 5’=>3’ or 3’=>5’.1 Mitochondria generate most of the cellular energy within the form of adenosine triphosphate ATP, regulate cellular oxidation-reduction state and integrate several of the signals for initiating necrobiosis. By means of retrograde signaling, mitochondrial communicate of these events to the nucleus and thus modulate nuclear organic phenomenon and cell cycle. In human, mitochondrial pathology leads to a massive array of pathologies, and many diseases result from various defects of mitochondrial biogenesis and maintenance, metabolism chain complexes or individual mitochondrial proteins.2
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人类与16种动物线粒体DNA全基因组进化距离的最大似然估计
线粒体DNA (mtDNA)是多核苷酸智能的杰作,是真核细胞分子活动的精神和管理者,是双链环状DNA。细胞核DNA的活性和调控取决于mtDNA在细胞中产生的tRNA和rRNA的信号和水平。最引人注目的问题是,mtDNA有能力通过稍微修改起始点和终止点的序列来适应每个细胞,同样,转录方向5 ' =>3 '或3 ' =>5 ' .1线粒体以三磷酸腺苷ATP的形式产生大部分细胞能量,调节细胞氧化还原状态,整合启动坏死的几种信号。线粒体通过逆行信号将这些事件传递给细胞核,从而调节细胞核有机现象和细胞周期。在人类中,线粒体病理导致了大量的病理,许多疾病是由线粒体生物发生和维持、代谢链复合物或单个线粒体蛋白的各种缺陷引起的
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