Your search keyword '"Sato, Akitsugu"' showing total 3 results

1. Deletion-mutant mtDNA increases in somatic tissues but decreases in female germ cells with age

Author

Sato, Akitsugu, Nakada, Kazuto, Shitara, Hiroshi, Kasahara, Atsuko, Yonekawa, Hiromichi, and Hayashi, Jun-Ichi

Subjects

Mitochondrial DNA -- Properties, Ovum -- Genetic aspects, Mitochondrial diseases -- Genetic aspects, Biological sciences

Abstract

The proportions of mutant and wild-type mtDNA are crucial in determining the severity of mitochondrial diseases. It has been generally considered that deletion-mutant mtDNA has replication advantages and accumulates with time. Here, we examine the tissue-by-tissue proportions of mutant mtDNA with a 4696-bp deletion ([DELTA]mtDNA) and wild-type mtDNA in mitochondrial disease model mice (mito-mice). Comparison of the proportions of [DELTA]mtDNA in each tissue at various ages showed that the rate of accumulation of [DELTA]mtDNA differed among tissues. The heart, skeletal muscles, kidney, liver, testis, and ovary showed increases in the proportion of [DELTA]mtDNA with age, but the pancreas, spleen, brain, and blood showed only a slight or no increase in proportion. In contrast to the somatic tissues, however, the germ cells of female mito-mice and resultant offspring showed a strong decrease in [DELTA]mtDNA with maternal age. The decrease was so acute that some offspring showed complete disappearance of [DELTA]mtDNA, even though their elder brothers and sisters had high proportions of [DELTA]mtDNA. Female germ cells have a machinery that prevents the inheritence of defective mtDNA to the following generation since germ cells are kept for a long time until they are ovulated.

Published

2007

2. In vivo interaction between mitochondria carrying mtDNAs from different mouse species

Author

Sato, Akitsugu, Nakada, Kazuto, Shitara, Hiroshi, Yonekawa, Hiromichi, and Hayashi, Jun-Ichi

Subjects

Mice as laboratory animals -- Research, Mitochondrial DNA, Biological sciences

Abstract

Mitochondrial disease model mice, mitomice, were created using zygotes of B6mtspr strain mice carrying mitochondrial DNA (mtDNA) from Mus spretus as recipients of exogenous mitochondria carrying wild-type and a deletion mutant mtDNA ([DELTA]mtDNA) of M. musculus domesticus. In these experiments, mtDNAs from different mouse species were used for identification of exo- and endogenous wild-type mtDNAs in the mitomice. Results showed transmission of exogenous [DELTA]mtDNA, but not exogenous wild-type mtDNA, of M. m. domesticus to following generations through the female germ line. Complete elimination of exogenous wild-type mtDNA would be due to stochastic segregation, whereas transmission of exogenous [DELTA]mtDNA would be due to its smaller size leading to a propagational advantage. Tissues in mitomice of the [F.sub.3] generation carrying exogenous [DELTA]mtDNA showed protection from respiration defects until AmtDNA accumulated predominantly. This protection from expression of mitochondrial dysfunction was attained with the help of endogenous wild-type mtDNA of M. spretus, since mitomice did not possess exogenous wild-type mtDNA of M. m. domesticus. These observations provide unambiguous evidence for the presence of interaction between exogenous mitochondria carrying [DELTA]mtDNA and endogenous mitochondria carrying M. spretus wild-type mtDNA.

Published

2004

3. Selective and Continuous Elimination of Mitochondria Microinjected Into Mouse Eggs From Spermatids, but Not From Liver Cells, Occurs Throughout Embryogenesis

Author

Shitara, Hiroshi, Kaneda, Hideki, Sato, Akitsugu, Inoue, Kimiko, Ogura, Atsuo, Yonekawa, Hiromichi, and Hayashi, Jun-Ichi

Subjects

Genetic research -- Analysis, Mitochondria -- Genetic aspects, Biological sciences

Abstract

Exclusion of paternal mitochondria in fertilized mammalian eggs is very stringent and ensures strictly maternal mtDNA inheritance. In this study, to examine whether elimination was specific to sperm mitochondria, we microinjected spermatid or liver mitochondria into mouse embryos. Congenic B6-[mt.sup.spr] strain mice, which are different from C57BL/6J (B6) strain mice (Mus musculus domesticus) only in possessing M. spretus mtDNA, were used as mitochondrial donors. B6-[mt.sup.spr] mice and a quantitative PCR method enabled selective estimation of the amount of M. spretus mtDNA introduced even in the presence of host M. m. domesticus mtDNA and monitoring subsequent changes of its amount during embryogenesis. Results showed that M. spretus mtDNA in spermatid mitochondria was not eliminated by the blastocyst stage, probably due to the introduction of a larger amount of spermatid mtDNA than of sperm mtDNA into embryos on fertilization. However, spermatid-derived M. spretus mtDNA was eliminated by the time of birth, whereas liver-derived M. spretus mtDNA was still present in most newborn mice, even though its amount introduced was significantly less than that of spermatid mtDNA. These observations suggest that mitochondria from spermatids but not from liver have specific factors that ensure their selective elimination and resultant elimination of mtDNA in them, and that the occurrence of elimination is not limited to early stage embryos, but continues throughout embryogenesis.

Published

2000