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・ Mateusz Ostaszewski
・ Mateusz Piskorski
・ Mateusz Piątkowski
・ Mateusz Polaczyk
・ Mateusz Ponitka
・ Mateusz Prus
・ Maternal hypothyroidism
・ Maternal impression
・ Maternal instinct
・ Maternal insult
・ Maternal mortality in fiction
・ Maternal near miss
・ Maternal physiological changes in pregnancy
・ Maternal sensitivity
・ Maternal somatic support after brain death
Maternal to zygotic transition
・ Maternal wall
・ Maternal-fetal medicine
・ Maternalism
・ Maternalist reform
・ Maternidad Sardá
・ Maternidad sin hombres
・ Maternidade
・ Maternien
・ Maternity (disambiguation)
・ Maternity (play)
・ Maternity Allowance
・ Maternity and Parental Leave, etc Regulations 1999
・ Maternity blues
・ Maternity clothing


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Maternal to zygotic transition : ウィキペディア英語版
Maternal to zygotic transition
Maternal to zygotic transition (MZT) is the stage in embryonic development during which development comes under the exclusive control of the zygotic genome. This requires both zygotic genome activation (ZGA) and degradation of maternal products. MZT is often thought to be synonymous with midblastula transition (MBT), but these processes are, in fact, distinct. However, the MBT roughly coincides with ZGA in many metazoans, and thus may share some common regulatory features. For example, both processes are proposed to be regulated by the nucleocytoplasmic ratio. MBT strictly refers to changes in the cell cycle and cell motility that occur just prior to gastrulation.〔〔 In the early cleavage stages of embryogenesis, rapid divisions occur synchronously and there are no "gap" stages in the cell cycle.〔 During these stages, there is also little to no transcription of mRNA from the zygotic genome,〔 but zygotic transcription is not required for MBT to occur.〔 Cellular functions during early cleavage are carried out primarily by maternal products – proteins and mRNAs contributed to the egg during oogenesis.
==Zygotic genome activation==

To begin transcription of zygotic genes, the embryo must first overcome the silencing that has been established. The cause of this silencing could be due to several factors: chromatin modifications leading to repression, lack of adequate transcription machinery, or lack of time in which significant transcription can occur due to the shortened cell cycles. Evidence for the first method was provided by Newport and Kirschner's experiments showing that nucleocytoplasmic ratio plays a role in activating zygotic transcription.〔 They suggest that a defined amount of repressor is packaged into the egg, and that the exponential amplification of DNA at each cell cycle results in titration of the repressor at the appropriate time. Indeed, in ''Xenopus'' embryos in which excess DNA is introduced, transcription begins earlier.〔〔 More recently, evidence has been shown that transcription of a subset of genes in ''Drosophila'' is delayed by one cell cycle in haploid embryos. The second mechanism of repression has also been addressed experimentally. Prioleau et al. show that by introducing TATA binding protein (TBP) into ''Xenopus'' oocytes, the block in transcription can be partially overcome. The hypothesis that shortened cell cycles can cause repression of transcription is supported by the observation that mitosis causes transcription to cease.

抄文引用元・出典: フリー百科事典『 ウィキペディア(Wikipedia)
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