Single nucleolus precursor body formation in the pronucleus of mouse zygotes and SCNT embryos.

Mammalian oocytes and zygotes have nucleoli that are transcriptionally inactive and structurally distinct from nucleoli in somatic cells. These nucleoli have been termed nucleolus precursor bodies (NPBs). Recent research has shown that NPBs are important for embryonic development, but they are only...

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Main Authors: Hirohisa Kyogoku, Teruhiko Wakayama, Tomoya S Kitajima, Takashi Miyano
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2018-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC6101414?pdf=render
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spelling doaj-a0f893b12b7b4d508437340e9429f7c52020-11-25T02:13:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032018-01-01138e020266310.1371/journal.pone.0202663Single nucleolus precursor body formation in the pronucleus of mouse zygotes and SCNT embryos.Hirohisa KyogokuTeruhiko WakayamaTomoya S KitajimaTakashi MiyanoMammalian oocytes and zygotes have nucleoli that are transcriptionally inactive and structurally distinct from nucleoli in somatic cells. These nucleoli have been termed nucleolus precursor bodies (NPBs). Recent research has shown that NPBs are important for embryonic development, but they are only required during pronuclear formation. After fertilization, multiple small NPBs are transiently formed in male and female pronuclei and then fuse into a single large NPB in zygotes. In cloned embryos produced by somatic cell nuclear transfer (SCNT), multiple NPBs are formed and maintained in the pseudo-pronucleus, and this is considered an abnormality of the cloned embryos. Despite this difference between SCNT and normal embryos, it is unclear how the size and number of NPBs in pronuclei is determined. Here, we show that in mouse embryos, the volume of NPB materials plays a major role in the NPB scaling through a limiting component mechanism and determines whether a single or multiple NPBs will form in the pronucleus. Extra NPB- and extra MII spindle-injection experiments demonstrated that the total volume of NPBs was maintained regardless of the pronucleus number and the ratio of pronucleus/NPB is important for fusion into a single NPB. Based on these results, we examined whether extra-NPB injection rescued multiple NPB maintenance in SCNT embryos. When extra-NPBs were injected into enucleated-MII oocytes before SCNT, the number of NPBs in pseudo-pronuclei of SCNT embryos was reduced. These results indicate that multiple NPB maintenance in SCNT embryos is caused by insufficient volume of NPB.http://europepmc.org/articles/PMC6101414?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Hirohisa Kyogoku
Teruhiko Wakayama
Tomoya S Kitajima
Takashi Miyano
spellingShingle Hirohisa Kyogoku
Teruhiko Wakayama
Tomoya S Kitajima
Takashi Miyano
Single nucleolus precursor body formation in the pronucleus of mouse zygotes and SCNT embryos.
PLoS ONE
author_facet Hirohisa Kyogoku
Teruhiko Wakayama
Tomoya S Kitajima
Takashi Miyano
author_sort Hirohisa Kyogoku
title Single nucleolus precursor body formation in the pronucleus of mouse zygotes and SCNT embryos.
title_short Single nucleolus precursor body formation in the pronucleus of mouse zygotes and SCNT embryos.
title_full Single nucleolus precursor body formation in the pronucleus of mouse zygotes and SCNT embryos.
title_fullStr Single nucleolus precursor body formation in the pronucleus of mouse zygotes and SCNT embryos.
title_full_unstemmed Single nucleolus precursor body formation in the pronucleus of mouse zygotes and SCNT embryos.
title_sort single nucleolus precursor body formation in the pronucleus of mouse zygotes and scnt embryos.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2018-01-01
description Mammalian oocytes and zygotes have nucleoli that are transcriptionally inactive and structurally distinct from nucleoli in somatic cells. These nucleoli have been termed nucleolus precursor bodies (NPBs). Recent research has shown that NPBs are important for embryonic development, but they are only required during pronuclear formation. After fertilization, multiple small NPBs are transiently formed in male and female pronuclei and then fuse into a single large NPB in zygotes. In cloned embryos produced by somatic cell nuclear transfer (SCNT), multiple NPBs are formed and maintained in the pseudo-pronucleus, and this is considered an abnormality of the cloned embryos. Despite this difference between SCNT and normal embryos, it is unclear how the size and number of NPBs in pronuclei is determined. Here, we show that in mouse embryos, the volume of NPB materials plays a major role in the NPB scaling through a limiting component mechanism and determines whether a single or multiple NPBs will form in the pronucleus. Extra NPB- and extra MII spindle-injection experiments demonstrated that the total volume of NPBs was maintained regardless of the pronucleus number and the ratio of pronucleus/NPB is important for fusion into a single NPB. Based on these results, we examined whether extra-NPB injection rescued multiple NPB maintenance in SCNT embryos. When extra-NPBs were injected into enucleated-MII oocytes before SCNT, the number of NPBs in pseudo-pronuclei of SCNT embryos was reduced. These results indicate that multiple NPB maintenance in SCNT embryos is caused by insufficient volume of NPB.
url http://europepmc.org/articles/PMC6101414?pdf=render
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AT tomoyaskitajima singlenucleolusprecursorbodyformationinthepronucleusofmousezygotesandscntembryos
AT takashimiyano singlenucleolusprecursorbodyformationinthepronucleusofmousezygotesandscntembryos
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