Gene Expression in Pre-MBT Embryos and Activation of Maternally-Inherited Program of Apoptosis to be Executed at around MBT as a Fail-Safe Mechanism in Xenopus Early Embryogenesis

S-adenosylmethionine decarboxylase (SAMDC) is an enzyme which converts S-adenosylmethione (SAM), a methyl donor, to decarboxylated SAM (dcSAM), an aminopropyl donor for polyamine biosynthesis. In our studies on gene expression control in Xenopus early embryogenesis, we cloned the mRNA for Xenopus SA...

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Autores principales: Shiokawa, Koichiro, Aso, Mai, Kondo, Takeshi, Uchiyama, Hiroaki, Kuroyanagi, Shinsaku, Takai, Jun-Ichi, Takahashi, Senji, Kajitani, Masayuki, Kaito, Chikara, Sekimizu, Kazuhisa, Takayama, Eiji, Igarashi, Kazuei, Hara, Hiroshi
Formato: Texto
Lenguaje:English
Publicado: Libertas Academica 2008
Materias:
Review
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2733083/
https://www.ncbi.nlm.nih.gov/pubmed/19787085
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author Shiokawa, Koichiro
Aso, Mai
Kondo, Takeshi
Uchiyama, Hiroaki
Kuroyanagi, Shinsaku
Takai, Jun-Ichi
Takahashi, Senji
Kajitani, Masayuki
Kaito, Chikara
Sekimizu, Kazuhisa
Takayama, Eiji
Igarashi, Kazuei
Hara, Hiroshi
author_facet Shiokawa, Koichiro
Aso, Mai
Kondo, Takeshi
Uchiyama, Hiroaki
Kuroyanagi, Shinsaku
Takai, Jun-Ichi
Takahashi, Senji
Kajitani, Masayuki
Kaito, Chikara
Sekimizu, Kazuhisa
Takayama, Eiji
Igarashi, Kazuei
Hara, Hiroshi
author_sort Shiokawa, Koichiro
collection PubMed
description S-adenosylmethionine decarboxylase (SAMDC) is an enzyme which converts S-adenosylmethione (SAM), a methyl donor, to decarboxylated SAM (dcSAM), an aminopropyl donor for polyamine biosynthesis. In our studies on gene expression control in Xenopus early embryogenesis, we cloned the mRNA for Xenopus SAMDC, and overexpressed the enzyme by microinjecting its mRNA into Xenopus fertilized eggs. In the mRNA-injected embryos, the level of SAMDC was enormously increased, the SAM was exhausted, and protein synthesis was greatly inhibited, but cellular polyamine content did not change appreciably. SAMDC-overexpressed embryos cleaved and developed normally up to the early blastula stage, but at the midblastula stage, or the stage of midblastula transition (MBT), all the embryos were dissociated into cells, and destroyed due to execution of apoptosis. During cleavage SAMDC-overexpressed embryos transcribed caspase-8 gene, and this was followed by activation of caspase-9. When we overexpressed p53 mRNA in fertilized eggs, similar apoptosis took place at MBT, but in this case, transcription of caspase-8 did not occur, however activation of caspase-9 took place. Apoptosis induced by SAMDC-overexpression was completely suppressed by Bcl-2, whereas apoptosis induced by p53 overexpression or treatments with other toxic agents was only partially rescued. When we injected SAMDC mRNA into only one blastomere of 8- to 32-celled embryos, descendant cells of the mRNA-injected blastomere were segregated into the blastocoel and underwent apoptosis within the blastocoel, although such embryos continued to develop and became tadpoles with various extents of anomaly, reflecting the developmental fate of the eliminated cells. Thus, embryonic cells appear to check themselves at MBT and if physiologically severely-damaged cells occur, they are eliminated from the embryo by activation and execution of the maternally-inherited program of apoptosis. We assume that the apoptosis executed at MBT is a “fail-safe” mechanism of early development to save the embryo from accidental damages that take place during cleavage.
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spelling pubmed-27330832009-09-28 Gene Expression in Pre-MBT Embryos and Activation of Maternally-Inherited Program of Apoptosis to be Executed at around MBT as a Fail-Safe Mechanism in Xenopus Early Embryogenesis Shiokawa, Koichiro Aso, Mai Kondo, Takeshi Uchiyama, Hiroaki Kuroyanagi, Shinsaku Takai, Jun-Ichi Takahashi, Senji Kajitani, Masayuki Kaito, Chikara Sekimizu, Kazuhisa Takayama, Eiji Igarashi, Kazuei Hara, Hiroshi Gene Regul Syst Bio Review S-adenosylmethionine decarboxylase (SAMDC) is an enzyme which converts S-adenosylmethione (SAM), a methyl donor, to decarboxylated SAM (dcSAM), an aminopropyl donor for polyamine biosynthesis. In our studies on gene expression control in Xenopus early embryogenesis, we cloned the mRNA for Xenopus SAMDC, and overexpressed the enzyme by microinjecting its mRNA into Xenopus fertilized eggs. In the mRNA-injected embryos, the level of SAMDC was enormously increased, the SAM was exhausted, and protein synthesis was greatly inhibited, but cellular polyamine content did not change appreciably. SAMDC-overexpressed embryos cleaved and developed normally up to the early blastula stage, but at the midblastula stage, or the stage of midblastula transition (MBT), all the embryos were dissociated into cells, and destroyed due to execution of apoptosis. During cleavage SAMDC-overexpressed embryos transcribed caspase-8 gene, and this was followed by activation of caspase-9. When we overexpressed p53 mRNA in fertilized eggs, similar apoptosis took place at MBT, but in this case, transcription of caspase-8 did not occur, however activation of caspase-9 took place. Apoptosis induced by SAMDC-overexpression was completely suppressed by Bcl-2, whereas apoptosis induced by p53 overexpression or treatments with other toxic agents was only partially rescued. When we injected SAMDC mRNA into only one blastomere of 8- to 32-celled embryos, descendant cells of the mRNA-injected blastomere were segregated into the blastocoel and underwent apoptosis within the blastocoel, although such embryos continued to develop and became tadpoles with various extents of anomaly, reflecting the developmental fate of the eliminated cells. Thus, embryonic cells appear to check themselves at MBT and if physiologically severely-damaged cells occur, they are eliminated from the embryo by activation and execution of the maternally-inherited program of apoptosis. We assume that the apoptosis executed at MBT is a “fail-safe” mechanism of early development to save the embryo from accidental damages that take place during cleavage. Libertas Academica 2008-05-29 /pmc/articles/PMC2733083/ /pubmed/19787085 Text en © 2008 by the authors http://creativecommons.org/licenses/by/3.0 This article is an open-access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/3.0/).
spellingShingle Review
Shiokawa, Koichiro
Aso, Mai
Kondo, Takeshi
Uchiyama, Hiroaki
Kuroyanagi, Shinsaku
Takai, Jun-Ichi
Takahashi, Senji
Kajitani, Masayuki
Kaito, Chikara
Sekimizu, Kazuhisa
Takayama, Eiji
Igarashi, Kazuei
Hara, Hiroshi
Gene Expression in Pre-MBT Embryos and Activation of Maternally-Inherited Program of Apoptosis to be Executed at around MBT as a Fail-Safe Mechanism in Xenopus Early Embryogenesis
title Gene Expression in Pre-MBT Embryos and Activation of Maternally-Inherited Program of Apoptosis to be Executed at around MBT as a Fail-Safe Mechanism in Xenopus Early Embryogenesis
title_full Gene Expression in Pre-MBT Embryos and Activation of Maternally-Inherited Program of Apoptosis to be Executed at around MBT as a Fail-Safe Mechanism in Xenopus Early Embryogenesis
title_fullStr Gene Expression in Pre-MBT Embryos and Activation of Maternally-Inherited Program of Apoptosis to be Executed at around MBT as a Fail-Safe Mechanism in Xenopus Early Embryogenesis
title_full_unstemmed Gene Expression in Pre-MBT Embryos and Activation of Maternally-Inherited Program of Apoptosis to be Executed at around MBT as a Fail-Safe Mechanism in Xenopus Early Embryogenesis
title_short Gene Expression in Pre-MBT Embryos and Activation of Maternally-Inherited Program of Apoptosis to be Executed at around MBT as a Fail-Safe Mechanism in Xenopus Early Embryogenesis
title_sort gene expression in pre-mbt embryos and activation of maternally-inherited program of apoptosis to be executed at around mbt as a fail-safe mechanism in xenopus early embryogenesis
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2733083/
https://www.ncbi.nlm.nih.gov/pubmed/19787085
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