Abstract

To study gene control mechanisms in Xenopus embryos, we analyzed polyamines, cloned SAMDC (S-adenosylmethionine decarboxylase), a key enzyme of polyamine metabolism, and microinjected its mRNA into Xenopus fertilized eggs. The microinjection induced a large increase in SAMDC activity, exhaustion of the substrate SAM (S-adenosylmethionine), and execution of apoptosis at the stage called midblastula transition (MBT). By tracing GFP (green fluorescence protein)-marked apoptotic cells, we reached a conclusion that the apoptosis provides pre-blastula embryos with a fail-safe mechanism of early development. We analyzed caspase mRNAs and found that caspase-9 and -3 mRNAs are maternal mRNA and activation of caspase-9 is one of the key steps for the execution of the apoptosis. We also found that over- expression of caspase-8, and in addition p53, a tumor suppressor protein, also induces apoptosis at MBT, just like the overexpression of SAMDC and caspase-9 does. The apoptosis induced by p53 was suppressed by Xdm-2, a negative regulator of p53, and by a peptide inhibitor and a dominant-negative type mutant of caspase-9, but not by those of caspase-8. By contrast, apoptosis induced by SAMDC was suppressed by peptide inhibitors and dominant-negative mutants of both caspase-9 and caspase-8, but not by Xdm-2. Unlike caspase-9 mRNA, caspase-8 mRNA was not a maternal mRNA, but newly expressed during cleavage stage (pre-MBT stage) only in embryos overexpressed with SAMDC. In SAMDC-induced apoptotic embryos activities to process procaspase-8 and procaspase-9 appeared, whereas in p53-induced apoptotic embryos only activity to process procaspase-9 appeared. Thus, Xenopus embryos have at least two pathways to execute the maternal program of apoptosis: One induced by SAMDC overexpression through activation of caspase-9 and do novo expression of caspase-8 gene, and the other induced by p53 overexpression through activation of caspase-9 but not caspase-8. In Xenopus embryos, it has long been believed that zygotic genes are silent until MBT, but results obtained with caspase-8 may provide a novel example of gene expression before MBT.

Highlights

  • The normal table of development for Xenopus laevis has been established by Nieuwkoop and Faber [1], in which the development is divided into 66 stages from fertilization to metamorphic climax

  • Xenopus embryos have at least two pathways to execute the maternal program of apoptosis: One induced by S-adenosylmethionine decarboxylase (SAMDC) overexpression through activation of caspase-9 and do novo expression of caspase-8 gene, and the other induced by p53 overexpression through activation of caspase-9 but not caspase-8

  • Based on the results obtained, we conclude that Xenopus embryos have at least two pathways to execute the maternal program of apoptosis; one executed by SAMDC-overexpression, and the other executed by p53-overexpression, and while the former is executed through activation of caspase-8 before the activation of caspase-9, the latter is activated not through caspase-8 but directly through caspase-9

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Summary

INTRODUCTION

The normal table of development for Xenopus laevis has been established by Nieuwkoop and Faber [1], in which the development is divided into 66 stages from fertilization to metamorphic climax. The results obtained lead us to conclude that the apoptosis which is executed so early in the development is a kind of “fail-safe” mechanism to check and eliminate damaged cells before embryos enter the morphogenic phase after the MBT stage. In the latter half of this article I describe the results of analyses on mRNAs of caspases 9 and 8 which were found to be involved in the maternal program of apoptosis. Based on the results obtained, we conclude that Xenopus embryos have at least two pathways to execute the maternal program of apoptosis; one executed by SAMDC-overexpression, and the other executed by p53-overexpression, and while the former is executed through activation of caspase-8 before the activation of caspase-9, the latter is activated not through caspase-8 but directly through caspase-9

RESULTS AND DISCUSSION
Overexpression of SAMDC mRNA in Xenopus Embryos and Discovery of Sudden
The Cell Dissociation Is Due to Apoptosis
Involvement of Caspase 9 in SAMDC mRNA-Induced Apoptosis
Maternal Nature of Caspase-9 in Xenopus
2.11. Caspase-8 mRNA Is Newly Synthesized in SAMDC-Overexpressed Cleavage Stage
CONCLUSION
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