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在非洲爪蟾早期胚胎发育过程中,母源遗传的凋亡程序在中囊胚转换(MBT)左右被激活,作为一种故障安全机制,此前母源-合子过渡前(Pre-MBT)胚胎中的基因表达情况。

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.

作者信息

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

机构信息

Department of Biosciences, School of Science and Engineering, Teikyo University; 1-1 Toyosatodai, Utsunomiya, Tochigi Prefecture 320-8551, Japan.

出版信息

Gene Regul Syst Bio. 2008 May 29;2:213-31. doi: 10.4137/grsb.s579.

Abstract

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.

摘要

S-腺苷甲硫氨酸脱羧酶(SAMDC)是一种将甲基供体S-腺苷甲硫氨酸(SAM)转化为多胺生物合成的氨丙基供体——脱羧SAM(dcSAM)的酶。在我们对非洲爪蟾早期胚胎发育过程中基因表达调控的研究中,我们克隆了非洲爪蟾SAMDC的mRNA,并通过将其mRNA显微注射到非洲爪蟾受精卵中来过表达该酶。在注射了mRNA的胚胎中,SAMDC的水平大幅增加,SAM被耗尽,蛋白质合成受到极大抑制,但细胞多胺含量没有明显变化。过表达SAMDC的胚胎在早期囊胚阶段之前正常分裂和发育,但在囊胚中期或囊胚中期转换(MBT)阶段,所有胚胎都解离成细胞,并因凋亡的执行而被破坏。在卵裂过程中,过表达SAMDC的胚胎转录caspase-8基因,随后caspase-9被激活。当我们在受精卵中过表达p53 mRNA时,在MBT阶段发生了类似的凋亡,但在这种情况下,caspase-8的转录没有发生,然而caspase-9被激活。SAMDC过表达诱导的凋亡被Bcl-2完全抑制,而p53过表达或用其他有毒剂处理诱导的凋亡仅得到部分挽救。当我们仅将SAMDC mRNA注射到8至32细胞胚胎的一个卵裂球中时,注射了mRNA的卵裂球的后代细胞被隔离到囊胚腔中,并在囊胚腔内发生凋亡,尽管这些胚胎继续发育并成为具有不同程度异常的蝌蚪,这反映了被消除细胞的发育命运。因此,胚胎细胞似乎在MBT阶段自我检查,如果出现生理上严重受损的细胞,它们会通过激活和执行母系遗传的凋亡程序从胚胎中被消除。我们假设在MBT阶段执行的凋亡是早期发育的一种“故障安全”机制,以保护胚胎免受卵裂过程中发生的意外损伤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e79d/2733083/3396e276d31b/grsb-2008-213f1.jpg

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