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The Protease Degrading Sperm Histones Post-Fertilization in Sea Urchin Eggs Is a Nuclear Cathepsin L That Is Further Required for Embryo Development

机译:蛋白酶降解组蛋白的精子受精后的海胆卵是一种核蛋白酶L将其进一步要求胚胎发育

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摘要

Proteolysis of sperm histones in the sea urchin male pronucleus is the consequence of the activation at fertilization of a maternal cysteine protease. We previously showed that this protein is required for male chromatin remodelling and for cell-cycle progression in the newly formed embryos. This enzyme is present in the nucleus of unfertilized eggs and is rapidly recruited to the male pronucleus after insemination. Interestingly, this cysteine-protease remains co-localized with chromatin during S phase of the first cell cycle, migrates to the mitotic spindle in M-phase and is re-located to the nuclei of daughter cells after cytokinesis. Here we identified the protease encoding cDNA and found a high sequence identity to cathepsin proteases of various organisms. A phylogenetical analysis clearly demonstrates that this sperm histone protease (SpHp) belongs to the cathepsin L sub-type. After an initial phase of ubiquitous expression throughout cleavage stages, SpHp gene transcripts become restricted to endomesodermic territories during the blastula stage. The transcripts are localized in the invaginating endoderm during gastrulation and a gut specific pattern continues through the prism and early pluteus stages. In addition, a concomitant expression of SpHp transcripts is detected in cells of the skeletogenic lineage and in accordance a pharmacological disruption of SpHp activity prevents growth of skeletal rods. These results further document the role of this nuclear cathepsin L during development.
机译:海胆雄性原核中精子组蛋白的蛋白水解是母体半胱氨酸蛋白酶受精时激活的结果。我们以前表明,这种蛋白质是雄性染色质重塑和新形成的胚胎中细胞周期进程所必需的。这种酶存在于未受精卵的核中,在受精后迅速被募集到雄性原核中。有趣的是,该半胱氨酸蛋白酶在第一个细胞周期的S期与染色质共定位,在M期迁移到有丝分裂纺锤体,并在胞质分裂后重新定位到子代细胞的核。在这里,我们鉴定了编码cDNA的蛋白酶,并发现了与各种生物组织蛋白酶的高度序列同一性。系统发育分析清楚地表明,该精子组蛋白蛋白酶(SpHp)属于组织蛋白酶L亚型。在整个卵裂期普遍表达的初始阶段之后,在囊胚阶段,SpHp基因转录物被限制在皮内膜区域。转录本在胃小肠形成过程中定位在侵入性内胚层中,并且肠道的特定模式持续贯穿棱镜和早期的臀肌阶段。另外,在骨骼生成系的细胞中检测到SpHp转录物的伴随表达,并且据此,SpHp活性的药理学破坏阻止了骨骼杆的生长。这些结果进一步证明了该组织蛋白酶L在发育过程中的作用。

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