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Caspase-12 processing and fragment translocation into nuclei of tunicamycin-treated cells.

机译:Caspase-12加工和片段转运到衣霉素处理的细胞核中。

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Excess endoplasmic reticulum (ER) stress induces processing of caspase-12, which is located in the ER, and cell death. However, little is known about the relationship between caspase-12 processing and cell death. We prepared antisera against putative caspase-12 cleavage sites (anti-m12D318 and anti-m12D341) and showed that overexpression of caspase-12 induced autoprocessing at D(318) but did not induce cell death. Mutation analysis confirmed that D(318) was a unique autoprocessing site. In contrast, tunicamycin, one of the ER stress stimuli, induced caspase-12 processing at the N-terminal region and the C-terminal region (both at D(318) and D(341)) and cell death. Anti-m12D318 and anti-m12D341 immunoreactivities were located in the ER of the tunicamycin-treated cells, and some immunoreactivities were located around and in the nuclei of the apoptotic cells. Thus, processing at the N-terminal region may be necessary for the translocation of processed caspase-12 into nuclei and cell death induced by ER stress. Some of the caspase-12 processed at the N-terminal and C-terminal regions may directly participate in the apoptotic events in nuclei. doi:10.1038/sj.cdd.4401080
机译:过多的内质网(ER)压力会诱导位于ER中的caspase-12的加工以及细胞死亡。但是,关于caspase-12加工与细胞死亡之间的关系知之甚少。我们准备了针对假定的caspase-12裂解位点(抗m12D318和抗m12D341)的抗血清,并表明caspase-12的过表达诱导了D(318)处的自动加工,但并未诱导细胞死亡。突变分析证实D(318)是一个独特的自动加工位点。相反,衣康霉素是内质网应激的一种刺激,在N端和C端区域(分别在D(318)和D(341)处)诱导caspase-12加工和细胞死亡。抗m12D318和抗m12D341免疫反应性位于衣霉素处理细胞的ER中,一些免疫反应性位于凋亡细胞周围和细胞核中。因此,在N末端区域进行处理对于处理后的caspase-12易位到核中以及ER应激诱导的细胞死亡可能是必需的。在N端和C端区域加工的某些caspase-12可能直接参与细胞核中的凋亡事件。 doi:10.1038 / sj.cdd.4401080

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