细胞死亡诱导DNA片段化因子(DFF45)样效应蛋白家族新成员CIDE-3的分子克隆与特性分析
Molecular cloning and characterization of CIDE-3, a novel member of the cell-death-inducing DNA-fragmentation-factor (DFF45)-like effector family.
作者信息
Liang Liang, Zhao Mujun, Xu Zhenhua, Yokoyama Kazunari K, Li Tsaiping
机构信息
State Key Laboratory of Molecular Biology, Institute of Biochemistry and Cell Biology, Shanghai Institutes for Biological Sciences, Chinese Academy of Sciences, 320 Yue Yang Road, Shanghai 200031, China.
出版信息
Biochem J. 2003 Feb 15;370(Pt 1):195-203. doi: 10.1042/BJ20020656.
DNA fragmentation is one of the critical steps in apoptosis, which is induced by DNA fragmentation factor (DFF). DFF is composed of two subunits, a 40 kDa caspase-activated nuclease (DFF40) and a 45 kDa inhibitor (DFF45). Recently a novel family of cell-death-inducing DFF45-like effectors (CIDEs) has been identified. Among CIDEs, two from human (CIDE-A and CIDE-B) and three from mouse (CIDE-A, CIDE-B and FSP27) have been reported. In this study human CIDE-3, a novel member of CIDEs, was identified upon sequence analysis of a previously unidentified cDNA that encoded a protein of 238 amino acids. It was shown to be a human homologue of mouse FSP27, and shared homology with the CIDE-N and CIDE-C domains of CIDEs. Apoptosis-inducing activity was clearly shown by DNA-fragmentation assay of the nuclear DNA of CIDE-3 transfected 293T cells. The expression pattern of CIDE-3 was different from that of CIDE-B. As shown by Northern-blot analysis, CIDE-3 was expressed mainly in human small intestine, heart, colon and stomach, while CIDE-B showed strong expression in liver and small intestine and at a lower level in colon, kidney and spleen. Green-fluorescent-protein-tagged CIDE-3 was revealed in some cytosolic corpuscles. Alternative splicing of the CIDE-3 gene was also identified by reverse transcription PCR, revealing that two transcripts, CIDE-3 and CIDE-3alpha, were present in HepG2 and A375 cells. CIDE-3 comprised a full-length open reading frame with 238 amino acids; in CIDE-3alpha exon 3 was deleted and it encoded a protein of 164 amino acids. Interestingly the CIDE-3alpha isoform still kept the apoptosis-inducing activity and showed the same pattern of subcellular localization as CIDE-3. Consistent with its chromosome localization at 3p25, a region associated with high frequency loss of heterozygosity in many tumours, CIDE-3 may play an important role in prevention of tumorigenesis.
DNA片段化是细胞凋亡的关键步骤之一,它由DNA片段化因子(DFF)诱导。DFF由两个亚基组成,一个是40 kDa的半胱天冬酶激活核酸酶(DFF40),另一个是45 kDa的抑制剂(DFF45)。最近,一个新的诱导细胞死亡的DFF45样效应蛋白(CIDE)家族被鉴定出来。在CIDE家族中,已报道了两种来自人类的蛋白(CIDE-A和CIDE-B)以及三种来自小鼠的蛋白(CIDE-A、CIDE-B和FSP27)。在本研究中,通过对一个先前未鉴定的编码238个氨基酸蛋白质的cDNA进行序列分析,鉴定出了CIDE家族的一个新成员——人类CIDE-3。它被证明是小鼠FSP27的人类同源物,并与CIDE家族的CIDE-N和CIDE-C结构域具有同源性。通过对转染了CIDE-3的293T细胞的核DNA进行DNA片段化分析,清楚地显示了其诱导细胞凋亡的活性。CIDE-3的表达模式与CIDE-B不同。如Northern印迹分析所示,CIDE-3主要在人类小肠、心脏、结肠和胃中表达,而CIDE-B在肝脏和小肠中表达强烈,在结肠、肾脏和脾脏中表达水平较低。绿色荧光蛋白标记的CIDE-3在一些胞质小体中被发现。通过逆转录PCR也鉴定出了CIDE-3基因的可变剪接,结果显示在HepG2和A375细胞中存在两种转录本,即CIDE-3和CIDE-3α。CIDE-3包含一个全长238个氨基酸的开放阅读框;在CIDE-3α中,外显子3缺失,它编码一个164个氨基酸的蛋白质。有趣的是,CIDE-3α异构体仍然保持诱导细胞凋亡的活性,并且显示出与CIDE-3相同的亚细胞定位模式。与其位于3p25的染色体定位一致,该区域在许多肿瘤中与高频杂合性缺失相关,CIDE-3可能在预防肿瘤发生中发挥重要作用。
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