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首页> 外文期刊>Oncogene >ARHI is a Ras-related small G-protein with a novel N-terminal extension that inhibits growth of ovarian and breast cancers
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ARHI is a Ras-related small G-protein with a novel N-terminal extension that inhibits growth of ovarian and breast cancers

机译:ARHI是与Ras相关的小G蛋白,具有新颖的N末端延伸,可抑制卵巢癌和乳腺癌的生长

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Our group recently identified Ras homolog member I (ARHI), a novel maternally imprinted tumor suppressor gene that encodes a 26kDa GTP-binding protein with high homology to Ras and Rap. Unlike other Ras family members, ARHI exhibits several unusual structural and functional properties. ARHI contains a unique 34 amino-acid extension at the N-terminus, and differs from Ras in residues critical for GTPase activity and in its putative effector domain. Like Ras, ARHI can bind to GTP with high affinity but has low intrinsic GTPase activity. In addition, while Ras is an oncogene, ARHI functions as an inhibitor for cell growth. 32Phosphorus labeling showed that ARHI is maintained in a constitutively activated GTP-bound state in resting cells, possibly because of impaired GTPase activity. ARHI is associated at the cell membrane through its prenylation at the C-terminal cysteine residue. Mutation of the conserved CAAX box at the C-terminus led to a loss of its membrane association and a decreased ability to inhibit cell growth. Conversion of Ser51 to Asn decreased GTP binding and reduced ARHI's biological activity. Mutation of Ala46 to Val increased the ability of ARHI to inhibit cell growth, associated with a further decrease of its intrinsic GTPase activity. Moreover, conversion of residues in ARHI that are conserved in the Ras family for GTPase activity partially restored the GTPase activity in ARHI. Most strikingly, deletion of ARHI's unique N-terminal extension nearly abolished its inhibitory effect on cell growth, suggesting its importance in ARHI's inhibitory function. Thus, ARHI is a unique Ras family member that retains basic small GTPase function, but exhibits many unusual features. In contrast to most other Ras family members, ARHI has a long N-terminal extension, modest GTPase activity, and constitutive GTP binding in resting cells. Furthermore, unlike the Ras oncogene, ARHI inhibits cell growth, and loss of its expression in cells may contribute to the development of breast and ovarian cancers.
机译:我们的小组最近鉴定出Ras同源成员I(ARHI),这是一种新颖的母体印迹肿瘤抑制基因,其编码与Ras和Rap具有高度同源性的26kDa GTP结合蛋白。与其他Ras家族成员不同,ARHI具有一些不同寻常的结构和功能特性。 ARHI在N端含有一个独特的34个氨基酸延伸,与Ras的区别在于对GTPase活性至关重要的残基及其推定的效应子域。像Ras一样,ARHI可以高亲和力结合GTP,但固有的GTPase活性低。此外,尽管Ras是致癌基因,但ARHI却充当细胞生长的抑制剂。 32磷标记显示ARHI在静止细胞中维持在组成型激活的GTP结合状态,这可能是因为GTPase活性受损。 ARHI通过其在C端半胱氨酸残基的异戊烯酸酯化而与细胞膜结合。 C末端保守的CAAX盒的突变导致其膜缔合的丧失和抑制细胞生长的能力降低。 Ser51转化为Asn会降低GTP结合并降低ARHI的生物活性。将Ala46突变为Val可增加ARHI抑制细胞生长的能力,并与其内在的GTPase活性进一步降低有关。而且,在Ras家族中对于GTP酶活性保守的ARHI中的残基的转化部分地恢复了ARHI中的GTP酶活性。最令人惊讶的是,删除ARHI独特的N末端延伸几乎消除了其对细胞生长的抑制作用,表明其在ARHI抑制功能中的重要性。因此,ARHI是Ras家族的独特成员,保留了基本的小GTPase功能,但具有许多非同寻常的功能。与大多数其他Ras家族成员相反,ARHI在静止细胞中具有长N端延伸,适度的GTP酶活性和组成型GTP结合。此外,与Ras癌基因不同,ARHI抑制细胞生长,其在细胞中表达的丧失可能有助于乳腺癌和卵巢癌的发展。

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