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AUUUA基序破坏与增强子插入之间的协同作用导致白细胞介素-3依赖的造血细胞发生自分泌转化。

Synergy between AUUUA motif disruption and enhancer insertion results in autocrine transformation of interleukin-3-dependent hematopoietic cells.

作者信息

Mayo M W, Wang X Y, Algate P A, Arana G F, Hoyle P E, Steelman L S, McCubrey J A

机构信息

Department of Microbiology and Immunology, East Carolina University School of Medicine, Greenville, NC 27858, USA.

出版信息

Blood. 1995 Oct 15;86(8):3139-50.

PMID:7579409
Abstract

Previously, we characterized the transposition of an intracisternal type A particle (IAP) to the 3' untranslated region (UTR) of the interleukin-3 (IL-3) gene, which displaced two of the six AUUUA motifs associated with mRNA stability in an IL-3-secreting clone. To determine whether this rearrangement was involved in the autocrine transformation of the parental IL-3-dependent FL5.12 cell line, the germline (gIL-3) and rearranged IL-3 (rIL-3) genes were isolated and subcloned into a gene transfer vector. Moreover, the IAP-long terminal repeat (LTR) and the IL-3 3' UTR AUUUA motifs were deleted (rIL-3 + delta LTR and gIL-3 + delta AUUUA) in some IL-3 constructs to ascertain their role in the transformation process. The IAP-LTR was also added to these constructs (rIL-3 + delta LTR + IAP-LTR, gIL-3 + delta AUUUA + IAP-LTR, and gIL-3 + IAP-LTR), to determine whether it was necessary for autocrine transformation. The ability of the modified IL-3 genes to abrogate the IL-3 dependency of FL5.12 cells had the following rank order: rIL-3 was greater than rIL-3 + delta LTR + IAP-LTR, which was greater than gIL-3 + delta AUUUA + IAP-LTR, which was greater than gIL-3 + delta AUUUA, which was equal to rIL-3 + delta LTR, which was greater than gIL-3. The half-life of IL-3 mRNA was 20-fold longer in cells containing a mutated as opposed to a wild-type AUUUA region. All of the factor-independent cells that expressed the IL-3 transgenes secreted IL-3 and were tumorigenic after injection into BALB/c nude mice. These results indicated that two events could synergize in the autocrine transformation of hematopoietic cells: (1) addition of a transcriptional enhancer present in a retroviral LTR, and (2) disruption of an mRNA stability region.

摘要

此前,我们对一个A型脑池内颗粒(IAP)转座至白细胞介素-3(IL-3)基因的3'非翻译区(UTR)进行了特征分析,在一个分泌IL-3的克隆中,该转座取代了六个与mRNA稳定性相关的AUUUA基序中的两个。为了确定这种重排是否参与了亲本IL-3依赖的FL5.12细胞系的自分泌转化,分离了种系(gIL-3)和重排的IL-3(rIL-3)基因,并亚克隆到一个基因转移载体中。此外,在一些IL-3构建体中删除了IAP长末端重复序列(LTR)和IL-3 3'UTR AUUUA基序(rIL-3 + ΔLTR和gIL-3 + ΔAUUUA),以确定它们在转化过程中的作用。还将IAP-LTR添加到这些构建体中(rIL-3 + ΔLTR + IAP-LTR、gIL-3 + ΔAUUUA + IAP-LTR和gIL-3 + IAP-LTR),以确定其对自分泌转化是否必要。修饰后的IL-3基因消除FL5.12细胞对IL-3依赖性的能力具有以下排序:rIL-3大于rIL-3 + ΔLTR + IAP-LTR,rIL-3 + ΔLTR + IAP-LTR大于gIL-3 + ΔAUUUA + IAP-LTR,gIL-3 + ΔAUUUA + IAP-LTR大于gIL-3 + ΔAUUUA,gIL-3 + ΔAUUUA等于rIL-3 + ΔLTR,rIL-3 + ΔLTR大于gIL-3。与野生型AUUUA区域相比,在含有突变型AUUUA区域的细胞中,IL-3 mRNA的半衰期长20倍。所有表达IL-3转基因的不依赖因子的细胞均分泌IL-3,并且在注射到BALB/c裸鼠后具有致瘤性。这些结果表明,两个事件可在造血细胞的自分泌转化中协同作用:(1)添加逆转录病毒LTR中存在的转录增强子,以及(2)破坏mRNA稳定区域。

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