GT-repeat多态性对人精氨酸琥珀酸合成酶mRNA 3'端形成的调控。

International journal of biochemistry and molecular biology Pub Date : 2013-12-15 eCollection Date: 2013-01-01
Shih-Heng Tseng, Cheng-Yi Cheng, Miao-Zeng Huang, Ming-Yi Chung, Tsung-Sheng Su
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引用次数: 0

摘要

微卫星在人类基因组中大量存在,可能具有上下文依赖的功能。一个高度多态性的GT微卫星位于人精氨酸琥珀酸合成酶(ASS1)基因多A信号的下游。ASS1参与尿素和一氧化氮的生产,是精氨酸生物合成中的限速酶。为了研究GT微卫星是否参与了ASS1 mRNA 3'端形成,我们利用瞬时转染的ASS1小基因构建物,通过S1核酸酶定位来评估poly(A)位点的使用情况。研究发现,人类主要ASS1 mRNA的合成受两个连续的非正则多聚(A)信号UAUAAA和AUUAAA控制,这两个信号相距7个核苷酸,其中U-rich序列和GU微卫星分别作为其下游的GU/U-rich元件。此外,AUUAAA的利用受到gu重复数的影响,可能导致不同重复数个体对ASS1多聚腺苷化的调节存在差异。有趣的是,效率较低的UAUAAA基序被认为是主要的ASS1 poly(A)信号,这可能是由于下游不可缺少的富u元素和延长的gu重复序列限制了AUUAAA基序的利用。UAUAAA基序和GT微卫星仅在灵长类动物中保守,而AUUAAA基序在所有哺乳动物中都存在。亚优的UAUAAA基序和多态的GT微卫星作为ASS1基因的多聚腺苷化信号,可能作为灵长类动物在遗传和环境因素相互作用下调节ASS1水平的策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Modulation of formation of the 3'-end of the human argininosuccinate synthetase mRNA by GT-repeat polymorphism.

Microsatellites are abundant in the human genome and may acquire context-dependent functions. A highly polymorphic GT microsatellite is located downstream of the poly(A) signal of the human argininosuccinate synthetase (ASS1) gene. The ASS1 participates in urea and nitric oxide production and is a rate-limiting enzyme in arginine biosynthesis. To examine possible involvement of the GT microsatellite in ASS1 mRNA 3'-end formation, ASS1 minigene constructs were used in transient transfection for assessment of poly(A) site usage by S1 nuclease mapping. Synthesis of the major human ASS1 mRNA is found to be controlled by two consecutive non-canonical poly(A) signals, UAUAAA and AUUAAA, located 7 nucleotides apart where a U-rich sequence and the GU microsatellite serve as their respective downstream GU/U-rich elements. Moreover, AUUAAA utilization is affected by the GU-repeat number possibly leading to differential regulation of ASS1 polyadenylation in individuals with different repeat numbers. Interestingly, the less efficient UAUAAA motif is noted to be the major ASS1 poly(A) signal possibly as a result of an indispensable downstream U-rich element and restricted utilization of the AUUAAA motif by the presence of extended GU-repeats. The UAUAAA motif and the GT microsatellite are conserved only in primates whereas AUUAAA motif is present in all mammals analyzed. The suboptimal UAUAAA motif and the utilization of the polymorphic GT microsatellite as polyadenylation signal of the ASS1 gene may be used as a strategy in primates to modulate ASS1 level in response to interactions of genetic and environmental factors.

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