Department of Neuroscience, University of Texas Southwestern Medical Center, Dallas, Texas 75390, USA.
Genes Dev. 2012 Dec 15;26(24):2724-36. doi: 10.1101/gad.208306.112.
Poly(A) tails are 3' modifications of eukaryotic mRNAs that are important in the control of translation and mRNA stability. We identified hundreds of mouse liver mRNAs that exhibit robust circadian rhythms in the length of their poly(A) tails. Approximately 80% of these are primarily the result of nuclear adenylation coupled with rhythmic transcription. However, unique decay kinetics distinguish these mRNAs from other mRNAs that are transcribed rhythmically but do not exhibit poly(A) tail rhythms. The remaining 20% are uncoupled from transcription and exhibit poly(A) tail rhythms even though the steady-state mRNA levels are not rhythmic. These are under the control of rhythmic cytoplasmic polyadenylation, regulated at least in some cases by cytoplasmic polyadenylation element-binding proteins (CPEBs). Importantly, we found that the rhythmicity in poly(A) tail length is closely correlated with rhythmic protein expression, with a several-hour delay between the time of longest tail and the time of highest protein level. Our study demonstrates that the circadian clock regulates the dynamic polyadenylation status of mRNAs, which can result in rhythmic protein expression independent of the steady-state levels of the message.
聚(A)尾是真核 mRNA 3' 的修饰,对翻译和 mRNA 稳定性的控制很重要。我们鉴定了数百种在小鼠肝脏中呈现出强大的聚(A)尾长度昼夜节律的 mRNAs。这些 mRNAs 中约有 80%主要是核腺苷酸化与有节奏的转录相结合的结果。然而,独特的降解动力学将这些 mRNAs 与其他有节奏转录但不表现出聚(A)尾节律的 mRNAs 区分开来。剩下的 20%与转录脱耦,即使稳态 mRNA 水平没有节律性,也表现出聚(A)尾节律。这些是由有节奏的细胞质聚腺苷酸化控制的,至少在某些情况下受到细胞质聚腺苷酸化元件结合蛋白(CPEB)的调节。重要的是,我们发现聚(A)尾长度的节律性与蛋白质表达的节律性密切相关,在最长尾和最高蛋白质水平之间有几个小时的延迟。我们的研究表明,生物钟调节 mRNAs 的动态多聚腺苷酸化状态,这可能导致蛋白质表达的节律性,而不依赖于信息的稳态水平。
