a novel rna transcript with antiapoptotic function is silenced in fragile x syndrome一种新型rna转录脆性x综合征的凋亡功能是沉默.pdfVIP
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a novel rna transcript with antiapoptotic function is silenced in fragile x syndrome一种新型rna转录脆性x综合征的凋亡功能是沉默
A Novel RNA Transcript with Antiapoptotic Function Is
Silenced in Fragile X Syndrome
Ahmad M. Khalil., Mohammad Ali Faghihi., Farzaneh Modarresi, Shaun P. Brothers, Claes Wahlestedt*
Molecular and Integrative Neurosciences Department (MIND), The Scripps Research Institute, Jupiter, Florida
Several genome-wide transcriptomics efforts have shown that a large percentage of the mammalian genome is transcribed into
RNAs, however, only a small percentage (1–2%) of these RNAs is translated into proteins. Currently there is an intense interest in
characterizing the function of the different classes of noncoding RNAs and their relevance to human disease. Using genomic
approaches we discovered FMR4, a primate-specific noncoding RNA transcript (2.4 kb) that resides upstream and likely shares a
bidirectional promoter with FMR1. FMR4 is a product of RNA polymerase II and has a similar half-life to FMR1. The CGG expansion in
the 59 UTR of FMR1 appears to affect transcription in both directions as we found FMR4, similar to FMR1, to be silenced in fragile X
patients and up-regulated in premutation carriers. Knockdown of FMR4 by several siRNAs did not affect FMR1 expression, nor vice
versa, suggesting that FMR4 is not a direct regulatory transcript for FMR1. However, FMR4 markedly affected human cell
proliferation in vitro; siRNAs knockdown of FMR4 resulted in alterations in the cell cycle and increased apoptosis, while the
overexpression of FMR4 caused an increase in cell proliferation. Collectively, our results demonstrate an antiapoptotic function of
FMR4 and provide evidence that a well-studied genomic locus can show unexpected functional complexity. It cannot be excluded
that altered FMR4 expression might contribute to aspects of the clinical presentation of fragile X syndrome and/or related disorders.
Citation: Khalil AM, Faghihi MA, Modarresi F, Brothers SP, Wahlestedt C (2008) A Novel RNA
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