Tradict enables accurate prediction of eukaryotic transcriptional states from 100 marker genes
نویسندگان
چکیده
Transcript levels are a critical determinant of the proteome and hence cellular function. Because the transcriptome is an outcome of the interactions between genes and their products, it may be accurately represented by a subset of transcript abundances. We develop a method, Tradict (transcriptome predict), capable of learning and using the expression measurements of a small subset of 100 marker genes to predict transcriptome-wide gene abundances and the expression of a comprehensive, but interpretable list of transcriptional programs that represent the major biological processes and pathways of the cell. By analyzing over 23,000 publicly available RNA-Seq data sets, we show that Tradict is robust to noise and accurate. Coupled with targeted RNA sequencing, Tradict may therefore enable simultaneous transcriptome-wide screening and mechanistic investigation at large scales.
منابع مشابه
Tradict enables accurate prediction of eukaryotic transcriptional states 1 " from 100 marker genes 2 " Supplemental
Supplemental Analysis 1 Our training transcriptomes are reflective of biology and are of 7" high technical quality 8" We manually annotated metadata for 1,626 (62.6%, A. thaliana) and 6,682 (32.1%, M. 9" musculus) of the training transcriptomes for both organisms, and found that the major drivers of 10" variation were tissue and developmental stage (Figure 1a-b, main text). The first three prin...
متن کاملTradict enables high fidelity reconstruction of the eukaryotic transcriptome from 100 marker genes
Transcript levels are a critical determinant of the proteome and hence cellular function. Because the transcriptome is an outcome of the interactions between genes and their products, we reasoned it might be accurately represented by a subset of transcript abundances. We develop a method, Tradict (transcriptome predict), capable of learning and using the expression measurements of a small subse...
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عنوان ژورنال:
دوره 8 شماره
صفحات -
تاریخ انتشار 2017