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Exploiting Single-Cell Quantitative Data to Map Genetic Variants Having Probabilistic Effects.

Florent Chuffart, Magali Richard, Daniel Jost, Claire Burny, Helene Duplus-Bottin, Yoshikazu Ohya, and Gael Yvert (2016)

PLoS Genet, 12(8):e1006213.

Despite the recent progress in sequencing technologies, genome-wide association studies (GWAS) remain limited by a statistical-power issue: many polymorphisms contribute little to common trait variation and therefore escape detection. The small contribution sometimes corresponds to incomplete penetrance, which may result from probabilistic effects on molecular regulations. In such cases, genetic mapping may benefit from the wealth of data produced by single-cell technologies. We present here the development of a novel genetic mapping method that allows to scan genomes for single-cell Probabilistic Trait Loci that modifythe statistical properties of cellular-level quantitative traits. Phenotypic values are acquired on thousands of individual cells, and genetic association isobtained from a multivariate analysis of a matrix of Kantorovich distances. No prior assumption is required on the mode of action of the genetic loci involved and, by exploiting all single-cell values, the method can reveal non-deterministic effects. Using both simulations and yeast experimental datasets, we show that it can detect linkages that are missed by classical genetic mapping. A probabilistic effect of a single SNP on cell shape was detected and validated. The method also detected a novel locus associated with elevated gene expression noise of the yeast galactose regulon. Our results illustrate how single-cell technologies can be exploited to improve the genetic dissection of certain common traits. The method is available as an open source Rpackage called ptlmapper.

 
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