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Multidimensional PTEN missense variant analysis reveals variant subgroups including potential dominant negatives


ABSTRACT: Determining the pathogenicity of human genetic variants is a critical challenge, and functional assessment is often the only option. Experimentally characterizing millions of possible missense variants in thousands of clinically important genes will likely require generalizable, scalable assays. We previously developed Variant Abundance by Massively Parallel Sequencing (VAMP-seq), which measures the effects of thousands of missense variants of a protein on intracellular abundance in a single experiment. Here, we reapplied VAMP-seq to quantify the abundances of additional PTEN missense variants which were missing from the original experiment.

ORGANISM(S): Escherichia coli Homo sapiens

PROVIDER: GSE159469 | GEO | 2021/09/13

REPOSITORIES: GEO

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