Project description:High-throughput discovery of functional RNA domains

Project description:A high-throughput assay for quantitative measurement of PCR errors

Project description:Systematic discovery of cap-independent translation sequences in human and viral genomes

Project description:Highly parallel identification of sequence preferences for eukaryotic C2H2 zinc finger domains using a bacterial 1-hybrid assay

Project description:Polycomb-directed repression of gene expression is frequently misregulated in human diseases. A quantitative and target-specific cellular assay was utilized to discover the first potent positive allosteric modulator (PAM) peptidomimetic, UNC4976, of nucleic acid binding by CBX7, a chromodomain methyl-lysine reader of Polycomb repressive complex 1. The PAM activity of UNC4976 resulted in enhanced efficacy across three orthogonal cellular assays by simultaneously antagonizing H3K27me3-specific recruitment of CBX7 to target genes while increasing non-specific binding to DNA and RNA. PAM activity thereby reequilibrates PRC1 away from H3K27me3 target regions. Together, our discovery and characterization of UNC4976 not only revealed the most cellularly potent PRC1-specific chemical probe to date, but also uncovers a potential mechanism of Polycomb regulation with implications for non-histone lysine methylated interaction partners.

Project description:PAM depletion assay of SpaCas12f1

Project description:PAM depletion assay of AcCas12n

Project description:Analysis of next generation sequencing data for an Affibody library

Project description:Methyl-Spec-seq data for HOXB13

Project description:synthetic construct Raw sequence reads