Publications by authors named "James E Annis"

Article Synopsis
  • - Rhabdomyosarcoma (RMS) is the most common soft-tissue cancer in kids, but patients with advanced disease have poor outcomes and limited treatment options, highlighting the need for new therapeutic strategies.
  • - Researchers conducted a high-throughput siRNA screen and discovered GRK5, a G-protein receptor kinase, as a key factor regulating RMS tumor growth and self-renewal, operating independently of its kinase activity.
  • - Inhibiting GRK5 with CCG-215022 in mouse models significantly reduced RMS tumor growth and self-renewal, suggesting that GRK5 could be a promising target for RMS treatment.
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The length of time required for preinvasive adenoma to progress to carcinoma, the immunogenicity of colorectal cancer (CRC), and the identification of high-risk populations make development and testing of a prophylactic vaccine for the prevention of CRC possible. We hypothesized that genes upregulated in adenoma relative to normal tissue, which maintained increased expression in CRC, would encode proteins suitable as putative targets for immunoprevention. We evaluated existing adenoma and CRC microarray datasets and identified 160 genes that were ≥2-fold upregulated in both adenoma and CRC relative to normal colon tissue.

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MYC oncogene family members are broadly implicated in human cancers, yet are considered "undruggable" as they encode transcription factors. MYC also carries out essential functions in proliferative tissues, suggesting that its inhibition could cause severe side effects. We elected to identify synthetic lethal interactions with c-MYC overexpression (MYC-SL) in a collection of ~3,300 druggable genes, using high-throughput siRNA screening.

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Site-specific genome engineering technologies are increasingly important tools in the postgenomic era, where biotechnological objectives often require organisms with precisely modified genomes. Rare-cutting endonucleases, through their capacity to create a targeted DNA strand break, are one of the most promising of these technologies. However, realizing the full potential of nuclease-induced genome engineering requires a detailed understanding of the variables that influence resolution of nuclease-induced DNA breaks.

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