Kenneth James Shaw | Researchain

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Featured researches published by Kenneth James Shaw.

Nature Genetics | 2004

Systematic generation of high-resolution deletion coverage of the Drosophila melanogaster genome

Annette L. Parks; Kevin R. Cook; Marcia Belvin; Nicholas Dompe; Robert Fawcett; Kari Huppert; Lory R Tan; Christopher G. Winter; Kevin Bogart; Jennifer E Deal; Megan E Deal-Herr; Deanna Grant; Marie Marcinko; Wesley Y Miyazaki; Stephanie A. Robertson; Kenneth James Shaw; Mariano Tabios; Valentina Vysotskaia; Lora Zhao; Rachel S. Andrade; Kyle Andrew Edgar; Elizabeth Howie; Keith Killpack; Brett Milash; Amanda Norton; Doua Thao; Kellie Whittaker; Millicent A Winner; Lori Friedman; Jonathan Margolis

In fruit fly research, chromosomal deletions are indispensable tools for mapping mutations, characterizing alleles and identifying interacting loci. Most widely used deletions were generated by irradiation or chemical mutagenesis. These methods are labor-intensive, generate random breakpoints and result in unwanted secondary mutations that can confound phenotypic analyses. Most of the existing deletions are large, have molecularly undefined endpoints and are maintained in genetically complex stocks. Furthermore, the existence of haplolethal or haplosterile loci makes the recovery of deletions of certain regions exceedingly difficult by traditional methods, resulting in gaps in coverage. Here we describe two methods that address these problems by providing for the systematic isolation of targeted deletions in the D. melanogaster genome. The first strategy used a P element–based technique to generate deletions that closely flank haploinsufficient genes and minimize undeleted regions. This deletion set has increased overall genomic coverage by 5–7%. The second strategy used FLP recombinase and the large array of FRT-bearing insertions described in the accompanying paper to generate 519 isogenic deletions with molecularly defined endpoints. This second deletion collection provides 56% genome coverage so far. The latter methodology enables the generation of small custom deletions with predictable endpoints throughout the genome and should make their isolation a simple and routine task.

Bioorganic & Medicinal Chemistry Letters | 2012

Discovery of Xl413, a Potent and Selective Cdc7 Inhibitor.

Elena S. Koltun; Amy Lew Tsuhako; David S. Brown; Naing Aay; Arlyn Arcalas; Vicky Chan; Hongwang Du; Stefan Engst; Kim Ferguson; Maurizio Franzini; Adam Antoni Galan; Charles R. Holst; Ping Huang; Brian Kane; Moon Hwan Kim; Jia Li; David Markby; Manisha Mohan; Kevin Noson; Arthur Plonowski; Steven Richards; Scott Robertson; Kenneth James Shaw; Gordon Mark Stott; Thomas J. Stout; Jenny Young; Peiwen Yu; Cristiana A. Zaharia; Wentao Zhang; Peiwen Zhou

CDC7 is a serine/threonine kinase that has been shown to be required for the initiation and maintenance of DNA replication. Up-regulation of CDC7 is detected in multiple tumor cell lines, with inhibition of CDC7 resulting in cell cycle arrest. In this paper, we disclose the discovery of a potent and selective CDC7 inhibitor, XL413 (14), which was advanced into Phase 1 clinical trials. Starting from advanced lead 3, described in a preceding communication, we optimized the CDC7 potency and selectivity to demonstrate in vitro CDC7 dependent cell cycle arrest and in vivo tumor growth inhibition in a Colo-205 xenograft model.

Archive | 2005