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Featured researches published by William H. Andrews.


Proceedings of the National Academy of Sciences of the United States of America | 2012

Antiproliferative small-molecule inhibitors of transcription factor LSF reveal oncogene addiction to LSF in hepatocellular carcinoma

Trevor Grant; Joshua A. Bishop; Lisa M. Christadore; Girish Barot; Hang Gyeong Chin; Sarah Woodson; John Kavouris; Ayesha Siddiq; Rachel Gredler; Xue-Ning Shen; Jennifer Sherman; Tracy L. Meehan; Kevin Fitzgerald; Sriharsa Pradhan; Laura Briggs; William H. Andrews; Devanand Sarkar; Scott E. Schaus; Ulla Hansen

Hepatocellular carcinoma (HCC) is the fifth most common cancer worldwide. Despite the prevalence of HCC, there is no effective, systemic treatment. The transcription factor LSF is a promising protein target for chemotherapy; it is highly expressed in HCC patient samples and cell lines, and promotes oncogenesis in rodent xenograft models of HCC. Here, we identify small molecules that effectively inhibit LSF cellular activity. The lead compound, factor quinolinone inhibitor 1 (FQI1), inhibits LSF DNA-binding activity both in vitro, as determined by electrophoretic mobility shift assays, and in cells, as determined by ChIP. Consistent with such inhibition, FQI1 eliminates transcriptional stimulation of LSF-dependent reporter constructs. FQI1 also exhibits antiproliferative activity in multiple cell lines. In LSF-overexpressing cells, including HCC cells, cell death is rapidly induced; however, primary or immortalized hepatocytes are unaffected by treatment with FQI1. The highly concordant structure–activity relationship of a panel of 23 quinolinones strongly suggests that the growth inhibitory activity is due to a single biological target or family. Coupled with the striking agreement between the concentrations required for antiproliferative activity (GI50s) and for inhibition of LSF transactivation (IC50s), we conclude that LSF is the specific biological target of FQIs. Based on these in vitro results, we tested the efficacy of FQI1 in inhibiting HCC tumor growth in a mouse xenograft model. As a single agent, tumor growth was dramatically inhibited with no observable general tissue cytotoxicity. These findings support the further development of LSF inhibitors for cancer chemotherapy.


Science | 1997

Telomerase Catalytic Subunit Homologs from Fission Yeast and Human

Toru M. Nakamura; Gregg B. Morin; Karen B. Chapman; Scott L. Weinrich; William H. Andrews; Joachim Lingner; Calvin B. Harley; Thomas R. Cech


Nature Genetics | 1997

Reconstitution of human telomerase with the template RNA component hTR and the catalytic protein subunit hTRT.

Scott L. Weinrich; Ron Pruzan; Libin Ma; Michel M. Ouellette; Valeric M. Tesmer; Shawn E. Holt; Andrea G. Bodnar; Serge Lichtsteiner; Nam Woo Kim; James B. Trager; Rebecca D. Taylor; Ruben Carlos; William H. Andrews; Woodring E. Wright; Jerry W. Shay; Calvin B. Harley; Gregg B. Morin


Nucleic Acids Research | 1995

Cataloging altered gene expression in young and senescent cells using enhanced differential display

Maarten H.K. Linskens; Junli Feng; William H. Andrews; Brett E. Enlow; Shahin M. Saati; Leath A. Tonkin; Walter Funk; Bryant Villeponteau


Archive | 1997

Human telomerase catalytic subunit

Thomas R. Cech; Joachim Lingner; Toru M. Nakamura; Karen B. Chapman; Gregg B. Morin; Calvin B. Harley; William H. Andrews


Archive | 1997

Telomerase reverse transcriptase

Thomas R. Cech; Joachim Lingner; Toru Nakamura; Karen B. Chapman; Gregg B. Morin; Calvin B. Harley; William H. Andrews


Rejuvenation Research | 2011

A Natural Product Telomerase Activator As Part of a Health Maintenance Program

Calvin B. Harley; Weimin Liu; Maria A. Blasco; Elsa Vera; William H. Andrews; Laura A. Briggs; Joseph M. Raffaele


Archive | 1998

Antisense compositions for detecting and inhibiting telomerase reverse transcriptase

Thomas R. Cech; Joachim Lingner; Toru Nakamura; Karen B. Chapman; Gregg B. Morin; Calvin B. Harley; William H. Andrews


Archive | 2002

Human telomerase catalytic subunit: diagnostic and therapeutic methods

Thomas R. Cech; Joachim Lingner; Toru Nakamura; Karen B. Chapman; Gregg B. Morin; Calvin B. Harley; William H. Andrews


Archive | 1997

Promoter for telomerase reverse transcriptase

Gregg B. Morin; William H. Andrews

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Gregg B. Morin

University of British Columbia

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Thomas R. Cech

Howard Hughes Medical Institute

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Joachim Lingner

École Polytechnique Fédérale de Lausanne

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Toru M. Nakamura

University of Illinois at Chicago

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