Karl D. Hargrave
Boehringer Ingelheim
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Featured researches published by Karl D. Hargrave.
Nature Medicine | 2002
James J. Crute; Christine A. Grygon; Karl D. Hargrave; Bruno Simoneau; Anne-Marie Faucher; Gordon Bolger; Philip Kibler; Michel Liuzzi; Michael G. Cordingley
Herpes simplex virus infections are the cause of significant morbidity, and currently used therapeutics are largely based on modified nucleoside analogs that inhibit viral DNA polymerase function. To target this disease in a new way, we have identified and optimized selective thiazolylphenyl-containing inhibitors of the herpes simplex virus (HSV) helicase-primase enzyme. The most potent compounds inhibited the helicase, the primase and the DNA-dependent ATPase activities of the enzyme with IC50 (50% inhibitory concentration) values less than 100 nM. Inhibition of the enzymatic activities was through stabilization of the interaction between the helicase-primase and DNA substrates, preventing the progression through helicase or primase catalytic cycles. Helicase-primase inhibitors also prevented viral replication as demonstrated in viral growth assays. One compound, BILS 179 BS, displayed an EC50 (effective concentration inhibiting viral growth by 50%) of 27 nM against viral growth with a selectivity index greater than 2,000. Antiviral activity was also demonstrated for multiple strains of HSV, including strains resistant to nucleoside-based therapies. Most importantly, BILS 179 BS was orally active against HSV infections in murine models of HSV-1 and HSV-2 disease and more effective than acyclovir when the treatment frequency per day was reduced or when initiation of treatment was delayed up to 65 hours after infection. These studies validate the use of helicase-primase inhibitors for the treatment of acute herpesvirus infections and provide new lead compounds for optimization and design of superior anti-HSV agents.
Tetrahedron | 1989
John P Devlin; Karl D. Hargrave
This report will provide an assessment of the progress that has been made in the design of immune regulatory agents and will draw attention to those areas that are considered to offer the greatest promise. We will begin with a brief outline of the matrix of cellular events that are associated with the immune response. Compounds that have been reported to alter these events are discussed in the context of the segment of this matrix wherein their primary activity is observed. Emphasis is placed on the diverse structural groups encountered and the opportunities for innovation in synthesis and the analysis of structure-activity relationships. Substances that have demonstrated clinical potential are highlighted
Journal of Medicinal Chemistry | 1983
Karl D. Hargrave; Friedrich K. Hess; James T. Oliver
Journal of Medicinal Chemistry | 1991
Karl D. Hargrave; John R. Proudfoot; Karl G. Grozinger; Ernest Cullen; Suresh R. Kapadia; Usha R. Patel; Victor Fuchs; Scott C. Mauldin; Jana Vitous; Mark L. Behnke; Janice M. Klunder; Kollol Pal; Jerry W. Skiles; Daniel W. McNeil; Janice M. Rose; Grace C. Chow; Mark T. Skoog; Joe C. Wu; Gunther Schmidt; Wolfhard Engel; Wolfgang Eberlein; Tracy D. Saboe; Scot Campbell; Alan S. Rosenthal; Julian Adams
Journal of Medicinal Chemistry | 1992
Janice M. Klunder; Karl D. Hargrave; West M; Ernest Cullen; Kollol Pal; Mark L. Behnke; Kapadia; Daniel W. McNeil; Joe C. Wu; Grace C. Chow
The Journal of Infectious Diseases | 1991
Richard A. Koup; Vincent J. Merluzzi; Karl D. Hargrave; Julian Adams; Karl G. Grozinger; Robert J. Eclmer; John L. Sullivan
AIDS Research and Human Retroviruses | 1992
Peter M. Grob; Joe C. Wu; Kenneth A. Cohen; Richard H. Ingraham; Cheng-Kon Shih; Karl D. Hargrave; Tari L. Mctague; Vincent J. Merluzzi
Archive | 1990
Karl D. Hargrave; John R. Proudfoot; Julian Adams; Karl G. Grozinger; Gunther Schmidt; Wolfhard Engel; Gunther Trummlitz; Wolfgang Eberlein
Archive | 1999
Rajashekhar Betageri; Charles L. Cywin; Karl D. Hargrave; Mary Ann Hoermann; Thomas M. Kirrane; Thomas M. Parks; Usha R. Patel; John R. Proudfoot; Rajiv Sharma; Sanxing Sun; Xiao-Jun Wang
Journal of Medicinal Chemistry | 1992
Philip W. Mui; Stephen P. Jacober; Karl D. Hargrave; Julian Adams