Matthew C. Franklin
Genentech
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Publication
Featured researches published by Matthew C. Franklin.
Cancer Cell | 2004
Matthew C. Franklin; Kendall D. Carey; Felix Vajdos; Daniel J. Leahy; Abraham M. de Vos; Mark X. Sliwkowski
We have determined the 3.2 A X-ray crystal structure of the extracellular domain of the human epidermal growth factor receptor 2 (ErbB2 or HER2) in a complex with the antigen binding fragment of pertuzumab, an anti-ErbB2 monoclonal antibody also known as 2C4 or Omnitarg. Pertuzumab binds to ErbB2 near the center of domain II, sterically blocking a binding pocket necessary for receptor dimerization and signaling. The ErbB2-pertuzumab structure, combined with earlier mutagenesis data, defines the pertuzumab residues essential for ErbB2 interaction. To analyze the ErbB2 side of the interface, we have mutated a number of residues contacting pertuzumab and examined the effects of these mutations on pertuzumab binding and ErbB2-ErbB3 heterodimerization. We have also shown that conserved residues previously shown to be necessary for EGF receptor homodimerization may be dispensible for ErbB2-ErbB3 heterodimerization.
Journal of Medicinal Chemistry | 2012
Jonah Cheung; Michael J. Rudolph; Fiana Burshteyn; Michael S. Cassidy; Ebony N. Gary; James Love; Matthew C. Franklin; Jude J. Height
Human acetylcholinesterase (AChE) is a significant target for therapeutic drugs. Here we present high resolution crystal structures of human AChE, alone and in complexes with drug ligands; donepezil, an Alzheimers disease drug, binds differently to human AChE than it does to Torpedo AChE. These crystals of human AChE provide a more accurate platform for further drug development than previously available.
Journal of Medicinal Chemistry | 2009
Fred E. Cohen; Bruno Alicke; Linda O. Elliott; John A. Flygare; Tatiana Goncharov; Stephen F. Keteltas; Matthew C. Franklin; Stacy Frankovitz; Jean-Philippe Stephan; Vickie Tsui; Domagoj Vucic; Harvey Wong; Wayne J. Fairbrother
A series of IAP antagonists based on an azabicyclooctane scaffold was designed and synthesized. The most potent of these compounds, 14b, binds to the XIAP BIR3 domain, the BIR domain of ML-IAP, and the BIR3 domain of c-IAP1 with K(i) values of 140, 38, and 33 nM, respectively. These compounds promote degradation of c-IAP1, activate caspases, and lead to decreased viability of breast cancer cells without affecting normal mammary epithelial cells. Finally, compound 14b inhibits tumor growth when dosed orally in a breast cancer xenograft model.
Bioorganic & Medicinal Chemistry Letters | 2010
Frederick Cohen; Michael F. T. Koehler; Philippe Bergeron; Linda O. Elliott; John A. Flygare; Matthew C. Franklin; Lewis J. Gazzard; Stephen F. Keteltas; Kevin Lau; Cuong Ly; Vickie Tsui; Wayne J. Fairbrother
A series of IAP antagonists based on thiazole or benzothiazole amide isosteres was designed and synthesized. These compounds were tested for binding to the XIAP-BIR3 and ML-IAP BIR using a fluorescence polarization assay. The most potent of these compounds, 19a and 33b, were found to have K(i)s of 20-30 nM against ML-IAP and 50-60 nM against XIAP-BIR3.
ACS Chemical Biology | 2006
Kerry Zobel; Lan Wang; Eugene Varfolomeev; Matthew C. Franklin; Linda O. Elliott; Heidi J.A. Wallweber; David C. Okawa; John A. Flygare; Domagoj Vucic; Wayne J. Fairbrother; Kurt Deshayes
Biochemical Journal | 2005
Domagoj Vucic; Matthew C. Franklin; Heidi J.A. Wallweber; Kanad Das; Brendan P. Eckelman; Hwain Shin; Linda O. Elliott; Saloumeh Kadkhodayan; Kurt Deshayes; Guy S. Salvesen; Wayne J. Fairbrother
Biochemistry | 2003
Matthew C. Franklin; Saloumeh Kadkhodayan; Heidi Ackerly; Daniela Alexandru; Mark D. Distefano; Linda O. Elliott; John A. Flygare; Grace Mausisa; David C. Okawa; Danny Ong; Domagoj Vucic; Kurt Deshayes; Wayne J. Fairbrother
Biochemistry | 2002
Guangwei Yang; Matthew C. Franklin; Jing Li; Tsung-Chung Lin; William H. Konigsberg
Biochemistry | 2002
Guangwei Yang; Matthew C. Franklin; Jing Li; Tsung-Chung Lin; William H. Konigsberg
Biochemistry | 2000
Timothy L. Born; Matthew C. Franklin; John S. Blanchard