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Dive into the research topics where Tracy S. Mitchell is active.

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Featured researches published by Tracy S. Mitchell.


Journal of Pharmacology and Experimental Therapeutics | 2014

Pharmacologic Profile of the Adnectin BMS-962476, a Small Protein Biologic Alternative to PCSK9 Antibodies for Low-Density Lipoprotein Lowering.

Tracy S. Mitchell; Ginger Chao; Doree Sitkoff; Fred Lo; Hossain Monshizadegan; Daniel Meyers; Simon Low; Katie A. Russo; Rose DiBella; Fabienne M. Denhez; Mian Gao; Joseph E. Myers; Gerald J. Duke; Mark R. Witmer; Bowman Miao; Siew P. Ho; Javed Khan; Rex A. Parker

Proprotein convertase subtilisin kexin-9 (PCSK9) is an important pharmacological target for decreasing low-density lipoprotein (LDL) in cardiovascular disease, although seemingly inaccessible to small molecule approaches. Compared with therapeutic IgG antibodies currently in development, targeting circulating PCSK9 with smaller molecular scaffolds could offer different profiles and reduced dose burdens. This inspired genesis of PCSK9-binding Adnectins, a protein family derived from human fibronectin-10th-type III–domain and engineered for high-affinity target binding. BMS-962476, an ∼11-kDa polypeptide conjugated to polyethylene glycol to enhance pharmacokinetics, binds with subnanomolar affinity to human. The X-ray cocrystal structure of PCSK9 with a progenitor Adnectin shows ∼910 Å2 of PCSK9 surface covered next to the LDL receptor binding site, largely by residues of a single loop of the Adnectin. In hypercholesterolemic, overexpressing human PCSK9 transgenic mice, BMS-962476 rapidly lowered cholesterol and free PCSK9 levels. In genomic transgenic mice, BMS-962476 potently reduced free human PCSK9 (ED50 ∼0.01 mg/kg) followed by ∼2-fold increases in total PCSK9 before return to baseline. Treatment of cynomolgus monkeys with BMS-962476 rapidly suppressed free PCSK9 >99% and LDL-cholesterol ∼55% with subsequent 6-fold increase in total PCSK9, suggesting reduced clearance of circulating complex. Liver sterol response genes were consequently downregulated, following which LDL and total PCSK9 returned to baseline. These studies highlight the rapid dynamics of PCSK9 control over LDL and liver cholesterol metabolism and characterize BMS-962476 as a potent and efficacious PCSK9 inhibitor.


Archive | 2011

Fibronectin based scaffold domain proteins that bind PCSK9

Ray Camphausen; Jonathan Davis; Sharon T. Cload; Fabienne M. Denhez; Amna Saeed-Kothe; Dasa Lipovsek; Ching-Hsiung Frederick Lo; Chee Meng Low; Bowman Miao; Tracy S. Mitchell; Rex A. Parker; Ginger Chao Rakestraw; Katie A. Russo; Doree Sitkoff


Archive | 2011

Serum albumin binding molecules

Michael L. Gosselin; David Fabrizio; Joanna Swain; Tracy S. Mitchell; Ray Camphausen; Sharon T. Cload; Eric Furfine; Paul E. Morin; Ranjan Mukherjee; Simeon I. Taylor


Archive | 2012

Fc fusion proteins comprising novel linkers or arrangements

Ray Camphausen; Amna Saeed-Kothe; Jonathan Davis; Tracy S. Mitchell


Archive | 2014

FIBRONECTIN BASED SCAFFOLD DOMAINS LINKED TO SERUM ALBUMIN OR A MOIETY BINDING THERETO

Ray Camphausen; Tracy S. Mitchell


Archive | 2015

SERUM ALBUMIN-BINDING FIBRONECTIN TYPE III DOMAINS

Tracy S. Mitchell; Michael L. Gosselin; Dasa Lipovsek; Rex A. Parker; Ray Camphausen; Jonathan Davis; David Fabrizio


Archive | 2016

Fast-off rate serum albumin binding fibronectin type iii domains

Stanley R. Krystek; Tracy S. Mitchell; Michael L. Gosselin; Dasa Lipovsek; Juhi Juneja


Archive | 2014

Domaines d'échafaudage à base de fibronectine liés à une sérum albumine ou fragment se liant à celle-ci

Ray Camphausen; Tracy S. Mitchell


Archive | 2012

Fc fusion proteins comprising linkers or new provisions

Ray Camphausen; Amna Saeed-Kothe; Jonathan Davis; Tracy S. Mitchell


Archive | 2012

Fc-fusionsproteine mit neuartigen linkern oder anordnungen

Ray Camphausen; Amna Saeed-Kothe; Jonathan Davis; Tracy S. Mitchell

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