Your search keyword '"Ricky Lieu"' showing total 3 results

1. Rapid and robust antibody Fab fragment crystallization utilizing edge-to-edge beta-sheet packing.

Author

Ricky Lieu, Stephen Antonysamy, Zhanna Druzina, Carolyn Ho, N Rebecca Kang, Anna Pustilnik, Jing Wang, and Shane Atwell

Subjects

Medicine, Science

Abstract

Antibody therapeutics are one of the most important classes of drugs. Antibody structures have become an integral part of predicting the behavior of potential therapeutics, either directly or as the basis of modeling. Structures of Fab:antigen complexes have even greater value. While the crystallization and structure determination of Fabs is easy relative to many other protein classes, especially membrane proteins, broad screening and optimization of crystalline hits is still necessary. Through a comprehensive review of rabbit Fab crystal contacts and their incompatibility with human Fabs, we identified a small secondary structural element from the rabbit light chain constant domain potentially responsible for hindering the crystallization of human Fabs. Upon replacing the human kappa constant domain FG loop (HQGLSSP) with the two residue shorter rabbit loop (QGTTS), we dramatically improved the crystallization of human Fabs and Fab:antigen complexes. Our design, which we call "Crystal Kappa", enables rapid crystallization of human fabs and fab complexes in a broad range of conditions, with less material in smaller screens or from dilute solutions.

Published

2020

2. Optimized clinical performance of growth hormone with an expanded genetic code

Author

Thea Norman, Tsotne Javahishvili, Stuart Bussell, David C. Litzinger, Stephanie Chu, Bruce E. Kimmel, Ricky Lieu, Sami Kaphle, Bee-Cheng Sim, Peter G. Schultz, Thomas L. Daniel, Mike Ong, Anna-Maria A. Hays Putnam, Zhenwei Maio, Ying Buechler, Richard D. DiMarchi, Ho Cho, Andrew R. Hoffman, Guillermo Viramontes, Paola Castiglioni, Douglas W. Axelrod, Becky Gc, Vadim Kraynov, and Nick Knudsen

Subjects

Male, Polymers, Phenylalanine, Mutant, Polyethylene glycol, Biology, Protein Engineering, medicine.disease_cause, Polyethylene Glycols, Rats, Sprague-Dawley, chemistry.chemical_compound, Residue (chemistry), Endocrinology, PEG ratio, Genetic variation, medicine, Animals, Humans, Expanded genetic code, chemistry.chemical_classification, Mutation, Multidisciplinary, Dose-Response Relationship, Drug, Human Growth Hormone, Genetic Variation, Biological Sciences, Rats, Amino acid, chemistry, Biochemistry, Peptides, Ribosomes

Abstract

The ribosomal incorporation of nonnative amino acids into polypeptides in living cells provides the opportunity to endow therapeutic proteins with unique pharmacological properties. We report here the first clinical study of a biosynthetic protein produced using an expanded genetic code. Incorporation of p -acetylphenylalanine (pAcF) at distinct locations in human growth hormone (hGH) allowed site-specific conjugation with polyethylene glycol (PEG) to produce homogeneous hGH variants. A mono-PEGylated mutant hGH modified at residue 35 demonstrated favorable pharmacodynamic properties in GH-deficient rats. Clinical studies in GH-deficient adults demonstrated efficacy and safety comparable to native human growth hormone therapy but with increased potency and reduced injection frequency. This example illustrates the utility of nonnative amino acids to optimize protein therapeutics in an analogous fashion to the use of medicinal chemistry to optimize conventional natural products, low molecular weight drugs, and peptides.

Published

2011

3. Fab-based bispecific antibody formats with robust biophysical properties and biological activity

Author

Arlene Sereno, Brian Kuhlman, Xiufeng Wu, F. Huang, Micheal A. Batt, Steven M. Lewis, Andrew L. Glasebrook, Ricky Lieu, Cody Fine, Carina Torres, S.J. Demarest, J.R. Fitchett, and Caroline Weldon

Subjects

Bispecific antibody, Protein Stability, Chemistry, Stereochemistry, Recombinant Fusion Proteins, Immunology, Biological activity, Computational biology, Protein engineering, Immunoglobulin light chain, Protein stability, Cell Line, Tumor, Antibodies, Bispecific, Humans, Immunology and Allergy, Single-Chain Antibodies, Reports

Abstract

A myriad of innovative bispecific antibody (BsAb) platforms have been reported. Most require significant protein engineering to be viable from a development and manufacturing perspective. Single-chain variable fragments (scFvs) and diabodies that consist only of antibody variable domains have been used as building blocks for making BsAbs for decades. The drawback with Fv-only moieties is that they lack the native-like interactions with CH1/CL domains that make antibody Fab regions stable and soluble. Here, we utilize a redesigned Fab interface to explore 2 novel Fab-based BsAbs platforms. The redesigned Fab interface designs limit heavy and light chain mixing when 2 Fabs are co-expressed simultaneously, thus allowing the use of 2 different Fabs within a BsAb construct without the requirement of one or more scFvs. We describe the stability and activity of a HER2×HER2 IgG-Fab BsAb, and compare its biophysical and activity properties with those of an IgG-scFv that utilizes the variable domains of the same parental antibodies. We also generated an EGFR × CD3 tandem Fab protein with a similar format to a tandem scFv (otherwise known as a bispecific T cell engager or BiTE). We show that the Fab-based BsAbs have superior biophysical properties compared to the scFv-based BsAbs. Additionally, the Fab-based BsAbs do not simply recapitulate the activity of their scFv counterparts, but are shown to possess unique biological activity.

Published

2015