Genetic Encoding of a Non-Canonical Amino Acid for the Generation of Antibody-Drug Conjugates Through a Fast Bioorthogonal Reaction

Benjam&#237; Oller-Salvia

doi:10.3791/58066

JoVE Journal > Chemistry

Chemistry

Codage génétique d’un acide aminé Non canonique pour la génération d’anticorps-médicament conjugués par une réaction rapide Bioorthogonal

Published: September 14, 2018

doi:

10.3791/58066

Please note that all translations are automatically generated. Click here for the English version.

Benjamí Oller-Salvia¹

¹Medical Research Council Laboratory of Molecular Biology

Summary

Abstract

Introduction

Protocol

Representative Results

Discussion

Disclosures

The authors have nothing to disclose.

Acknowledgements

Materials

Expi293F	ThermoFisher Scientific	A14527	HEK suspension cells
Expi293 Expression Medium	ThermoFisher Scientific	A1435101	Expression medium
Antibiotic-antimycotic	ThermoFisher Scientific	15240062	Penicillin-streptomycin-amphotericin B
125mL Polycarbonate Erlenmeyer Flask with Vent Cap	Corning	431143	Shake flasks
Brunswick S41i incubator	Eppendorf	S41I230011	CO2 incubator with a shaker
Sodium hydroxide 4 mol/l (4 N) in aqueous solution	VWR	191373M
Cyclopropene lysine	Sichem	SC-8017	In this study it was synthesized as described by Elliot et al. 2014
Steriflip-GP, 0.22 µm, polyethersulfone, gamma irradiated	Merck Millipore	SCGP00525
Opti-MEM, Reduced Serum Medium	ThermoFisher Scientific	31985070	Reduced serum medium
ExpiFectamine 293 Transfection Kit	ThermoFisher Scientific	A14525	Transfection reagent
5810 R centrifuge	Eppendorf	5811000460
Millex-GP Syringe Filter Unit, 0.22 µm, polyethersulfone, 33 mm, gamma sterilized	Merck Millipore	SLGP033RS
Protein A resin	Sino Biological	10600-P07E-RN-25
Poly-Prep Chromatography Columns, Pkg of 50	Bio-Rad	7311550	Polypropylene chromatography column
Econo-Column Funnel	Bio-Rad	7310003
Sodium citrate	Fluka	71635
ÄKTA explorer FPLC	GE Healthcare
HiTrap HIC Selection Kit	GE Healthcare	28-4110-07	Includes HiTrap 1 mL Butyl HP
Ammonium sulfate	VWR	2133.296
Isopropanol	Honywell	34863-2.5L
Dymethyl sulfoxide	Sigma-Aldrich	D8418-50ML
Tetrazine-vcMMAE	ChemPartner	–	Costum synthesized
Tetrazine-5-TAMRA	Jena Bioscience	CLK-017-05
NuPAGE 4-12% Bis-Tris Gel 1.0mm x 10 well	ThermoFisherScientific	NP0321BOX
Xcell SureLock Mini-Cell	ThermoFisherScientific	EI0001
UltiMate 3000 HPLC	ThermoFisherScientific
Thermo Scientific MAbPac, HIC-20, 4.6 x 100 mm, 5 µm	ThermoFisherScientific	088553
PNGase F	New England BioLabs	P0704S
NanoAcquity	Waters
C4 BEH 1-5 µm 1.0 x 100 mm UPLC column	Waters
96-well microplates for cell culture	ThermoFisherScientific	156545
Human serum	Sigma-Aldrich	H4522-20mL
CO2 incubator	Panasonic
HER2 ECD	Sino Biological	10004-HCCH
Anti-TAMRA	Abcam	an171120
Anti-mouse HRP	Santa Cruz	sc-2005
TMB	BioLengend	421101
Sulfuric acid	Sigma-Aldrich	84727-500ML
PHERAstar FS	BMG Labtech		Plate reader
DMEM	Sigma-Aldrich	D5671-500ML
SK-BR-3	ATCC	HTB-30
MCF-7	ATCC	HTB-22
CellTiterGlo 2.0 Assay	Promega	G9242	Cell viability assay based on the measurement of ATP released after cell lysis. The output signal is luminscence.
Monomethyl Auristatin E	Cayman Chemical	16267
NanoDrop 2000	ThermoFisherScientific		Microvolume spectrophotometer
Human IgG ELISA Quantificaiton Set	Bethyl	E80-104
MaxEnt1 in MassLynx	Waters		Software application for mass spectrum deconvolution
IntantBlue	Expedeon	ISB1L	Coomassie-based stain
Intact MMAE-ADC ELISA Kit (Sandwich Assay)	Epitope Diagnostics, Inc.	KTR 782
Tube 50 mL, 114x28mm, PP	Sarstedt	62.547.254	Conical tube
Amicon Ultra-15 Centrifugal Filter Units 50,000 NMWL	Merck	UFC905024	Centrifugal filtration concentrator (after protein A pull down)
Amicon Ultra-4 Centrifugal Filter Units 50,000 NMWL	Merck	UFC805024	Centrifugal filtration concentrators (after FPLC or HPLC purification)
Zeba Spin Desalting Columns, 7K MWCO, 0.5 mL	ThermoFisherScientific	89882	Size exclusion spin columns
Tube PCR 0.2ml Flat Cap	Thistle Scientific Ltd	AX-PCR-02-C-CS	PCR tubes
Nunc MaxiSorpª flat-bottom	ThermoFisherScientific	44-2404-21	Plates for ELISA

References

Beck, A., Goetsch, L., Dumontet, C., Corvaia, N. Strategies and challenges for the next generation of antibody-drug conjugates. Nature Reviews Drug Discovery. 16 (5), 315-337 (2017).
Wakankar, A. A., et al. Physicochemical Stability of the Antibody−Drug Conjugate Trastuzumab-DM1: Changes due to Modification and Conjugation Processes. Bioconjugate Chemistry. 21 (9), 1588-1595 (2010).
Stan, A. C., Radu, D. L., Casares, S., Bona, C. A., Brumeanu, T. -. D. Antineoplastic Efficacy of Doxorubicin Enzymatically Assembled on Galactose Residues of a Monoclonal Antibody Specific for the Carcinoembryonic Antigen. Cancer Research. 59 (1), 115-121 (1999).
Hamblett, K. J., et al. Effects of Drug Loading on the Antitumor Activity of a Monoclonal Antibody Drug Conjugate. Clinical Cancer Research. 10 (20), 7063-7070 (2004).
Chari, R. V. J., Miller, M. L., Widdison, W. C. Antibody-Drug Conjugates: An Emerging Concept in Cancer Therapy. Angewandte Chemie International Edition. 53 (15), 3796-3827 (2014).
Chin, J. W. Expanding and Reprogramming the Genetic Code. Nature. 550 (7674), 53-60 (2017).
Axup, J. Y., et al. Synthesis of Site-Specific Antibody-Drug Conjugates Using Unnatural Amino Acids. Proceedings of the National Academy of Sciences of the United States of America. 109 (40), 16101-16106 (2012).
Hallam, T. J., Wold, E., Wahl, A., Smider, V. V. Antibody Conjugates with Unnatural Amino Acids. Molecular Pharmaceutics. 12 (6), 1848-1862 (2015).
Tian, F., et al. A General Approach to Site-Specific Antibody Drug Conjugates. Proceedings of the National Academy of Sciences of the United States of America. 111 (5), 1766-1771 (2014).
Kern, J. C., et al. Discovery of Pyrophosphate Diesters as Tunable, Soluble, and Bioorthogonal Linkers for Site-Specific Antibody-Drug Conjugates. Journal of the American Chemical Society. 138 (4), 1430-1445 (2016).
Zimmerman, E. S., et al. Production of Site-Specific Antibody-Drug Conjugates Using Optimized Non-Natural Amino Acids in a Cell-Free Expression System. Bioconjugate Chemistry. 25 (2), 351-361 (2014).
VanBrunt, M. P., et al. Genetically Encoded Azide Containing Amino Acid in Mammalian Cells Enables Site-Specific Antibody-Drug Conjugates Using Click Cycloaddition Chemistry. Bioconjugate Chemistry. 26 (11), 2249-2260 (2015).
Xiao, H., et al. Genetic Incorporation of Multiple Unnatural Amino Acids into Proteins in Mammalian Cells. Angewandte Chemie International Edition. 52 (52), 14080-14083 (2013).
Milles, S., et al. Click Strategies for Single-Molecule Protein Fluorescence. Journal of the American Chemical Society. 134 (11), 5187-5195 (2012).
Lallana, E., Riguera, R., Fernandez-Megia, E. Reliable and Efficient Procedures for the Conjugation of Biomolecules through Huisgen Azide-Alkyne Cycloadditions. Angewandte Chemie International Edition. 50 (38), 8794-8804 (2011).
Koehler, C., et al. Genetic Code Expansion for Multiprotein Complex Engineering. Nature Methods. 13 (12), 997-1000 (2016).
Lyon, R. P., et al. Reducing Hydrophobicity of Homogeneous Antibody-Drug Conjugates Improves Pharmacokinetics and Therapeutic Index. Nature Biotechnology. 33 (7), 733-735 (2015).
Elliott, T. S., et al. Proteome Labeling and Protein Identification in Specific Tissues and at Specific Developmental Stages in an Animal. Nature Biotechnology. 32, 465-472 (2014).
Ravasco, J. M. J. M., Monteiro, C. M., Trindade, A. F. Cyclopropenes: A New Tool for the Study of Biological Systems. Organic Chemistry Frontiers. 4 (6), 1167-1198 (2017).
Yang, J., Šečkutė, J., Cole, C. M., Devaraj, N. K. Live-Cell Imaging of Cyclopropene Tags with Fluorogenic Tetrazine Cycloadditions. Angewandte Chemie International Edition. 124 (30), 7594-7597 (2012).
Oller-Salvia, B., Kym, G., Chin, J. W. Rapid and Efficient Generation of Stable Antibody-Drug Conjugates via an Encoded Cyclopropene and an Inverse-Electron-Demand Diels-Alder Reaction. Angewandte Chemie International Edition. 57, 2831-2834 (2018).
Schmied, W. H., Elsässer, S. J., Uttamapinant, C., Chin, J. W. Efficient Multisite Unnatural Amino Acid Incorporation in Mammalian Cells via Optimized Pyrrolysyl tRNA Synthetase/tRNA Expression and Engineered eRF1. Journal of the American Chemical Society. 136 (44), 15577-15583 (2014).
Junutula, J. R., et al. Site-Specific Conjugation of a Cytotoxic Drug to an Antibody Improves the Therapeutic Index. Nature Biotechnology. 26 (8), 925-932 (2008).
Junutula, J. R., et al. Rapid Identification of Reactive Cysteine Residues for Site-Specific Labeling of Antibody-Fabs. Journal of Immunological Methods. 332 (1), 41-52 (2008).
Doronina, S. O., et al. Development of potent monoclonal antibody auristatin conjugates for cancer therapy. Nature Biotechnology. 21 (7), 778-784 (2003).
Shiraishi, Y., et al. Identification of Highly Reactive Cysteine Residues at Less Exposed Positions in the Fab Constant Region for Site-Specific Conjugation. Bioconjugate Chemistry. 26 (6), 1032-1040 (2015).
Sabourin, M., et al. Increasing Antibody Yield and Modulating Final Product Quality using the Freedom(TM). CHO-S(TM) Production Platform. BMC Proceedings. 5 (8), 102 (2011).
Xiao, Y., Gao, X., Maragh, S., Telford, W. G., Tona, A. Cell Lines as Candidate Reference Materials for Quality Control of ERBB2 Amplification and Expression Assays in Breast Cancer. Clinical Chemistry. 55 (7), 1307-1315 (2009).
Shinmi, D., et al. One-Step Conjugation Method for Site-Specific Antibody-Drug Conjugates through Reactive Cysteine-Engineered Antibodies. Bioconjugate Chemistry. 27 (5), 1324-1331 (2016).
Badescu, G., et al. Bridging Disulfides for Stable and Defined Antibody Drug Conjugates. Bioconjugate Chemistry. 25 (6), 1124-1136 (2014).
Vazquez-Lombardi, R., et al. Transient expression of human antibodies in mammalian cells. Nature Protocols. 13 (1), 99-117 (2018).
Baldi, L., Hacker, D. L., Meerschman, C., Wurm, F. M., Hartley, J. L. . Protein Expression in Mammalian Cells: Methods and Protocols. , 13-26 (2012).

Play Video

PDF

DOI

DOWNLOAD MATERIALS LIST

Cite This Article

Oller-Salvia, B. Genetic Encoding of a Non-Canonical Amino Acid for the Generation of Antibody-Drug Conjugates Through a Fast Bioorthogonal Reaction. J. Vis. Exp. (139), e58066, doi:10.3791/58066 (2018).