Your search keyword '"Katherine R. Kozak"' showing total 24 results

1. Antibody-Mediated Delivery of Chimeric BRD4 Degraders. Part 2: Improvement of In Vitro Antiproliferation Activity and In Vivo Antitumor Efficacy

Author

Steven J. Hartman, Ying Lu, Wentao Wei, Hao Zhou, Geoffrey Del Rosario, Robert A. Blake, Xiaoyu Zhu, Nicholas Corr, Aaron Fullerton, Shang-Fan Yu, Peter S. Dragovich, Jing Wang, Rebecca K. Rowntree, Donglu Zhang, Hui Yao, Emel Adaligil, Fan Jiang, Hongyan Zhang, Jack Sadowsky, John S. Wai, Jinhua Chen, Thomas H. Pillow, Susan Kaufman, Zijin Xu, Katherine R. Kozak, Jeremy Murray, Shenhua Zhang, Leanna Staben, Josefa dela Cruz-Chuh, Pragya Adhikari, Aimee O'Donohue, Tracy Kleinheinz, Liling Liu, Melinda M. Mulvihill, William S. Sawyer, Yongxin Zhao, and Binqing Wei

Subjects

BRD4, Immunoconjugates, Antineoplastic Agents, Cell Cycle Proteins, Mice, SCID, 01 natural sciences, 03 medical and health sciences, Mouse xenograft, Ubiquitin, In vivo, Antigens, Neoplasm, Cell Line, Tumor, Neoplasms, Drug Discovery, Animals, Humans, 030304 developmental biology, Cell Proliferation, 0303 health sciences, biology, Chemistry, Antibodies, Monoclonal, Dipeptides, Xenograft Model Antitumor Assays, In vitro, 0104 chemical sciences, Cell biology, 010404 medicinal & biomolecular chemistry, Proteasome, Von Hippel-Lindau Tumor Suppressor Protein, Proteolysis, biology.protein, Molecular Medicine, Female, Antibody, Oxidoreductases, Heterocyclic Compounds, 3-Ring, Conjugate, Transcription Factors

Abstract

Heterobifunctional compounds that direct the ubiquitination of intracellular proteins in a targeted manner via co-opted ubiquitin ligases have enormous potential to transform the field of medicinal chemistry. These chimeric molecules, often termed proteolysis-targeting chimeras (PROTACs) in the chemical literature, enable the controlled degradation of specific proteins via their direction to the cellular proteasome. In this report, we describe the second phase of our research focused on exploring antibody-drug conjugates (ADCs), which incorporate BRD4-targeting chimeric degrader entities. We employ a new BRD4-binding fragment in the construction of the chimeric ADC payloads that is significantly more potent than the corresponding entity utilized in our initial studies. The resulting BRD4-degrader antibody conjugates exhibit potent and antigen-dependent BRD4 degradation and antiproliferation activities in cell-based experiments. Multiple ADCs bearing chimeric BRD4-degrader payloads also exhibit strong, antigen-dependent antitumor efficacy in mouse xenograft assessments that employ several different tumor models.

Published

2021

2. Systematic Variation of Pyrrolobenzodiazepine (PBD)-Dimer Payload Physicochemical Properties Impacts Efficacy and Tolerability of the Corresponding Antibody-Drug Conjugates

Author

Peter S. Dragovich, Jun Guo, Josefa dela Cruz-Chuh, Guangmin Li, Binqing Wei, Zijin Xu, Leanna Staben, Geoff Del Rosario, Shang-Fan Yu, Thomas H. Pillow, Katherine R. Kozak, Mary Ann Go, Jinhua Chen, Rebecca K. Rowntree, John S. Wai, Carl Ng, Keyang Xu, Donglu Zhang, S. Cyrus Khojasteh, and Gail Lewis Phillips

Subjects

Models, Molecular, Immunoconjugates, Chemical Phenomena, Pyrrolobenzodiazepine, behavioral disciplines and activities, chemistry.chemical_compound, Benzodiazepines, In vivo, Cell Line, Tumor, Drug Discovery, Moiety, Humans, Pyrroles, Binding site, Cytotoxicity, Cell Proliferation, Binding Sites, DNA, Combinatorial chemistry, In vitro, body regions, chemistry, Molecular Medicine, Nucleic Acid Conformation, Safety, Dimerization, Conjugate

Abstract

Cytotoxic pyrrolobenzodiazepine (PBD)-dimer molecules are frequently utilized as payloads for antibody-drug conjugates (ADCs), and many examples are currently in clinical development. In order to further explore this ADC payload class, the physicochemical properties of various PBD-dimer molecules were modified by the systematic introduction of acidic and basic moieties into their chemical structures. The impact of these changes on DNA binding, cell membrane permeability, and in vitro antiproliferation potency was, respectively, determined using a DNA alkylation assay, PAMPA assessments, and cell-based cytotoxicity measurements conducted with a variety of cancer lines. The modified PBD-dimer compounds were subsequently incorporated into CD22-targeting ADCs, and these entities were profiled in a variety of in vitro and in vivo experiments. The introduction of a strongly basic moiety into the PBD-dimer scaffold afforded a conjugate with dramatically worsened mouse tolerability properties relative to ADCs derived from related payloads, which lacked the basic group.

Published

2020

3. Calicheamicin Antibody-Drug Conjugates with Improved Properties

Author

Chris Frantz, Keyang Xu, Katherine R. Kozak, Thomas H. Pillow, Zijin Xu, Geoffrey Del Rosario, Pragya Adhikari, Douglas D. Leipold, Andrew Polson, Jinhua Chen, Shang-Fan Yu, Mary Ann T. Go, Breanna S. Vollmar, Josefa dela Cruz-Chuh, Peter S. Dragovich, Amrita V. Kamath, Hans Erickson, Fiona Zhong, John S. Wai, Carl Ng, and Melissa Schutten

Subjects

0301 basic medicine, Cancer Research, Immunoconjugates, Gemtuzumab ozogamicin, CD33, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Calicheamicin, medicine, Animals, Humans, Inotuzumab ozogamicin, Antibiotics, Antineoplastic, CD22, Myeloid leukemia, body regions, Disease Models, Animal, 030104 developmental biology, Oncology, chemistry, Calicheamicins, 030220 oncology & carcinogenesis, Cancer research, Linker, medicine.drug, Conjugate

Abstract

Calicheamicin antibody–drug conjugates (ADCs) are effective therapeutics for leukemias with two recently approved in the United States: Mylotarg (gemtuzumab ozogamicin) targeting CD33 for acute myeloid leukemia and Besponsa (inotuzumab ozogamicin) targeting CD22 for acute lymphocytic leukemia. Both of these calicheamicin ADCs are heterogeneous, aggregation-prone, and have a shortened half-life due to the instability of the acid-sensitive hydrazone linker in circulation. We hypothesized that we could improve upon the heterogeneity, aggregation, and circulation stability of calicheamicin ADCs by directly attaching the thiol of a reduced calicheamicin to an engineered cysteine on the antibody via a disulfide bond to generate a linkerless and traceless conjugate. We report herein that the resulting homogeneous conjugates possess minimal aggregation and display high in vivo stability with 50% of the drug remaining conjugated to the antibody after 21 days. Furthermore, these calicheamicin ADCs are highly efficacious in mouse models of both solid tumor (HER2+ breast cancer) and hematologic malignancies (CD22+ non-Hodgkin lymphoma). Safety studies in rats with this novel calicheamicin ADC revealed an increased tolerability compared with that reported for Mylotarg. Overall, we demonstrate that applying novel linker chemistry with site-specific conjugation affords an improved, next-generation calicheamicin ADC.

Published

2020

4. Improved translation of stability for conjugated antibodies using an in vitro whole blood assay

Author

John C. Tran, Carl Ng, Josefa Chuh, Shang-Fan Yu, Siao Ping Tsai, Thomas H. Pillow, Keyang Xu, Phillip Y. Chu, Jack Sadowsky, Dian Su, Robert Tchelepi, Peter S. Dragovich, Katherine R. Kozak, Yichin Liu, Aimee Fourie-O'Donohue, and William S. Sawyer

Subjects

Drug, Antibody-drug conjugate, Immunoconjugates, media_common.quotation_subject, Immunology, In Vitro Techniques, Mass Spectrometry, antibody-drug conjugate, 03 medical and health sciences, 0302 clinical medicine, In vivo, Report, Animals, Humans, Immunology and Allergy, plasma, 030304 developmental biology, Whole blood, media_common, 0303 health sciences, biology, Protein Stability, Chemistry, whole blood, drug modification, In vitro, Biochemistry, 030220 oncology & carcinogenesis, biology.protein, Antibody, Stability, Linker, Chromatography, Liquid, Conjugate

Abstract

For antibody-drug conjugates to be efficacious and safe, they must be stable in circulation to carry the payload to the site of the targeted cell. Several components of a drug-conjugated antibody are known to influence stability: 1) the site of drug attachment on the antibody, 2) the linker used to attach the payload to the antibody, and 3) the payload itself. In order to support the design and optimization of a high volume of drug conjugates and avoid unstable conjugates prior to testing in animal models, we wanted to proactively identify these potential liabilities. Therefore, we sought to establish an in vitro screening method that best correlated with in vivo stability. While traditionally plasma has been used to assess in vitro stability, our evaluation using a variety of THIOMABTM antibody-drug conjugates revealed several disconnects between the stability assessed in vitro and the in vivo outcomes when using plasma. When drug conjugates were incubated in vitro for 24 h in mouse whole blood rather than plasma and then analyzed by affinity capture LC-MS, we found an improved correlation to in vivo stability with whole blood (R2 = 0.87, coefficient of determination) compared to unfrozen or frozen mouse plasma (R2 = 0.34, 0.01, respectively). We further showed that this whole blood assay was also able to predict in vivo stability of other preclinical species such as rat and cynomolgus monkey, as well as in human. The screening method utilized short (24 h) incubation times, as well as a custom analysis software, allowing increased throughput and in-depth biotransformation characterization. While some instabilities that were more challenging to identify remain, the method greatly enhanced the process of screening, optimizing, and lead candidate selection, resulting in the substantial reduction of animal studies.

Published

2020

5. Preclinical pharmacokinetics and pharmacodynamics of DCLL9718A: An antibody-drug conjugate for the treatment of acute myeloid leukemia

Author

Melissa Schutten, Brandon Latifi, Ola Saad, Steven T Laing, Shabkhaiz Masih, Jintang He, Isabel Figueroa, Katherine R. Kozak, Douglas D. Leipold, Randall C. Dere, M. Violet Lee, Brian R. Vuillemenot, Andrew Polson, Keyang Xu, Ben-Quan Shen, Montserrat Carrasco-Triguero, Luna Liu, Dian Su, Victor Yip, Bing Zheng, and Amrita V. Kamath

Subjects

0301 basic medicine, Antibody-drug conjugate, Immunoconjugates, Metabolic Clearance Rate, Immunology, acute myeloid leukemia, Pharmacology, Benzodiazepines, Mice, 03 medical and health sciences, Species Specificity, Pharmacokinetics, Report, hemic and lymphatic diseases, Preclinical pharmacokinetics, Animals, Humans, Immunology and Allergy, Medicine, receptor occupancy, Lectins, C-Type, Pyrroles, Receptor, neoplasms, business.industry, PBD dimer, Antibodies, Monoclonal, Treatment options, Myeloid leukemia, Rats, Macaca fascicularis, 030104 developmental biology, Leukemia, Myeloid, Area Under Curve, Immunoglobulin G, Receptors, Mitogen, Pharmacodynamics, Acute Disease, CLL-1, business, pharmacokinetics, Conjugate

Abstract

Few treatment options are available for acute myeloid leukemia (AML) patients. DCLL9718A is an antibody-drug conjugate that targets C-type lectin-like molecule-1 (CLL-1). This receptor is prevalent on monocytes, neutrophils, and AML blast cells, and unlike CD33, is not expressed on hematopoietic stem cells, thus providing possible hematopoietic recovery. DCLL9718A comprises an anti-CLL-1 IgG1 antibody (MCLL0517A) linked to a pyrrolobenzodiazepine (PBD) dimer payload, via a cleavable disulfide-labile linker. Here, we characterize the in vitro and in vivo stability, the pharmacokinetics (PK) and pharmacodynamics (PD) of DCLL9718A and MCLL0517A in rodents and cynomolgus monkeys. Three key PK analytes were measured in these studies: total antibody, antibody-conjugated PBD dimer and unconjugated PBD dimer. In vitro, DCLL9718A, was stable with most (> 80%) of the PBD dimer payload remaining conjugated to the antibody over 96 hours. This was recapitulated in vivo with antibody-conjugated PBD dimer clearance estimates similar to DCLL9718A total antibody clearance. Both DCLL9718A and MCLL0517A showed linear PK in the non-binding rodent species, and non-linear PK in cynomolgus monkeys, a binding species. The PK data indicated minimal impact of conjugation on the disposition of DCLL9718A total antibody. Finally, in cynomolgus monkey, MCLL0517A showed target engagement at all doses tested (0.5 and 20 mg/kg) as measured by receptor occupancy, and DCLL9718A (at doses of 0.05, 0.1 and 0.2 mg/kg) showed strong PD activity as evidenced by notable reduction in monocytes and neutrophils.

Published

2018

6. Exploration of Pyrrolobenzodiazepine (PBD)-Dimers Containing Disulfide-Based Prodrugs as Payloads for Antibody–Drug Conjugates

Author

Peter S. Dragovich, Sheila Ulufatu, John S. Wai, James Lee, Reginald Delarosa, Carl Ng, Zijin Xu, Chunjiao Chen, Shang-Fan Yu, S. Cyrus Khojasteh, Gail Lewis Phillips, Rebecca K. Rowntree, Keyang Xu, Aimee Fourie-O'Donohue, Zhonghua Pei, Isabel Figueroa, Liling Liu, Josefa dela Cruz-Chuh, Jiawei Lu, Jun Guo, Weiwei Jin, Jing Wang, Jinhua Chen, Eva Lin, Nicola J. Stagg, David Stokoe, Scott E. Martin, Trung Nguyen, Donglu Zhang, Hui Yao, Guangmin Li, Rachana Ohri, Thomas H. Pillow, Katherine R. Kozak, Brandon Latifi, Yuzhong Deng, and Vishal Verma

Subjects

0301 basic medicine, Antibody-drug conjugate, Immunoconjugates, Stereochemistry, Pharmaceutical Science, Pyrrolobenzodiazepine, Cleavage (embryo), Benzodiazepines, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, Drug Discovery, Humans, Prodrugs, Pyrroles, Cysteine, Disulfides, Molecular Structure, Chemistry, Glutathione, Prodrug, In vitro, 030104 developmental biology, 030220 oncology & carcinogenesis, Molecular Medicine, Conjugate

Abstract

A number of cytotoxic pyrrolobenzodiazepine (PBD) monomers containing various disulfide-based prodrugs were evaluated for their ability to undergo activation (disulfide cleavage) in vitro in the presence of either glutathione (GSH) or cysteine (Cys). A good correlation was observed between in vitro GSH stability and in vitro cytotoxicity toward tumor cell lines. The prodrug-containing compounds were typically more potent against cells with relatively high intracellular GSH levels (e.g., KPL-4 cells). Several antibody-drug conjugates (ADCs) were subsequently constructed from PBD dimers that incorporated selected disulfide-based prodrugs. Such HER2 conjugates exhibited potent antiproliferation activity against KPL-4 cells in vitro in an antigen-dependent manner. However, the disulfide prodrugs contained in the majority of such entities were surprisingly unstable toward whole blood from various species. One HER2-targeting conjugate that contained a thiophenol-derived disulfide prodrug was an exception to this stability trend. It exhibited potent activity in a KPL-4 in vivo efficacy model that was approximately three-fold weaker than that displayed by the corresponding parent ADC. The same prodrug-containing conjugate demonstrated a three-fold improvement in mouse tolerability properties in vivo relative to the parent ADC, which did not contain the prodrug.

Published

2018

7. Automated On-tip Affinity Capture Coupled with Mass Spectrometry to Characterize Intact Antibody-Drug Conjugates from Blood

Author

Neha Srikumar, Aimee Fourie-O'Donohue, Yichin Liu, John C. Tran, Phillip Y. Chu, Katherine R. Kozak, and Ke Sherry Li

Subjects

0301 basic medicine, Antibody-drug conjugate, Immunoconjugates, Chromatography, Chemistry, Elution, Antibodies, Monoclonal, Haplorhini, Repeatability, Mass spectrometry, Proteomics, Mass Spectrometry, In vitro, Rats, 03 medical and health sciences, 030104 developmental biology, Structural Biology, In vivo, Animals, Humans, Spectroscopy, Chromatography, Liquid, Conjugate

Abstract

Antibody-drug conjugates (ADCs) present unique challenges for ligand-binding assays primarily due to the dynamic changes of the drug-to-antibody ratio (DAR) distribution in vivo and in vitro. Here, an automated on-tip affinity capture platform with subsequent mass spectrometry analysis was developed to accurately characterize the DAR distribution of ADCs from biological matrices. A variety of elution buffers were tested to offer optimal recovery, with trastuzumab serving as a surrogate to the ADCs. High assay repeatability (CV 3%) was achieved for trastuzumab antibody when captured below the maximal binding capacity of 7.5 μg. Efficient on-tip deglycosylation was also demonstrated in 1 h followed by affinity capture. Moreover, this tip-based platform affords higher throughput for DAR characterization when compared with a well-characterized bead-based method. Graphical Abstract ᅟ.

Published

2018

8. Prediction of non-linear pharmacokinetics in humans of an antibody-drug conjugate (ADC) when evaluation of higher doses in animals is limited by tolerability: Case study with an anti-CD33 ADC

Author

Melissa Schutten, Keyang Xu, Bing Zheng, Aimee Fourie-O'Donohue, Hong Wang, Katherine R. Kozak, Steve R. Leong, Amrita V. Kamath, Andrew Polson, Isabel Figueroa, Montserrat Triguero-Carrasco, and Doug Leipold

Subjects

Antibody-drug conjugate, Immunoconjugates, Sialic Acid Binding Ig-like Lectin 3, Immunology, CD33, Pharmacology, Models, Biological, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Species Specificity, Pharmacokinetics, Cell Line, Tumor, Animals, Humans, Immunology and Allergy, Prospective Studies, Receptor, biology, Chemistry, Antibodies, Monoclonal, Pre-clinical development, Macaca fascicularis, HEK293 Cells, Tolerability, 030220 oncology & carcinogenesis, biology.protein, Antibody, Algorithms, Conjugate

Abstract

For antibody-drug conjugates (ADCs) that carry a cytotoxic drug, doses that can be administered in preclinical studies are typically limited by tolerability, leading to a narrow dose range that can be tested. For molecules with non-linear pharmacokinetics (PK), this limited dose range may be insufficient to fully characterize the PK of the ADC and limits translation to humans. Mathematical PK models are frequently used for molecule selection during preclinical drug development and for translational predictions to guide clinical study design. Here, we present a practical approach that uses limited PK and receptor occupancy (RO) data of the corresponding unconjugated antibody to predict ADC PK when conjugation does not alter the non-specific clearance or the antibody-target interaction. We used a 2-compartment model incorporating non-specific and specific (target mediated) clearances, where the latter is a function of RO, to describe the PK of anti-CD33 ADC with dose-limiting neutropenia in cynomolgus monkeys. We tested our model by comparing PK predictions based on the unconjugated antibody to observed ADC PK data that was not utilized for model development. Prospective prediction of human PK was performed by incorporating in vitro binding affinity differences between species for varying levels of CD33 target expression. Additionally, this approach was used to predict human PK of other previously tested anti-CD33 molecules with published clinical data. The findings showed that, for a cytotoxic ADC with non-linear PK and limited preclinical PK data, incorporating RO in the PK model and using data from the corresponding unconjugated antibody at higher doses allowed the identification of parameters to characterize monkey PK and enabled human PK predictions.

Published

2018

9. Immolation of p-Aminobenzyl Ether Linker and Payload Potency and Stability Determine the Cell-Killing Activity of Antibody–Drug Conjugates with Phenol-Containing Payloads

Author

Leanna Staben, Josefa dela Cruz-Chuh, Hoa Le, Thomas H. Pillow, Binqing Wei, Dian Su, Peter S. Dragovich, Breanna S. Vollmar, Peter W. Fan, S. Cyrus Khojasteh, Gail Lewis Phillips, Yong Ma, Richard Vandlen, Cornelis E. C. A. Hop, Sudheer Bobba, Chenghong Zhang, Jun Guo, Donglu Zhang, Jack Sadowsky, and Katherine R. Kozak

Subjects

Cyclopropanes, 0301 basic medicine, Immunoconjugates, Cell Survival, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Ether, 01 natural sciences, 03 medical and health sciences, chemistry.chemical_compound, Antineoplastic Agents, Immunological, Cell Line, Tumor, Neoplasms, Humans, Phenol, Potency, Brentuximab Vedotin, Pharmacology, Dipeptide, 010405 organic chemistry, Organic Chemistry, Combinatorial chemistry, 0104 chemical sciences, DNA Alkylation, 030104 developmental biology, Cell killing, chemistry, Linker, Biotechnology, Conjugate

Abstract

The valine-citrulline (Val-Cit) dipeptide and p-aminobenzyl (PAB) spacer have been commonly used as a cleavable self-immolating linker in ADC design including in the clinically approved ADC, brentuximab vedotin (Adcetris). When the same linker was used to connect to the phenol of the cyclopropabenzindolone (CBI) (P1), the resulting ADC1 showed loss of potency in CD22 target-expressing cancer cell lines (e.g., BJAB, WSU-DLCL2). In comparison, the conjugate (ADC2) of a cyclopropapyrroloindolone (CPI) (P2) was potent despite the two corresponding free drugs having similar picomolar cell-killing activity. Although the corresponding spirocyclization products of P1 and P2, responsible for DNA alkylation, are a prominent component in buffer, the linker immolation was slow when the PAB was connected as an ether (PABE) to the phenol in P1 compared to that in P2. Additional immolation studies with two other PABE-linked substituted phenol compounds showed that electron-withdrawing groups accelerated the immolation to release an acidic phenol-containing payload (to delocalize the negative charge on the anticipated anionic phenol oxygen during immolation). In contrast, efficient immolation of LD4 did not result in an active ADC4 because the payload (P4) had a low potency to kill cells. In addition, nonimmolation of LD5 did not affect the cell-killing potency of its ADC5 since immolation is not required for DNA alkylation by the center-linked pyrrolobenzodiazepine. Therefore, careful evaluation needs to be conducted when the Val-Cit-PAB linker is used to connect antibodies to a phenol-containing drug as the linker immolation, as well as payload potency and stability, affects the cell-killing activity of an ADC.

Published

2018

10. Pyrrolobenzodiazepine Dimer Antibody–Drug Conjugates: Synthesis and Evaluation of Noncleavable Drug-Linkers

Author

Binqing Wei, Janet Gunzner-Toste, Guangmin Li, Helga Raab, Susan D. Spencer, Gail Lewis Phillips, Shang-Fan Yu, Katherine R. Kozak, Rachana Ohri, Jeffrey Lau, Philip Howard, Andrew Polson, Brian Safina, Luke Masterson, John A. Flygare, Thomas H. Pillow, Martine Darwish, Stephen J. Gregson, Gyoung-Dong Kang, and Josefa dela Cruz-Chuh

Subjects

Models, Molecular, 0301 basic medicine, Immunoconjugates, Cell Survival, Receptor, ErbB-2, Stereochemistry, Sialic Acid Binding Ig-like Lectin 2, Triazole, Pyrrolobenzodiazepine, Antineoplastic Agents, Breast Neoplasms, Benzodiazepines, Mice, 03 medical and health sciences, chemistry.chemical_compound, In vivo, Cell Line, Tumor, Neoplasms, Drug Discovery, Animals, Humans, Pyrroles, Maleimide, Piperazine, 030104 developmental biology, chemistry, Molecular Medicine, Female, Dimerization, Linker, Conjugate, Cysteine

Abstract

Three rationally designed pyrrolobenzodiazepine (PBD) drug-linkers have been synthesized via intermediate 19 for use in antibody–drug conjugates (ADCs). They lack a cleavable trigger in the linker and consist of a maleimide for cysteine antibody conjugation, a hydrophilic spacer, and either an alkyne (6), triazole (7), or piperazine (8) link to the PBD. In vitro IC50 values were 11–48 ng/mL in HER2 3+ SK-BR-3 and KPL-4 (7 inactive) for the anti-HER2 ADCs (HER2 0 MCF7, all inactive) and 0.10–1.73 μg/mL (7 inactive) in CD22 3+ BJAB and WSU-DLCL2 for anti-CD22 ADCs (CD22 0 Jurkat, all inactive at low doses). In vivo antitumor efficacy for the anti-HER2 ADCs in Founder 5 was observed with tumor stasis at 0.5–1 mg/kg, 1 mg/kg, and 3–6 mg/kg for 6, 8, and 7, respectively. Tumor stasis at 2 mg/kg was observed for anti-CD22 6 in WSU-DLCL2. In summary, noncleavable PBD-ADCs exhibit potent activity, particularly in HER2 models.

Published

2017

11. Development of Efficient Chemistry to Generate Site-Specific Disulfide-Linked Protein– and Peptide–Payload Conjugates: Application to THIOMAB Antibody–Drug Conjugates

Author

Douglas D. Leipold, Jinhua Chen, Aimee O'Donohue, Gang Yan, Zijin Xu, Shanique Martin, Gail Lewis Phillips, Josefa dela Cruz-Chuh, Thomas H. Pillow, Changrong He, Fang Fan, John S. Wai, Jintang He, Geoffrey Del Rosario, Carl Ng, Phillip Y. Chu, Shang-Fan Yu, Luna Liu, Dian Su, Guangmin Li, Keyang Xu, Yanli Wang, Katherine R. Kozak, Donglu Zhang, Hui Yao, and Jack Sadowsky

Subjects

0301 basic medicine, Drug, Immunoconjugates, media_common.quotation_subject, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Peptide, Conjugated system, Protein Engineering, 01 natural sciences, Mice, 03 medical and health sciences, Cell Line, Tumor, Animals, Humans, Cysteine, Disulfides, media_common, Pharmacology, chemistry.chemical_classification, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, Protein engineering, Combinatorial chemistry, Small molecule, 0104 chemical sciences, Cell Transformation, Neoplastic, 030104 developmental biology, biology.protein, Antibody, Peptides, Biotechnology, Conjugate

Abstract

Conjugation of small molecule payloads to cysteine residues on proteins via a disulfide bond represents an attractive strategy to generate redox-sensitive bioconjugates, which have value as potential diagnostic reagents or therapeutics. Advancement of such "direct-disulfide" bioconjugates to the clinic necessitates chemical methods to form disulfide connections efficiently, without byproducts. The disulfide connection must also be resistant to premature cleavage by thiols prior to arrival at the targeted tissue. We show here that commonly employed methods to generate direct disulfide-linked bioconjugates are inadequate for addressing these challenges. We describe our efforts to optimize direct-disulfide conjugation chemistry, focusing on the generation of conjugates between cytotoxic payloads and cysteine-engineered antibodies (i.e., THIOMAB antibody-drug conjugates, or TDCs). This work culminates in the development of novel, high-yielding conjugation chemistry for creating direct payload disulfide connections to any of several Cys mutation sites in THIOMAB antibodies or to Cys sites in other biomolecules (e.g., human serum albumin and cell-penetrating peptides). We conclude by demonstrating that hindered direct disulfide TDCs with two methyl groups adjacent to the disulfide, which have heretofore not been described for any bioconjugate, are more stable and more efficacious in mouse tumor xenograft studies than less hindered analogs.

Published

2017

12. Antibody Conjugation of a Chimeric BET Degrader Enables in vivo Activity

Author

Isabel Figueroa, Shang-Fan Yu, Hao Zhou, Ruina Li, Hongyan Zhang, Douglas D. Leipold, Peter S. Dragovich, Karen E. Gascoigne, Amrita V. Kamath, Thomas H. Pillow, Gauri Deshmukh, Pragya Adhikari, Jinhua Chen, John S. Wai, Xinxin Wang, Robert A. Blake, Richard Zang, Xiaoyu Zhu, Tracy Kleinheinz, Chun Sing Li, Donglu Zhang, Geoffrey Del Rosario, Rebecca K. Rowntree, Hui Yao, Melinda M. Mulvihill, Katherine R. Kozak, Jack Sadowsky, Susan Kaufman, Aimee O'Donohue, Cong Wu, Zijin Xu, and Brandon Latifi

Subjects

Antibody-drug conjugate, Immunoconjugates, Cell Survival, Cell Cycle Proteins, Mice, SCID, Protein degradation, 01 natural sciences, Biochemistry, Heterocyclic Compounds, 4 or More Rings, Proto-Oncogene Proteins c-myc, Mice, In vivo, Cell Line, Tumor, Drug Discovery, Animals, Humans, Lectins, C-Type, General Pharmacology, Toxicology and Pharmaceutics, Pharmacology, Drug Carriers, 010405 organic chemistry, Chemistry, Organic Chemistry, Antibodies, Monoclonal, Surface Plasmon Resonance, Fusion protein, Small molecule, Xenograft Model Antitumor Assays, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Leukemia, Myeloid, Acute, Von Hippel-Lindau Tumor Suppressor Protein, Receptors, Mitogen, Drug delivery, Proteolysis, Biophysics, Molecular Medicine, Female, Linker, Conjugate, Half-Life, Protein Binding, Transcription Factors

Abstract

The ability to selectively degrade proteins with bifunctional small molecules has the potential to fundamentally alter therapy in a variety of diseases. However, the relatively large size of these chimeric molecules often results in challenging physico-chemical properties (e. g., low aqueous solubility) and poor pharmacokinetics which may complicate their in vivo applications. We recently discovered an exquisitely potent chimeric BET degrader (GNE-987) which exhibited picomolar cell potencies but also demonstrated low in vivo exposures. In an effort to improve the pharmacokinetic properties of this molecule, we discovered the first degrader-antibody conjugate by attaching GNE-987 to an anti-CLL1 antibody via a novel linker. A single IV dose of the conjugate afforded sustained in vivo exposures that resulted in antigen-specific tumor regressions. Enhancement of a chimeric protein degrader with poor in vivo properties through antibody conjugation thereby expands the utility of directed protein degradation as both a biological tool and a therapeutic possibility.

Published

2019

13. Evaluation and use of an anti-cynomolgus monkey CD79b surrogate antibody-drug conjugate to enable clinical development of polatuzumab vedotin

Author

Shan Chung, Mary Ann T. Go, Kirsten Achilles Poon, Donna W. Lee, Daniela Bumbaca Yadav, Dimitry M. Danilenko, Marna Williams, Denise Nazzal, Katherine R. Kozak, Dongwei Li, Bing Zheng, Franklin Fuh, Andrew Polson, Randall C. Dere, Shang-Fan Yu, and Saileta Prabhu

Subjects

0301 basic medicine, Male, Antibody-drug conjugate, Immunoconjugates, medicine.drug_class, Molecular Conformation, Antineoplastic Agents, Mice, SCID, Pharmacology, Monoclonal antibody, Antibodies, Monoclonal, Humanized, Cell Line, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, 0302 clinical medicine, medicine, Animals, Humans, Binding Sites, biology, Dose-Response Relationship, Drug, business.industry, Receptors, IgG, Antibodies, Monoclonal, Neoplasms, Experimental, medicine.disease, Burkitt Lymphoma, Research Papers, Non-Hodgkin's lymphoma, Polatuzumab vedotin, Rats, body regions, Macaca fascicularis, 030104 developmental biology, Monomethyl auristatin E, chemistry, Monoclonal, biology.protein, Female, Antibody, business, 030217 neurology & neurosurgery, CD79 Antigens, Conjugate, Research Paper

Abstract

Background and Purpose Polatuzumab vedotin is an antibody–drug conjugate (ADC) being developed for non‐Hodgkin's lymphoma. It contains a humanized anti‐CD79b IgG1 monoclonal antibody linked to monomethyl auristatin E (MMAE), an anti‐mitotic agent. Polatuzumab vedotin binds to human CD79b only. Therefore, a surrogate ADC that binds to cynomolgus monkey CD79b was used to determine CD79b‐mediated pharmacological effects in the monkey and to enable first‐in‐human clinical trials. Experimental Approach Polatuzumab vedotin, the surrogate ADC, and the corresponding antibodies were evaluated in different assays in vitro and in animals. In vitro assessments included binding to peripheral blood mononuclear cells from different species, binding to a human and monkey CD79b‐expressing cell line, binding to human Fcγ receptors, and stability in plasma across species. In vivo, ADCs were assessed for anti‐tumour activity in mice, pharmacokinetics/pharmacodynamics in monkeys, and toxicity in rats and monkeys. Key Results Polatuzumab vedotin and surrogate ADC bind with similar affinity to human and cynomolgus monkey B cells, respectively. Comparable in vitro plasma stability, in vivo anti‐tumour activity, and mouse pharmacokinetics were also observed between the surrogate ADC and polatuzumab vedotin. In monkeys, only the surrogate ADC showed B‐cell depletion and B‐cell‐mediated drug disposition, but both ADCs showed similar MMAE‐driven myelotoxicity, as expected. Conclusions and Implications The suitability of the surrogate ADC for evaluation of CD79b‐dependent pharmacology was demonstrated, and anti‐tumour activity, pharmacokinetics/pharmacodynamics, and toxicity data with both ADCs supported the entry of polatuzumab vedotin into clinical trials.

Published

2018

14. Modulating Antibody-Drug Conjugate Payload Metabolism by Conjugation Site and Linker Modification

Author

H. Zhou, Ely Cosino, Keyang Xu, Yichin Liu, Josefa dela Cruz-Chuh, Yong Ma, Thomas H. Pillow, Surinder Kaur, Aimee Fourie-O'Donohue, Luna Liu, Geoffrey Del Rosario, Jintang He, Jeff Lau, Christopher Nelson, Dian Su, Martine Darwish, Richard Vandlen, Shang-Fan Yu, Carl Ng, Chunjiao Chen, Jiawei Lu, Rachana Ohri, Donglu Zhang, Helen Davis, Katherine R. Kozak, Wenwen Cai, and Jack Sadowsky

Subjects

0301 basic medicine, Antibody-drug conjugate, Immunoconjugates, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Antibodies, 03 medical and health sciences, 0302 clinical medicine, Drug Stability, In vivo, Humans, Immunologic Factors, Antigens, Pharmacology, Binding Sites, Chemistry, Payload, Organic Chemistry, technology, industry, and agriculture, Metabolism, body regions, 030104 developmental biology, Pharmaceutical Preparations, Homogeneous, Cryptophycin, 030220 oncology & carcinogenesis, Biophysics, Linker, Biotechnology, Conjugate

Abstract

Previous investigations on antibody-drug conjugate (ADC) stability have focused on drug release by linker-deconjugation due to the relatively stable payloads such as maytansines. Recent development of ADCs has been focused on exploring technologies to produce homogeneous ADCs and new classes of payloads to expand the mechanisms of action of the delivered drugs. Certain new ADC payloads could undergo metabolism in circulation while attached to antibodies and thus affect ADC stability, pharmacokinetics, and efficacy and toxicity profiles. Herein, we investigate payload stability specifically and seek general guidelines to address payload metabolism and therefore increase the overall ADC stability. Investigation was performed on various payloads with different functionalities (e.g., PNU-159682 analog, tubulysin, cryptophycin, and taxoid) using different conjugation sites (HC-A118C, LC-K149C, and HC-A140C) on THIOMAB antibodies. We were able to reduce metabolism and inactivation of a broad range of payloads of THIOMAB antibody-drug conjugates by employing optimal conjugation sites (LC-K149C and HC-A140C). Additionally, further payload stability was achieved by optimizing the linkers. Coupling relatively stable sites with optimized linkers provided optimal stability and reduction of payloads metabolism in circulation in vivo.

Published

2018

15. Conjugation of Indoles to Antibodies through a Novel Self-Immolating Linker

Author

Peter S. Dragovich, Keyang Xu, John S. Wai, Jason Oeh, Willem den Besten, Yong Ma, Richard Vandlen, Ellen Ingalla, Fang Fan, Ingrid E. Wertz, Chunjiao Chen, Steven R. Leong, Deepak Sampath, Jiawei Lu, Donglu Zhang, Katherine R. Kozak, Thomas H. Pillow, Steven J. Hartman, Breanna S. Vollmar, Changrong He, Zijin Xu, Robert A. Blake, Gail Lewis Phillips, Josefa Chuh, Rebecca K. Rowntree, Jinhua Chen, Michelle Nannini, Rachana Ohri, Jintang He, Aimee Fourie, and Lingyao Meng

Subjects

Immunoconjugates, Indoles, Estrogen receptor, 010402 general chemistry, 01 natural sciences, Catalysis, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Line, Tumor, Moiety, Animals, Humans, skin and connective tissue diseases, Whole blood, biology, Chemistry, Organic Chemistry, Antibodies, Monoclonal, General Chemistry, 0104 chemical sciences, Biochemistry, 030220 oncology & carcinogenesis, Drug delivery, biology.protein, MCF-7 Cells, Antibody, Linker, Selective Estrogen Receptor Down Regulator, Conjugate

Abstract

A novel strategy to attach indole-containing payloads to antibodies through a carbamate moiety and a self-immolating, disulfide-based linker is described. This new strategy was employed to connect a selective estrogen receptor down-regulator (SERD) to various antibodies in a site-selective manner. The resulting conjugates displayed potent, antigen-dependent down-regulation of estrogen receptor levels in MCF7-neo/HER2 and MCF7-hB7H4 cells. They also exhibited similar antigen-dependent modulation of the estrogen receptor in tumors when administered intravenously to mice bearing MCF7-neo/HER2 tumor xenografts. The indole-carbamate moiety present in the new linker was stable in whole blood from various species and also exhibited good in vivo stability properties in mice.

Published

2018

16. High-Throughput Cysteine Scanning To Identify Stable Antibody Conjugation Sites for Maleimide- and Disulfide-Based Linkers

Author

Aaron B. Bos, Athena W. Wong, Hans Erickson, Rachana Ohri, Richard Vandlen, Helga Raab, Paul Polakis, Siao Ping Tsai, Katherine R. Kozak, Yichin Liu, Jiten Bhakta, Carl Ng, Ryan Cook, Sunil Bhakta, Josefa dela Cruz-Chuh, Farzam Farahi, Thomas H. Pillow, Binqing Wei, Jagath Reddy Junutula, and Aimee Fourie-O'Donohue

Subjects

0301 basic medicine, Models, Molecular, Immunoconjugates, Stereochemistry, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Protein aggregation, Maleimides, 03 medical and health sciences, chemistry.chemical_compound, Protein Aggregates, Antineoplastic Agents, Immunological, Drug Stability, Animals, Humans, Cysteine, Disulfides, Maleimide, Pharmacology, biology, Chemistry, Protein Stability, Organic Chemistry, Mutagenesis, Trastuzumab, Small molecule, High-Throughput Screening Assays, Rats, 030104 developmental biology, Nat, biology.protein, Mutagenesis, Site-Directed, Antibody, Oligopeptides, Biotechnology, Conjugate

Abstract

THIOMAB antibody technology utilizes cysteine residues engineered onto an antibody to allow for site-specific conjugation. The technology has enabled the exploration of different attachment sites on the antibody in combination with small molecules, peptides, or proteins to yield antibody conjugates with unique properties. As reported previously ( Shen , B. Q. , et al. ( 2012 ) Nat. Biotechnol. 30 , 184 - 189 ; Pillow , T. H. , et al. ( 2017 ) Chem. Sci. 8 , 366 - 370 ), the specific location of the site of conjugation on an antibody can impact the stability of the linkage to the engineered cysteine for both thio-succinimide and disulfide bonds. High stability of the linkage is usually desired to maximize the delivery of the cargo to the intended target. In the current study, cysteines were individually substituted into every position of the anti-HER2 antibody (trastuzumab), and the stabilities of drug conjugations at those sites were evaluated. We screened a total of 648 THIOMAB antibody-drug conjugates, each generated from a trastuzamab prepared by sequentially mutating non-cysteine amino acids in the light and heavy chains to cysteine. Each THIOMAB antibody variant was conjugated to either maleimidocaproyl-valine-citrulline-p-aminobenzyloxycarbonyl-monomethyl auristatin E (MC-vc-PAB-MMAE) or pyridyl disulfide monomethyl auristatin E (PDS-MMAE) using a high-throughput, on-bead conjugation and purification method. Greater than 50% of the THIOMAB antibody variants were successfully conjugated to both MMAE derivatives with a drug to antibody ratio (DAR) of0.5 and50% aggregation. The relative in vitro plasma stabilities for approximately 750 conjugates were assessed using enzyme-linked immunosorbent assays, and stable sites were confirmed with affinity-capture LC/MS-based detection methods. Highly stable conjugation sites for the two types of MMAE derivatives were identified on both the heavy and light chains. Although the stabilities of maleimide conjugates were shown to be greater than those of the disulfide conjugates, many sites were identified that were stable for both. Furthermore, in vitro stabilities of selected stable sites translated across different cytotoxic payloads and different target antibodies as well as to in vivo stability.

Published

2018

17. Intratumoral Payload Concentration Correlates with the Activity of Antibody-Drug Conjugates

Author

Cornelis E. C. A. Hop, Donglu Zhang, Katherine R. Kozak, Keyang Xu, Shang-Fan Yu, Jack Sadowsky, S. Cyrus Khojasteh, Yong Ma, Thomas H. Pillow, Andrew Polson, Dian Su, and Peter S. Dragovich

Subjects

0301 basic medicine, Drug, Cancer Research, Immunoconjugates, Receptor, ErbB-2, media_common.quotation_subject, Mice, Nude, Mice, SCID, Antibodies, 03 medical and health sciences, Benzodiazepines, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, Pyrroles, media_common, Mice, Inbred BALB C, biology, Chemistry, Payload (computing), Cancer, medicine.disease, Xenograft Model Antitumor Assays, Tumor Burden, body regions, Drug Liberation, 030104 developmental biology, Key factors, Oncology, Cancer research, Molecular mechanism, biology.protein, Antibody, Linker, Conjugate

Abstract

Antibody–drug conjugates (ADC) have become important scaffolds for targeted cancer therapies. However, ADC exposure–response correlation is not well characterized. We demonstrated that intratumor payload exposures correlated well with the corresponding efficacies of several disulfide-linked ADCs, bearing an DNA alkylating agent, pyrrolo[2,1-c][1,4]benzodiazepine-dimer (PBD), in HER2-expressing xenograft models. The correlation suggests that a threshold concentration of intratumor payload is required to support sustained efficacy and an ADC can deliver an excessive level of payload to tumors that does not enhance efficacy (“Plateau” effect). In contrast to tumor PBD concentrations, related assessments of systemic exposures, plasma stability, and drug-to-antibody ratio changes of related ADCs did not consistently rationalize the observed ADC efficacies. A minimal efficacious dose could be determined by ADC dose-fractionation studies in the xenograft models. Mechanistic investigations revealed that both linker immolation and linker disulfide stability are the key factors that determine intratumor PBD concentrations. Overall, this study demonstrates how a linker design can impact ADC efficacy and that the intratumor exposure of a payload drug as the molecular mechanism quantitatively correlate with and predict the antitumor efficacy of ADCs. Mol Cancer Ther; 17(3); 677–85. ©2018 AACR.

Published

2017

18. Stabilizing a Tubulysin Antibody-Drug Conjugate To Enable Activity Against Multidrug-Resistant Tumors

Author

Geoffrey Del Rosario, Jun Guo, Jinhua Chen, Zijin Xu, Shang-Fan Yu, Gang Yan, Andrew Polson, Luna Liu, Rachana Ohri, Jeffrey Lau, Bing Zheng, Byoung-Chul Lee, H. Zhou, Keyang Xu, Jiawei Lu, John S. Wai, Leanna Staben, Josefa dela Cruz-Chuh, Thomas H. Pillow, Gail Lewis Phillips, Katherine R. Kozak, and Wenwen Cai

Subjects

0301 basic medicine, Drug, Antibody-drug conjugate, Tertiary amine, 010405 organic chemistry, Chemistry, media_common.quotation_subject, medicine.medical_treatment, Organic Chemistry, Pharmacology, 01 natural sciences, Biochemistry, 0104 chemical sciences, Targeted therapy, 03 medical and health sciences, 030104 developmental biology, Mechanism of action, In vivo, Drug Discovery, medicine, medicine.symptom, Cytotoxicity, media_common, Conjugate

Abstract

The tubulysins are promising anticancer cytotoxic agents due to the clinical validation of their mechanism of action (microtubule inhibition) and their particular activity against multidrug-resistant tumor cells. Yet their high potency and subsequent systemic toxicity make them prime candidates for targeted therapy, particularly in the form of antibody–drug conjugates (ADCs). Here we report a strategy to prepare stable and bioreversible conjugates of tubulysins to antibodies without loss of activity. A peptide trigger along with a quaternary ammonium salt linker connection to the tertiary amine of tubulysin provided ADCs that were potent in vitro. However, we observed metabolism of a critical acetate ester of the drug in vivo, resulting in diminished conjugate activity. We were able to circumvent this metabolic liability with the judicious choice of a propyl ether replacement. This modified tubulysin ADC was stable and effective against multidrug-resistant lymphoma cell lines and tumors.

Published

2017

19. Total Antibody Quantification for MMAE-Conjugated Antibody–Drug Conjugates: Impact of Assay Format and Reagents

Author

Ryan Cook, Crystal Zhang, Rachana Ohri, Helga Raab, Leslie Roth, Aimee Fourie-O'Donohue, Siao Ping Tsai, Wai Lee T. Wong, Katherine R. Kozak, Josefa Chuh, Martine Darwish, Kedan Lin, Elton Chan, and Pamela Chan

Subjects

Drug, medicine.drug_class, media_common.quotation_subject, Biomedical Engineering, Pharmaceutical Science, Antineoplastic Agents, Enzyme-Linked Immunosorbent Assay, Bioengineering, Mice, SCID, Conjugated system, Monoclonal antibody, Mice, chemistry.chemical_compound, Pharmacokinetics, medicine, Animals, media_common, Pharmacology, Chromatography, biology, Immunotoxins, Organic Chemistry, Tubulin Modulators, Monomethyl auristatin E, chemistry, Reagent, biology.protein, Antibody, Oligopeptides, Biotechnology, Conjugate

Abstract

Antibody-drug conjugates (ADCs) are target-specific anticancer agents consisting of cytotoxic drugs covalently linked to a monoclonal antibody. The number of ADCs in the clinic is growing, and therefore thorough characterization of the quantitative assays used to measure ADC concentrations in support of pharmacokinetic, efficacy, and safety studies is of increasing importance. Cytotoxic drugs such as the tubulin polymerization inhibiting auristatin, monomethyl auristatin E, have been conjugated to antibodies via cleavable linkers (MC-vc-PAB) through internal cysteines. This results in a heterogeneous mixture of antibody species with drug-to-antibody ratios (DAR) ranging from 0 to 8. In order to characterize the assays used to quantitate total MC-vc-PAB-MMAE ADCs (conjugated and unconjugated antibody), we used purified fractions with defined DARs from 6 therapeutic antibodies to evaluate different assay formats and reagents. Our investigations revealed that for quantitation of total antibody, including all unconjugated and conjugated antibody species, sandwich ELISA formats did not always allow for recovery of all purified DAR fractions (DAR 0-8) to within ±20% of the expected values at the reagent concentrations tested. In evaluating alternative approaches, we found that the recovery of DAR fractions with semihomogeneous assay (SHA) formats, in which sample, capture, and detection reagents are preincubated in solution, were less affected by the antibody's MMAE drug load as compared to traditional stepwise sandwich ELISAs. Thus, choosing the optimal assay format and reagents for total antibody assays is valuable for developing accurate quantitative assays.

Published

2013

20. Decoupling stability and release in disulfide bonds with antibody-small molecule conjugates

Author

Keyang Xu, Geoffrey Del Rosario, Rachana Ohri, Jagath Reddy Junutula, Edward Ha, John A. Flygare, Donglu Zhang, Thomas H. Pillow, Jack Sadowsky, Katherine R. Kozak, Jintang He, Sunil Bhakta, and Shang-Fan Yu

Subjects

010405 organic chemistry, Stereochemistry, Catabolism, media_common.quotation_subject, Catabolite repression, General Chemistry, 010402 general chemistry, Cleavage (embryo), 01 natural sciences, Small molecule, 0104 chemical sciences, chemistry.chemical_compound, Chemistry, chemistry, Functional group, Biophysics, Internalization, Intracellular, media_common, Conjugate

Abstract

A novel bioconjugation strategy utilizes a disulfide bond to site-specifically couple a small molecule drug to an antibody, enabling both high circulation stability and quick intracellular release., Disulfide bonds provide a bioactivatable connection with applications in imaging and therapy. The circulation stability and intracellular release of disulfides are problematically coupled in that increasing stability causes a corresponding decrease in cleavage and payload release. However, an antibody offers the potential for a reversible stabilization. We examined this by attaching a small molecule directly to engineered cysteines in an antibody. At certain sites this unhindered disulfide was stable in circulation yet cellular internalization and antibody catabolism generated a disulfide catabolite that was rapidly reduced. We demonstrated that this stable connection and facile release is applicable to a variety of payloads. The ability to reversibly stabilize a labile functional group with an antibody may offer a way to improve targeted probes and therapeutics.

Published

2016

21. Targeted drug delivery through the traceless release of tertiary and heteroaryl amines from antibody-drug conjugates

Author

Jun Guo, Binqing Wei, Leanna Staben, Carl Ng, Shang-Fan Yu, Tao Wang, MaryAnn Go, Yanzhou Liu, Aimee Fourie-O'Donohue, Katherine R. Kozak, Xin Linghu, Nathaniel L. Segraves, Sophie M. Lehar, Richard Vandlen, Gail Lewis Phillips, John A. Flygare, Keyang Xu, Sanjeev Mariathasan, Stefan G. Koenig, Jinhua Chen, Thomas H. Pillow, Donglu Zhang, and Josefa Chuh

Subjects

Drug, Immunoconjugates, Cell Survival, General Chemical Engineering, media_common.quotation_subject, Antineoplastic Agents, 010402 general chemistry, 01 natural sciences, chemistry.chemical_compound, Therapeutic index, Drug Stability, In vivo, Amide, Cell Line, Tumor, Humans, Amines, media_common, Drug Carriers, 010405 organic chemistry, Antibodies, Monoclonal, General Chemistry, Combinatorial chemistry, Cathepsins, In vitro, 0104 chemical sciences, Anti-Bacterial Agents, Quaternary Ammonium Compounds, Drug Liberation, chemistry, Targeted drug delivery, Pharmaceutical Preparations, Solubility, Drug delivery, Hydrophobic and Hydrophilic Interactions, Conjugate

Abstract

The reversible attachment of a small-molecule drug to a carrier for targeted delivery can improve pharmacokinetics and the therapeutic index. Previous studies have reported the delivery of molecules that contain primary and secondary amines via an amide or carbamate bond; however, the ability to employ tertiary-amine-containing bioactive molecules has been elusive. Here we describe a bioreversible linkage based on a quaternary ammonium that can be used to connect a broad array of tertiary and heteroaryl amines to a carrier protein. Using a concise, protecting-group-free synthesis we demonstrate the chemoselective modification of 12 complex molecules that contain a range of reactive functional groups. We also show the utility of this connection with both protease-cleavable and reductively cleavable antibody-drug conjugates that were effective and stable in vitro and in vivo. Studies with a tertiary-amine-containing antibiotic show that the resulting antibody-antibiotic conjugate provided appropriate stability and release characteristics and led to an unexpected improvement in activity over the conjugates previously connected via a carbamate.

Published

2016

22. Differential Effects of Predosing on Tumor and Tissue Uptake of an 111In-Labeled Anti-TENB2 Antibody–Drug Conjugate

Author

C. Andrew Boswell, Aimee Fourie, Eduardo E. Mundo, Paul Polakis, Leslie A. Khawli, Crystal Zhang, Shang-Fan Yu, Weiguang Mao, Katherine R. Kozak, Jennifer A. Lacap, Shannon Stainton, and Kedan Lin

Subjects

Male, Biodistribution, Antibody-drug conjugate, Immunoconjugates, Pharmacology, Multimodal Imaging, Antibodies, Mice, chemistry.chemical_compound, Antigen, Cell Line, Tumor, Animals, Humans, Radiology, Nuclear Medicine and imaging, Dose-Response Relationship, Drug, biology, Chemistry, Indium Radioisotopes, Membrane Proteins, Prostatic Neoplasms, Biological Transport, Neoplasm Proteins, Monomethyl auristatin E, Isotope Labeling, Positron-Emission Tomography, Pharmacodynamics, Toxicity, biology.protein, Antibody, Tomography, X-Ray Computed, Conjugate

Abstract

TENB2, also known as tomoregulin or transmembrane protein with epidermal growth factor–like and 2 follistatin-like domains, is a transmembrane proteoglycan overexpressed in human prostate tumors. This protein is a promising target for antimitotic monomethyl auristatin E (MMAE)–based antibody–drug conjugate (ADC) therapy. Nonlinear pharmacokinetics in normal mice suggested that antigen expression in normal tissues may contribute to targeted mediated disposition. We evaluated a predosing strategy with unconjugated antibody to block ADC uptake in target-expressing tissues in a mouse model while striving to preserve tumor uptake and efficacy. Methods: Unconjugated, unlabeled antibody was preadministered to mice bearing the TENB2-expressing human prostate explant model, LuCaP 77, followed by a single administration of 111In-labeled anti-TENB2-MMAE for biodistribution and SPECT/CT studies. A tumor-growth-inhibition study was conducted to determine the pharmacodynamic consequences of predosing. Results: Preadministration of anti-TENB2 at 1 mg/kg significantly increased blood exposure of the radiolabeled ADC and reduced intestinal, hepatic, and splenic uptake while not affecting tumor accretion. Similar tumor-to-heart ratios were measured by SPECT/CT at 24 h with and without the predose. Consistent with this, the preadministration of 0.75 mg/kg did not interfere with efficacy in a tumor-growth study dosed at 0.75 mg or 2.5 mg of ADC per kilogram. Conclusion: Overall, the potential to mask peripheral, nontumor antigen uptake while preserving tumor uptake and efficacy could ameliorate toxicity and may significantly affect future dosing strategies for ADCs.

Published

2012

23. Mechanism-Based Pharmacokinetic/Pharmacodynamic Model for THIOMAB™ Drug Conjugates

Author

Luna Liu, Crystal Zhang, Kedan Lin, Shang-Fan Yu, Sunil Bhakta, Helga Raab, Jagath Reddy Junutula, Elaine Mai, Siddharth Sukumaran, Saroja Ramanujan, Katherine R. Kozak, Keyang Xu, Aimee Fourie-O'Donohue, and Kapil Gadkar

Subjects

Drug, Male, Metabolic Clearance Rate, media_common.quotation_subject, Pharmaceutical Science, Biological Availability, Mice, Nude, Antineoplastic Agents, Breast Neoplasms, Mice, SCID, Pharmacology, Models, Biological, Pharmacokinetics, Antigen, Trastuzumab, Antigens, Neoplasm, parasitic diseases, medicine, Animals, Pharmacology (medical), Tumor growth, Cysteine, Sulfhydryl Compounds, media_common, biology, Pharmacokinetic pharmacodynamic, Chemistry, fungi, Organic Chemistry, Antibodies, Monoclonal, biology.protein, Molecular Medicine, Administration, Intravenous, Female, Antibody, Neoplasm Transplantation, Biotechnology, medicine.drug, Conjugate

Abstract

THIOMAB™ drug conjugates (TDCs) with engineered cysteine residues allow site-specific drug conjugation and defined Drug-to-Antibody Ratios (DAR). In order to help elucidate the impact of drug-loading, conjugation site, and subsequent deconjugation on pharmacokinetics and efficacy, we have developed an integrated mathematical model to mechanistically characterize pharmacokinetic behavior and preclinical efficacy of MMAE conjugated TDCs with different DARs. General applicability of the model structure was evaluated with two different TDCs. Pharmacokinetics studies were conducted for unconjugated antibody and purified TDCs with DAR-1, 2 and 4 for trastuzumab TDC and Anti-STEAP1 TDC in mice. Total antibody concentrations and individual DAR fractions were measured. Efficacy studies were performed in tumor-bearing mice. An integrated model consisting of distinct DAR species (DAR0-4), each described by a two-compartment model was able to capture the experimental data well. Time series measurements of each Individual DAR species allowed for the incorporation of site-specific drug loss through deconjugation and the results suggest a higher deconjugation rate from heavy chain site HC-A114C than the light chain site LC-V205C. Total antibody concentrations showed multi-exponential decline, with a higher clearance associated with higher DAR species. The experimentally observed effects of TDC on tumor growth kinetics were successfully described by linking pharmacokinetic profiles to DAR-dependent killing of tumor cells. Results from the integrated model evaluated with two different TDCs highlight the impact of DAR and site of conjugation on pharmacokinetics and efficacy. The model can be used to guide future drug optimization and in-vivo studies.

Published

2014

24. Impact of drug conjugation on pharmacokinetics and tissue distribution of anti-STEAP1 antibody-drug conjugates in rats

Author

Surinder Kaur, Herman Gill, Ben-Quan Shen, Neelima Koppada, Nicole Valle, Kedan Lin, Aimee Fourie, Katherine R. Kozak, Crystal Zhang, Jay Tibbitts, Ola Saad, Paul J. Fielder, Josefa Chuh, Bonnee Rubinfeld, Eduardo E. Mundo, Leslie A. Khawli, Daniela Bumbaca, Frank-Peter Theil, and C. Andrew Boswell

Subjects

Drug, Male, Models, Molecular, Immunoconjugates, media_common.quotation_subject, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Pharmacology, Rats, Sprague-Dawley, Pharmacokinetics, Antigen, Antigens, Neoplasm, Animals, Humans, Tissue Distribution, Disulfides, media_common, biology, Chemistry, Organic Chemistry, Antibodies, Monoclonal, Tumor antigen, Rats, body regions, biology.protein, Antibody, Oxidoreductases, Linker, Oligopeptides, Biotechnology, Cysteine, Conjugate

Abstract

Antibody-drug conjugates (ADCs) are designed to combine the exquisite specificity of antibodies to target tumor antigens with the cytotoxic potency of chemotherapeutic drugs. In addition to the general chemical stability of the linker, a thorough understanding of the relationship between ADC composition and biological disposition is necessary to ensure that the therapeutic window is not compromised by altered pharmacokinetics (PK), tissue distribution, and/or potential organ toxicity. The six-transmembrane epithelial antigen of prostate 1 (STEAP1) is being pursued as a tumor antigen target. To assess the role of ADC composition in PK, we evaluated plasma and tissue PK profiles in rats, following a single dose, of a humanized anti-STEAP1 IgG1 antibody, a thio-anti-STEAP1 (ThioMab) variant, and two corresponding thioether-linked monomethylauristatin E (MMAE) drug conjugates modified through interchain disulfide cysteine residues (ADC) and engineered cysteines (TDC), respectively. Plasma PK of total antibody measured by enzyme-linked immunosorbent assay (ELISA) revealed ∼45% faster clearance for the ADC relative to the parent antibody, but no apparent difference in clearance between the TDC and unconjugated parent ThioMab. Total antibody clearances of the two unconjugated antibodies were similar, suggesting minimal effects on PK from cysteine mutation. An ELISA specific for MMAE-conjugated antibody indicated that the ADC cleared more rapidly than the TDC, but total antibody ELISA showed comparable clearance for the two drug conjugates. Furthermore, consistent with relative drug load, the ADC had a greater magnitude of drug deconjugation than the TDC in terms of free plasma MMAE levels. Antibody conjugation had a noticeable, albeit minor, impact on tissue distribution with a general trend toward increased hepatic uptake and reduced levels in other highly vascularized organs. Liver uptakes of ADC and TDC at 5 days postinjection were 2-fold and 1.3-fold higher, respectively, relative to the unmodified antibodies. Taken together, these results indicate that the degree of overall structural modification in anti-STEAP1-MMAE conjugates has a corresponding level of impact on both PK and tissue distribution.

Published

2011