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1. Targeting and Efficacy of Novel mAb806-Antibody-Drug Conjugates in Malignant Mesothelioma

Author

Puey-Ling Chia, Sagun Parakh, Ming-Sound Tsao, Nhu-An Pham, Hui K. Gan, Diana Cao, Ingrid J. G. Burvenich, Angela Rigopoulos, Edward B. Reilly, Thomas John, and Andrew M. Scott

Subjects
EGFR, malignant mesothelioma, 806-ADC, 89Zr-ch806, Medicine, Pharmacy and materia medica, RS1-441
Abstract

Epidermal growth factor receptor (EGFR) is highly overexpressed in malignant mesothelioma (MM). MAb806 is a novel anti-EGFR antibody that selectively targets a tumor-selective epitope. MAb806-derived antibody drug conjugates (ADCs), ABT-414, ABBV-221 and ABBV-322, may represent a novel therapeutic strategy in MM. EGFR and mAb806 epitope expressions in mesothelioma cell lines were evaluated using an array of binding assays, and the in vitro cell effects of ABT-414 and ABBV-322 were determined. In vivo therapy studies were conducted in mesothelioma xenograft and patient-derived xenograft (PDX) tumor models. We also performed biodistribution and imaging studies to allow the quantitative targeting of MM by mAb806 using a 89Zr-labeled immunoconjugate—ch806. A high EGFR expression was present in all mesothelioma cell lines evaluated and mAb806 binding present in all cell lines, except NCIH-2452. ABT-414 and ABBV-322 resulted in significant tumor growth inhibition in MM models with high EGFR and mAb806 epitope expressions. In contrast, in an EGFR-expressing PDX model that was negative for the mAb806 epitope, no growth inhibition was observed. We demonstrated the specific targeting of the mAb806 epitope expressing MM tumors using 89Zr-based PET imaging. Our data suggest that targeting EGFR in MM using specific ADCs is a valid therapeutic strategy and supports further investigation of the mAb806 epitope expression as a predictive biomarker.

Published
2020
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2. Figure S1 from Characterization of ABBV-221, a Tumor-Selective EGFR-Targeting Antibody Drug Conjugate

Author

Edward B. Reilly, Andrew M. Scott, Hui K. Gan, Diana Cao, Sherry L. Ralston, Lise I. Loberg, Sarah R. Mudd, David R. Reuter, Martin J. Voorbach, Kenneth R. Durbin, Fritz G. Buchanan, Sanjay C. Panchal, Jonathan A. Meulbroek, Chung-Ming Hsieh, Lorenzo Benatuil, Peter J. DeVries, Michael J. Mitten, Hugh D. Falls, Kedar S. Vaidya, Erwin R. Boghaert, and Andrew C. Phillips

Abstract

Amino Acid Sequence of AM-1 VH Region

Published
2023

3. Data from Characterization of ABBV-221, a Tumor-Selective EGFR-Targeting Antibody Drug Conjugate

Author

Edward B. Reilly, Andrew M. Scott, Hui K. Gan, Diana Cao, Sherry L. Ralston, Lise I. Loberg, Sarah R. Mudd, David R. Reuter, Martin J. Voorbach, Kenneth R. Durbin, Fritz G. Buchanan, Sanjay C. Panchal, Jonathan A. Meulbroek, Chung-Ming Hsieh, Lorenzo Benatuil, Peter J. DeVries, Michael J. Mitten, Hugh D. Falls, Kedar S. Vaidya, Erwin R. Boghaert, and Andrew C. Phillips

Abstract

Depatuxizumab mafodotin (depatux-m, ABT-414) is a tumor-selective antibody drug conjugate (ADC) comprised of the anti-EGFR antibody ABT-806 and the monomethyl auristatin F (MMAF) warhead. Depatux-m has demonstrated promising clinical activity in glioblastoma multiforme (GBM) patients and is currently being evaluated in clinical trials in first-line and recurrent GBM disease settings. Depatux-m responses have been restricted to patients with amplified EGFR, highlighting the need for therapies with activity against tumors with nonamplified EGFR overexpression. In addition, depatux-m dosing has been limited by corneal side effects common to MMAF conjugates. We hypothesized that a monomethyl auristatin E (MMAE) ADC utilizing an EGFR-targeting antibody with increased affinity may have broader utility against tumors with more modest EGFR overexpression while mitigating the risk of corneal side effects. We describe here preclinical characterization of ABBV-221, an EGFR-targeting ADC comprised of an affinity-matured ABT-806 conjugated to MMAE. ABBV-221 binds to a similar EGFR epitope as depatux-m and retains tumor selectivity with increased binding to EGFR-positive tumor cells and greater in vitro potency. ABBV-221 displays increased tumor uptake and antitumor activity against wild-type EGFR-positive xenografts with a greatly reduced incidence of corneal side effects relative to depatux-m. ABBV-221 has similar activity as depatux-m against an EGFR-amplified GBM patient derived xenograft (PDX) model and is highly effective alone and in combination with standard-of-care temozolomide in an EGFRvIII-positive GBM xenograft model. Based on these results, ABBV-221 has advanced to a phase I clinical trial in patients with advanced solid tumors associated with elevated levels of EGFR. Mol Cancer Ther; 17(4); 795–805. ©2018 AACR.

Published
2023

5. Data from Targeting Multiple EGFR-expressing Tumors with a Highly Potent Tumor-selective Antibody–Drug Conjugate

Author

Edward B. Reilly, Andrew M. Scott, Hui K. Gan, Thomas John, Puey-Ling Chia, Diana Cao, Joann P. Palma, Wenqing Gao, Erwin R. Boghaert, Kedar S. Vaidya, Anatol Oleksijew, Michael J. Mitten, Hugh D. Falls, and Mark G. Anderson

Abstract

ABBV-321 (serclutamab talirine), a next-generation EGFR-targeted antibody–drug conjugate (ADC) incorporates a potent pyrrolobenzodiazepine (PBD) dimer toxin conjugated to the EGFR-targeting ABT-806 affinity-matured AM1 antibody. ABBV-321 follows the development of related EGFR-targeted ADCs including depatuxizumab mafodotin (depatux-m, ABT-414), ABT-806 conjugated to monomethyl auristatin F (MMAF), and ABBV-221 (losatuxizumab vedotin), AM1 antibody conjugated to monomethyl auristatin E (MMAE). The distinct tumor selectivity of ABBV-321 differentiates it from many previous highly active antibody PBD conjugates that lack a therapeutic window. Potency of the PBD dimer, combined with increased binding of AM1 to EGFR-positive tumor cells, opens the possibility to target a wide array of tumors beyond those with high levels of EGFR overexpression or amplification, including those insensitive to auristatin-based ADCs. ABBV-321 exhibits potent antitumor activity in cellular and in vivo studies including xenograft cell line and patient-derived xenograft glioblastoma, colorectal, lung, head and neck, and malignant mesothelioma tumor models that are less sensitive to depatux-m or ABBV-221. Combination studies with ABBV-321 and depatux-m suggest a promising treatment option permitting suboptimal, and potentially better tolerated, doses of both ADCs while providing improved potency. Collectively, these data suggest that ABBV-321 may offer an extended breadth of efficacy relative to other EGFR ADCs while extending utility to multiple EGFR-expressing tumor indications. Despite its highly potent PBD dimer payload, the tumor selectivity of ABBV-321, coupled with its pharmacology, toxicology, and pharmacokinetic profiles, support continuation of ongoing phase I clinical trials in patients with advanced EGFR-expressing malignancies.

Published
2023

6. Supplementary Figure S3 from Molecular Imaging of Death Receptor 5 Occupancy and Saturation Kinetics In Vivo by Humanized Monoclonal Antibody CS-1008

Author

Andrew M. Scott, Reinhard von Roemeling, Kosaku Fujiwara, Robert A. Beckman, Martin W. Brechbiel, John M. Mariadason, Anderly C. Chueh, Sylvia Gong, Diana Cao, Dahna Makris, Graeme J. O'Keefe, Glenn A. Cartwright, Fook T. Lee, and Ingrid J.G. Burvenich

Abstract

Supplementary Figure S3 - PDF file 489K, In vivo saturation of 111In-CHX-A"-DTPA-CS-1008 in WiDr tumors demonstrated by planar gamma camera imaging (A, 0.2 mg/kg; B, 0.5 mg/kg and C, 10 mg/kg). Representative whole body images (left), surface-rendered CT (middle) and fused images (right) are shown. Dorsal 20-minute images were collected

Published
2023

9. Data from Molecular Imaging of Death Receptor 5 Occupancy and Saturation Kinetics In Vivo by Humanized Monoclonal Antibody CS-1008

Author

Andrew M. Scott, Reinhard von Roemeling, Kosaku Fujiwara, Robert A. Beckman, Martin W. Brechbiel, John M. Mariadason, Anderly C. Chueh, Sylvia Gong, Diana Cao, Dahna Makris, Graeme J. O'Keefe, Glenn A. Cartwright, Fook T. Lee, and Ingrid J.G. Burvenich

Abstract

Purpose: CS-1008 (tigatuzumab; phase I/II), an antihuman death receptor 5 (DR5) agonist, induces apoptosis and has cytotoxic activity against human cancer cell lines. This study reports on the preclinical validation of 111In-labeled anti-DR5 humanized antibody CS-1008 as a diagnostic tool to study the DR5 occupancy in patients with cancer and establish dose ranges for receptor saturation kinetics in vivo.Experimental Design: CS-1008 was radiolabeled and characterized for DR5 binding and labeling efficiency on TRAIL-sensitive DR5–positive colorectal cancer cells (COLO 205 and WiDr). Pharmacokinetic and biodistribution studies were conducted in BALB/c nu/nu mice bearing COLO 205, WiDr, or DR5-negative CT26 colon tumors. Planar gamma camera imaging and computerized tomography (CT) images were obtained to study receptor occupancy in vivo.Results: Scatchard analysis showed high and specific binding affinity (Kd, 1.05 ± 0.12 nmol/L) of 111In-labeled CS-1008. 111In-labeled CS-1008 was specifically taken up in mice bearing COLO 205 and WiDr tumors with prolonged tumor retention (26.25 ± 2.85%ID/g vs. 12.20 ± 2.24 at 168 hours post injection; n = 5, SD), and uptake correlated both with DR5 expression on tumor cells and antitumor activity. DR5 saturation was shown in vivo via both biodistribution studies and planar gamma camera imaging/CT imaging of 111In-labeled CS-1008. Saturation of DR5 corresponded to maximal in vivo antitumor efficacy.Conclusions: Imaging of DR5 receptor occupancy in vivo correlates with tumor concentration and in vivo efficacy, and is a novel molecular imaging technique that can be used to determine receptor occupancy and effective dose levels of DR5 agonist antibodies in the clinic. Clin Cancer Res; 19(21); 5984–93. ©2013 AACR.

Published
2023

12. Radiolabelling and preclinical characterization of 89Zr-Df-radiolabelled bispecific anti-PD-L1/TGF-βRII fusion protein bintrafusp alfa

Author

Wanping Geng, Christian Wichmann, Yit Wooi Goh, Angela Rigopoulos, Diana Cao, Linghui Li, Hui K Gan, Yan Lan, Nhi Huynh, Fiona Scott, Andrew M. Scott, Alexander Franklin McDonald, Anup Zutshi, Zhanqi Liu, Sylvia J. Gong, Nancy Guo, Uwe Ackermann, Ingrid Burvenich, and Graeme O'Keefe

Subjects
Biodistribution, biology, Chemistry, medicine.medical_treatment, virus diseases, General Medicine, Immunotherapy, Pharmacology, Fusion protein, Isotype, In vitro, 030218 nuclear medicine & medical imaging, Avelumab, 03 medical and health sciences, 0302 clinical medicine, In vivo, 030220 oncology & carcinogenesis, medicine, biology.protein, Radiology, Nuclear Medicine and imaging, Antibody, medicine.drug
Abstract

Τhis study aimed to optimize the 89Zr-radiolabelling of bintrafusp alfa investigational drug product and controls, and perform the in vitro and in vivo characterization of 89Zr-Df-bintrafusp alfa and 89Zr-Df-control radioconjugates. Bintrafusp alfa (anti-PD-L1 human IgG1 antibody fused to TGF-β receptor II (TGF-βRII), avelumab (anti-PD-L1 human IgG1 control antibody), isotype control (mutated inactive anti-PD-L1 IgG1 control antibody), and trap control (mutated inactive anti-PD-L1 human IgG1 fused to active TGF-βRII) were chelated with p-isothiocyanatobenzyl-desferrioxamine (Df). After radiolabelling with zirconium-89 (89Zr), radioconjugates were assessed for radiochemical purity, immunoreactivity, antigen binding affinity, and serum stability in vitro. In vivo biodistribution and imaging studies were performed with PET/CT to identify and quantitate 89Zr-Df-bintrafusp alfa tumour uptake in a PD-L1/TGF-β-positive murine breast cancer model (EMT-6). Specificity of 89Zr-Df-bintrafusp alfa was assessed via a combined biodistribution and imaging experiment in the presence of competing cold bintrafusp alfa (1 mg/kg). Nanomolar affinities for PD-L1 were achieved with 89Zr-Df-bintrafusp alfa and 89Zr-avelumab. Biodistribution and imaging studies in PD-L1- and TGF-β-positive EMT-6 tumour-bearing BALB/c mice demonstrated the biologic similarity of 89Zr-Df-bintrafusp alfa and 89Zr-avelumab indicating the in vivo distribution pattern of bintrafusp alfa is driven by its PD-L1 binding arm. Competition study with 1 mg of unlabelled bintrafusp alfa or avelumab co-administered with trace dose of 89Zr-labelled bintrafusp alfa demonstrated the impact of dose and specificity of PD-L1 targeting in vivo. Molecular imaging of 89Zr-Df-bintrafusp alfa biodistribution was achievable and allows non-invasive quantitation of tumour uptake of 89Zr-Df-bintrafusp alfa, suitable for use in bioimaging clinical trials in cancer patients.

Published
2021

13. Targeting Multiple EGFR-expressing Tumors with a Highly Potent Tumor-selective Antibody–Drug Conjugate

Author

Anatol Oleksijew, Thomas John, Diana Cao, Mark Anderson, Joann P. Palma, Kedar S. Vaidya, Puey-Ling Chia, Michael J. Mitten, Hugh D. Falls, Hui K Gan, Edward B. Reilly, Andrew M. Scott, Wenqing Gao, and Erwin R. Boghaert

Subjects
0301 basic medicine, Cancer Research, Antibody-drug conjugate, Immunoconjugates, Mice, Nude, Pyrrolobenzodiazepine, Depatuxizumab mafodotin, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Cell Line, Tumor, medicine, Animals, Humans, ErbB Receptors, 030104 developmental biology, Monomethyl auristatin F, Oncology, Monomethyl auristatin E, chemistry, 030220 oncology & carcinogenesis, Cancer research, Female, Erlotinib, medicine.drug, Conjugate
Abstract

ABBV-321 (serclutamab talirine), a next-generation EGFR-targeted antibody–drug conjugate (ADC) incorporates a potent pyrrolobenzodiazepine (PBD) dimer toxin conjugated to the EGFR-targeting ABT-806 affinity-matured AM1 antibody. ABBV-321 follows the development of related EGFR-targeted ADCs including depatuxizumab mafodotin (depatux-m, ABT-414), ABT-806 conjugated to monomethyl auristatin F (MMAF), and ABBV-221 (losatuxizumab vedotin), AM1 antibody conjugated to monomethyl auristatin E (MMAE). The distinct tumor selectivity of ABBV-321 differentiates it from many previous highly active antibody PBD conjugates that lack a therapeutic window. Potency of the PBD dimer, combined with increased binding of AM1 to EGFR-positive tumor cells, opens the possibility to target a wide array of tumors beyond those with high levels of EGFR overexpression or amplification, including those insensitive to auristatin-based ADCs. ABBV-321 exhibits potent antitumor activity in cellular and in vivo studies including xenograft cell line and patient-derived xenograft glioblastoma, colorectal, lung, head and neck, and malignant mesothelioma tumor models that are less sensitive to depatux-m or ABBV-221. Combination studies with ABBV-321 and depatux-m suggest a promising treatment option permitting suboptimal, and potentially better tolerated, doses of both ADCs while providing improved potency. Collectively, these data suggest that ABBV-321 may offer an extended breadth of efficacy relative to other EGFR ADCs while extending utility to multiple EGFR-expressing tumor indications. Despite its highly potent PBD dimer payload, the tumor selectivity of ABBV-321, coupled with its pharmacology, toxicology, and pharmacokinetic profiles, support continuation of ongoing phase I clinical trials in patients with advanced EGFR-expressing malignancies.

Published
2020

14. Tumor volumes as a predictor of response to the anti-EGFR antibody drug conjugate depatuxizumab mafadotin

Author

Malaka Ameratunga, Yuliya Perchyonok, Diana Cao, Andrew Mark Scott, Eddie Lau, Graeme O'Keefe, Angela Rigopoulos, Sze Ting Lee, Andrew B. Lassman, David Maag, Hui K Gan, Sagun Parakh, Aidan Seow, Ingrid Burvenich, and Erica Gomez

Subjects
Oncology, Drug, medicine.medical_specialty, Biodistribution, media_common.quotation_subject, Brain tumor, Depatuxizumab, depatuxizumab mafadotin, GBM, chemistry.chemical_compound, Internal medicine, medicine, AcademicSubjects/MED00300, media_common, biology, Tumor size, business.industry, medicine.disease, chemistry, tumor volume, Basic and Translational Investigations, biology.protein, Surgery, AcademicSubjects/MED00310, Neurology (clinical), Antibody, Growth inhibition, business, Conjugate
Abstract

BackgroundThe adverse impact of increasing brain tumor size on the efficacy of antibody-drug conjugates (ADCs) was investigated preclinically then validated with clinical data.Methods—Preclinical studyThe impact of tumor size on ADC tumor delivery and treatment response was evaluated in an EGFR-amplified patient-derived glioblastoma (GBM) model following treatment with Depatuxizumab mafadotin (Depatux-M). Biodistribution and imaging studies correlated drug distribution with starting treatment volume and anti-tumor activity.Methods—Clinical studyM12-356 was a Phase I study of Depatux-M in patients with GBM. Blinded volumetric analysis of baseline tumor volumes of M12-356 patients was undertaken by two reviewers and results correlated with response and survival.ResultsPreclinically, imaging and biodistribution studies showed specific and significantly higher tumor uptake of zirconium-89 labeled Depatux-M (89Zr-Depatux-M) in mice with smaller tumor volume (~98 mm3) versus those with larger volumes (~365 mm3); concordantly, mice with tumor volumes ≤100 mm3 at treatment commencement had significantly better growth inhibition by Depatux-M (93% vs 27%, P < .001) and significantly longer overall survival (P < .0001) compared to tumors ≥400 mm3. Clinically, patients with tumor volumes ConclusionBoth preclinical and clinical data showed intra-tumoral concentration and efficacy of Depatux-m inversely correlated with tumor size. This finding merit further investigation with pretreatment tumor volume as a predictor for response to ADCs, in both gliomas and other solid tumors.

Published
2021

15. Targeting and Efficacy of Novel mAb806-Antibody-Drug Conjugates in Malignant Mesothelioma

Author

Ming-Sound Tsao, Thomas John, Angela Rigopoulos, Diana Cao, Sagun Parakh, Puey-Ling Chia, Andrew M. Scott, Ingrid Burvenich, Nhu-An Pham, Hui K Gan, and Edward B. Reilly

Subjects
EGFR, Pharmaceutical Science, lcsh:Medicine, lcsh:RS1-441, Epitope, Article, lcsh:Pharmacy and materia medica, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, 89Zr-ch806, Growth factor receptor, In vivo, Drug Discovery, medicine, Epidermal growth factor receptor, Mesothelioma, 030304 developmental biology, 0303 health sciences, biology, Chemistry, lcsh:R, medicine.disease, 806-ADC, 030220 oncology & carcinogenesis, malignant mesothelioma, Cancer research, biology.protein, Molecular Medicine, Erlotinib, Growth inhibition, Antibody, medicine.drug
Abstract

Epidermal growth factor receptor (EGFR) is highly overexpressed in malignant mesothelioma (MM). MAb806 is a novel anti-EGFR antibody that selectively targets a tumor-selective epitope. MAb806-derived antibody drug conjugates (ADCs), ABT-414, ABBV-221 and ABBV-322, may represent a novel therapeutic strategy in MM. EGFR and mAb806 epitope expressions in mesothelioma cell lines were evaluated using an array of binding assays, and the in vitro cell effects of ABT-414 and ABBV-322 were determined. In vivo therapy studies were conducted in mesothelioma xenograft and patient-derived xenograft (PDX) tumor models. We also performed biodistribution and imaging studies to allow the quantitative targeting of MM by mAb806 using a 89Zr-labeled immunoconjugate&mdash, ch806. A high EGFR expression was present in all mesothelioma cell lines evaluated and mAb806 binding present in all cell lines, except NCIH-2452. ABT-414 and ABBV-322 resulted in significant tumor growth inhibition in MM models with high EGFR and mAb806 epitope expressions. In contrast, in an EGFR-expressing PDX model that was negative for the mAb806 epitope, no growth inhibition was observed. We demonstrated the specific targeting of the mAb806 epitope expressing MM tumors using 89Zr-based PET imaging. Our data suggest that targeting EGFR in MM using specific ADCs is a valid therapeutic strategy and supports further investigation of the mAb806 epitope expression as a predictive biomarker.

Published
2020

16. Radiolabelling and preclinical characterization of

Author

Ingrid Julienne Georgette, Burvenich, Yit Wooi, Goh, Nancy, Guo, Hui Kong, Gan, Angela, Rigopoulos, Diana, Cao, Zhanqi, Liu, Uwe, Ackermann, Christian Werner, Wichmann, Alexander Franklin, McDonald, Nhi, Huynh, Graeme Joseph, O'Keefe, Sylvia Jie, Gong, Fiona Elizabeth, Scott, Linghui, Li, Wanping, Geng, Anup, Zutshi, Yan, Lan, and Andrew Mark, Scott

Subjects
Mice, Mice, Inbred BALB C, Cell Line, Tumor, Positron Emission Tomography Computed Tomography, Positron-Emission Tomography, Animals, Humans, Immunologic Factors, Tissue Distribution, Zirconium, B7-H1 Antigen
Abstract

Τhis study aimed to optimize theBintrafusp alfa (anti-PD-L1 human IgG1 antibody fused to TGF-β receptor II (TGF-βRII), avelumab (anti-PD-L1 human IgG1 control antibody), isotype control (mutated inactive anti-PD-L1 IgG1 control antibody), and trap control (mutated inactive anti-PD-L1 human IgG1 fused to active TGF-βRII) were chelated with p-isothiocyanatobenzyl-desferrioxamine (Df). After radiolabelling with zirconium-89 (Nanomolar affinities for PD-L1 were achieved withMolecular imaging of

Published
2020

18. Characterization of ABBV-221, a Tumor-Selective EGFR-Targeting Antibody Drug Conjugate

Author

Chung-Ming Hsieh, Jonathan A. Meulbroek, Michael J. Mitten, Edward B. Reilly, Hui K Gan, David R. Reuter, Lorenzo Benatuil, Kenneth R. Durbin, Kedar S. Vaidya, Diana Cao, Devries Peter J, Erwin R. Boghaert, Sanjay C. Panchal, Andrew M. Scott, Martin J. Voorbach, Andrew C. Phillips, Hugh D. Falls, Fritz G. Buchanan, Sarah R. Mudd, Lise I. Loberg, and Ralston Sherry L

Subjects
0301 basic medicine, Cancer Research, Antibody-drug conjugate, Immunoconjugates, Phases of clinical research, Mice, Nude, Apoptosis, Antibodies, Monoclonal, Humanized, Depatuxizumab mafodotin, Epitope, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Tumor Cells, Cultured, Medicine, Animals, Humans, Cell Proliferation, Mice, Inbred BALB C, Temozolomide, business.industry, Cancer, medicine.disease, Xenograft Model Antitumor Assays, ErbB Receptors, 030104 developmental biology, Monomethyl auristatin F, Oncology, Monomethyl auristatin E, chemistry, 030220 oncology & carcinogenesis, Cancer research, Female, business, Glioblastoma, Oligopeptides, medicine.drug
Abstract

Depatuxizumab mafodotin (depatux-m, ABT-414) is a tumor-selective antibody drug conjugate (ADC) comprised of the anti-EGFR antibody ABT-806 and the monomethyl auristatin F (MMAF) warhead. Depatux-m has demonstrated promising clinical activity in glioblastoma multiforme (GBM) patients and is currently being evaluated in clinical trials in first-line and recurrent GBM disease settings. Depatux-m responses have been restricted to patients with amplified EGFR, highlighting the need for therapies with activity against tumors with nonamplified EGFR overexpression. In addition, depatux-m dosing has been limited by corneal side effects common to MMAF conjugates. We hypothesized that a monomethyl auristatin E (MMAE) ADC utilizing an EGFR-targeting antibody with increased affinity may have broader utility against tumors with more modest EGFR overexpression while mitigating the risk of corneal side effects. We describe here preclinical characterization of ABBV-221, an EGFR-targeting ADC comprised of an affinity-matured ABT-806 conjugated to MMAE. ABBV-221 binds to a similar EGFR epitope as depatux-m and retains tumor selectivity with increased binding to EGFR-positive tumor cells and greater in vitro potency. ABBV-221 displays increased tumor uptake and antitumor activity against wild-type EGFR-positive xenografts with a greatly reduced incidence of corneal side effects relative to depatux-m. ABBV-221 has similar activity as depatux-m against an EGFR-amplified GBM patient derived xenograft (PDX) model and is highly effective alone and in combination with standard-of-care temozolomide in an EGFRvIII-positive GBM xenograft model. Based on these results, ABBV-221 has advanced to a phase I clinical trial in patients with advanced solid tumors associated with elevated levels of EGFR. Mol Cancer Ther; 17(4); 795–805. ©2018 AACR.

Published
2017

19. Radiolabelling and evaluation of a novel sulfoxide as a PET imaging agent for tumor hypoxia

Author

Diana Cao, Uwe Ackermann, Shinn Dee Yeoh, Graeme O'Keefe, Glenn A Cartwright, Henri Tochon-Danguy, Jonathan M. White, Andrew M. Scott, Evelyn Laurens, and Angela Rigopoulos

Subjects
Cancer Research, Mice, chemistry.chemical_compound, Pharmacokinetics, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Radiology, Nuclear Medicine and imaging, Fluoroethyl, Radiochemistry, Tumor hypoxia, medicine.diagnostic_test, business.industry, Cell Hypoxia, Kidney Neoplasms, chemistry, Positron emission tomography, Isotope Labeling, Positron-Emission Tomography, Sulfoxides, Molecular Medicine, Azide, Nuclear medicine, business, Hydrophobic and Hydrophilic Interactions, FMISO, Preclinical imaging
Abstract

[¹⁸F]FMISO is the most widely validated PET radiotracer for imaging hypoxic tissue. However, as a result of the pharmacokinetics of [¹⁸F]FMISO a 2h wait between tracer administration and patient scanning is required for optimal image acquisition. In order to develop hypoxia imaging agents with faster kinetics, we have synthesised and evaluated several F-18 labelled anilino sulfoxides. In this manuscript we report on the synthesis, in vitro and in vivo evaluation of a novel fluoroethyltriazolyl propargyl anilino sulfoxide. The radiolabelling of the novel tracer was achieved via 2-[¹⁸F]fluoroethyl azide click chemistry. Radiochemical yields were 23 ± 4% based on 2-[¹⁸F]fluoroethyl azide and 7 ± 2% based on K[¹⁸F]F. The radiotracer did not undergo metabolism or defluorination in an in vitro assay using S9 liver fractions. Imaging studies using SK-RC-52 tumors in BALB/c nude mice have indicated that the tracer may have a higher pO₂ threshold than [¹⁸F]FMISO for uptake in hypoxic tumors. Although clearance from muscle was faster than [¹⁸F]FMISO, uptake in hypoxic tumors was slower. The average tumor to muscle ratio at 2h post injection in large, hypoxic tumors with a volume greater than 686 mm³ was 1.7, which was similar to the observed ratio of 1.75 for [¹⁸F]FMISO. Although the new tracer showed improved pharmacokinetics when compared with the previously synthesised sulfoxides, further modifications to the chemical structure need to be made in order to offer significant in vivo imaging advantages over [¹⁸F]FMISO.

Published
2014

20. ABT-806 derived antibody drug conjugates (ADCs) inhibit growth of malignant mesothelioma in-vivo

Author

Diana Cao, Andrew M. Scott, Hui K Gan, Andrew C. Phillips, Puey Ling Chia, Edward B. Reilly, and Thomas John

Subjects
Drug, Cancer Research, Poor prognosis, biology, business.industry, media_common.quotation_subject, Malignancy, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Oncology, In vivo, 030220 oncology & carcinogenesis, medicine, biology.protein, Cancer research, Mesothelioma, Antibody, business, 030215 immunology, media_common, Conjugate
Abstract

e14677 Background: Malignant mesothelioma (MM) is an aggressive malignancy of the pleura with limited therapeutic options, and is associated with a poor prognosis. EGFR is known to be highly over-expressed in mesothelioma with reported EGFR overexpression between 44 to 97%. We have investigated an anti-EGFR antibody (ABT-806), which is tumor specific and robustly inhibits EGFR-expressing tumors. We have previously shown that ABT-806 ADCs demonstrate potent anti-tumor activity in 806 immunohistochemistry (IHC) positive MSTO-211H MM cell line xenograft model. We present data in MM using ABT-806 novel ADCs [ABT-414 (ABT-806- monomethyl auristatin F), ABBV-221 (ABT-806- monomethyl auristatin E) and ABBV-321 (ABT-806- pyrrolobenzodiazepine)] in MM patient derived xenografts (PDX). Methods: We evaluated expression of EGFR and mAb 806 IHC in MM cell lines and PDXs. PDXs were implanted into 5 to 10 NOD-Scid mice per group and treated with control ADC, saline, cisplatin or ABT-806 ADCs and followed longitudinally with caliper measurements. Comparative statistics were performed in Graphpad prism. Results: Three PDX models were selected according to their 806 IHC statuses (2 epithelioid 806 IHC positive, 1 biphasic histology 806 IHC negative). In one epithelioid PDX model, ABBV-321 resulted in significantly reduced tumor growth on day 27 post therapy with median tumor volumes of 180 mm3 (ADC control) compared with 78mm3 (ABBV-321; p = 0.0159 two-sided). Moreover, the median survival was also significantly longer in ABBV-321 treated models (p = 0.018). In the other epithelioid PDX model, ABBV-321 also resulted in significant responses (median 428mm3 (ADC control) vs 167mm3 (ABBV-321, p = 0.0201). In the 806 IHC negative PDX model, the differences in tumor volumes between all groups were found to be non-statistically significant (ADC control vs ABT-414, ADC control vs ABBV-221, ADC-control vs ABBV-321 groups) with p = 0.0597 for one-way ANOVA. MSTO211H cell line xenograft model also demonstrated significant anti-tumor response to both ABT-414 and ABBV-221 (p < 0.01). Conclusions: In a disease with limited therapies, ABT-806 targeting ADCs in MM demonstrated significant responses in 806+ PDX and cell lines. These data support clinical expansion of these compounds in 806+ MM patients.

Published
2019

21. Cross-species analysis of Fc engineered anti-Lewis-Y human IgG1 variants in human neonatal receptor transgenic mice reveal importance of S254 and Y436 in binding human neonatal Fc receptor

Author

Fook T. Lee, Andrew M. Scott, Bruno Catimel, Dahna Makris, Ingrid Burvenich, William Farrugia, Graeme O'Keefe, Laura Allan, Dylan King, Martin W. Brechbiel, Violeta Spirkoska, Zhanqi Liu, Diana Cao, and Paul A. Ramsland

Subjects
0301 basic medicine, Genetically modified mouse, Transgene, Immunology, Mice, Transgenic, Receptors, Fc, Protein Engineering, Immunoglobulin G, 03 medical and health sciences, Mice, Neonatal Fc receptor, Lewis Blood Group Antigens, Report, Immunology and Allergy, Animals, Humans, Binding site, Receptor, Mice, Inbred BALB C, biology, Chemistry, Protein Stability, Histocompatibility Antigens Class I, Antibodies, Monoclonal, Molecular biology, Fragment crystallizable region, 030104 developmental biology, biology.protein, Antibody, Half-Life
Abstract

IgG has a long half-life through engagement of its Fc region with the neonatal Fc receptor (FcRn). The FcRn binding site on IgG1 has been shown to contain I253 and H310 in the CH2 domain and H435 in the CH3 domain. Altering the half-life of IgG has been pursued with the aim to prolong or reduce the half-life of therapeutic IgGs. More recent studies have shown that IgGs bind differently to mouse and human FcRn. In this study we characterize a set of hu3S193 IgG1 variants with mutations in the FcRn binding site. A double mutation in the binding site is necessary to abrogate binding to murine FcRn, whereas a single mutation in the FcRn binding site is sufficient to no longer detect binding to human FcRn and create hu3S193 IgG1 variants with a half-life similar to previously studied hu3S193 F(ab')2 (t1/2β, I253A, 12.23 h; H310A, 12.94; H435A, 12.57; F(ab')2, 12.6 h). Alanine substitutions in S254 in the CH2 domain and Y436 in the CH3 domain showed reduced binding in vitro to human FcRn and reduced elimination half-lives in huFcRn transgenic mice (t1/2β, S254A, 37.43 h; Y436A, 39.53 h; wild-type, 83.15 h). These variants had minimal effect on half-life in BALB/c nu/nu mice (t1/2β, S254A, 119.9 h; Y436A, 162.1 h; wild-type, 163.1 h). These results provide insight into the interaction of human Fc by human FcRn, and are important for antibody-based therapeutics with optimal pharmacokinetics for payload strategies used in the clinic.

Published
2016

22. 18F-THK523: a novel in vivo tau imaging ligand for Alzheimer's disease

Author

Christopher C. Rowe, Kazuhiko Yanai, Nobuyuki Okamura, Angela Rigopoulos, Glenn A Cartwright, Yukitsuka Kudo, Victor L. Villemagne, Roberto Cappai, Andrea R Connor, Rachel S. Mulligan, Michelle T. Fodero-Tavoletti, Catriona McLean, Colin L. Masters, Sylvia J. Gong, Shozo Furumoto, Graeme O'Keefe, Kevin J. Barnham, Paul A. Adlard, and Diana Cao

Subjects
Male, Genetically modified mouse, Pathology, medicine.medical_specialty, Amyloid, tau Proteins, Mice, chemistry.chemical_compound, Alzheimer Disease, Fluorodeoxyglucose F18, In vivo, mental disorders, medicine, Animals, Humans, Radionuclide Imaging, Analysis of Variance, Aniline Compounds, Binding Sites, medicine.diagnostic_test, Brain, medicine.disease, Immunohistochemistry, In vitro, chemistry, Positron emission tomography, Quinolines, Autoradiography, Female, Neurology (clinical), Radiopharmaceuticals, Alzheimer's disease, Pittsburgh compound B
Abstract

While considerable effort has focused on developing positron emission tomography β-amyloid imaging radiotracers for the early diagnosis of Alzheimer's disease, no radiotracer is available for the non-invasive quantification of tau. In this study, we detail the characterization of (18)F-THK523 as a novel tau imaging radiotracer. In vitro binding studies demonstrated that (18)F-THK523 binds with higher affinity to a greater number of binding sites on recombinant tau (K18Δ280K) compared with β-amyloid(1-42) fibrils. Autoradiographic and histofluorescence analysis of human hippocampal serial sections with Alzheimer's disease exhibited positive THK523 binding that co-localized with immunoreactive tau pathology, but failed to highlight β-amyloid plaques. Micro-positron emission tomography analysis demonstrated significantly higher retention of (18)F-THK523 (48%; P

Published
2011

23. ACTR-55. TUMOR VOLUME AS A PREDICTOR OF RESPONSE TO ANTI-EGFR ADC ABT-414

Author

Andrew M. Scott, Lee Sze-Ting, David Maag, Malaka Ameratunga, Diana Cao, Angela Rigopoulos, Eddie Lau, Aidan Seow, Erica Gomez, Ho-Jin Lee, Yuliya Perchyonok, and Hui K Gan

Subjects
Abstracts, Cancer Research, Temozolomide, Oncology, Volume (thermodynamics), Tumor size, Chemistry, medicine, Cancer research, Neurology (clinical), medicine.disease, Glioblastoma, medicine.drug
Abstract

BACKGROUND: Adverse biophysical factors (abnormal vessels and increased interstitial pressure) are increased in larger brain tumors, which negatively impacts penetration of antibody drug conjugates (ADC). The tumour-specific anti-EGFR ADC, depatuxizumab mafadotin (depatux-m), demonstrated encouraging activity in a Phase 1 glioblastoma study (M12-356 study, NCT01800695). The impact of tumour size on depatux-m efficacy was investigated. PRECLINICAL STUDY: Forty mice were engrafted with patient derived xenografts from an M12-356 patient. Eight mice were imaged in a zirconium-labelled depatux-m (3mg/kg) biodistribution study at small (70mm3,n=2) or large (350mm3,n=2) tumour volumes; another 4 mice were imaged with a control ADC. In the controls, non-specific uptake due to blood pool activity was 5% ID/g. In the 89Zr-depatux-m treated groups, mice with larger tumours had significantly less uptake compared smaller tumours (11 vs 21 %ID/gram, p 25cm3 vs 17% in < 25cm3, p=0.009) and worse overall survival (0.52 vs 0.81 years, p=0.001). The results were similar in patients treated with depatux-m monotherapy for response (n=60, 0% vs 10%, p=0.287) and survival (n=62, 0.50 vs 0.89 years, p=0.001) CONCLUSIONS: Increased tumour volumes results in significant reduction in ADC penetration. The impact of this as a modifiable factor, within the broader prognostic impact of increased tumour volume, warrants further investigation with prospective and/or randomized data.

Published
2018

24. Abstract 743: ABT-806-derived antibody-drug conjugates (ADCs) inhibit growth of malignant mesothelioma in vivo

Author

Andrew Mark Scott, Diana Cao, Hui K Gan, Puey Ling Chia, Thomas John, Angela Rigopoulos, Ed Reilly, and Andrew C. Phillips

Subjects
Drug, Cancer Research, Oncology, biology, Chemistry, media_common.quotation_subject, biology.protein, Pharmacology, Antibody, Conjugate, media_common
Abstract

Introduction: Malignant mesothelioma (MM) is an aggressive malignancy of the pleura with limited therapeutic options, and is associated with a poor prognosis. EGFR is known to be highly over-expressed in mesothelioma with reported EGFR overexpression between 44 to 97%. We have developed an anti-EGFR antibody (ABT-806), which is tumour specific and robustly inhibits EGFR-expressing tumours. We aimed to establish the validity and feasibility of targeting tumour expressed EGFR in MM using ABT-806 novel ADCs (ABT-414 and ABBV-221). Methods: We evaluated EGFR and mAb 806 immunohistochemistry in 4 MM cell lines (MSTO-211H, NCI-H2052, NCI-H28, NCI-H2452) and performed in-vitro cell proliferation assays (CPA) to evaluate the antineoplastic potential of mAb806-related ADCs. In-vivo therapeutic studies using the biphasic mesothelioma cell line (MSTO-211H) were conducted with treatment groups involving ABT-414, ABBV-221, ADC control, cisplatin chemotherapy. We also performed quantitative biodistribution and imaging of mAb806 ADC uptake (89Zr mAb806 ADC) to allow correlation of mAb806 ADC concentration in tumours. Results: mAb806 elicited strong binding to three of four MM cell lines (MSTO-211H, NCI-H2052 and NCI-H28). CPAs also demonstrated ABT-414 and ABBV- 221 had significant cell growth inhibition demonstrated in the range between 1 to 10ug/ml for MM cell lines. In MSTO-211H xenograft model significant anti-tumour response to both ABT-414 and ABBV-221 (p Conclusion: ABT-806 ADCs show potent anti-tumour activity in MM model, and warrant further exploration as a potential therapy for MM. Citation Format: Puey Ling Chia, Diana Cao, Angela Rigopoulos, Hui Gan, Ed Reilly, Andrew Phillips, Thomas John, Andrew M. Scott. ABT-806-derived antibody-drug conjugates (ADCs) inhibit growth of malignant mesothelioma in vivo [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 743.

Published
2018

25. Integral membrane protease fibroblast activation protein sensitizes fibrosarcoma to chemotherapy and alters cell death mechanisms

Author

Christoph Renner, Sarah K. Baird, Laura Allan, Diana Cao, Angela Rigopoulos, Andrew M. Scott, and Fiona Scott

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Cell signaling, Programmed cell death, Necroptosis, Fibrosarcoma, Clinical Biochemistry, Pharmaceutical Science, Antineoplastic Agents, Apoptosis, Biology, Fibroblast activation protein, alpha, Cell Line, Tumor, Endopeptidases, Autophagy, Humans, neoplasms, Pharmacology, Biochemistry (medical), Serine Endopeptidases, Membrane Proteins, Cell Biology, digestive system diseases, Organelle membrane, Cell biology, Cell culture, Doxorubicin, Gelatinases, HT1080
Abstract

Fibroblast activation protein (FAP), an integral membrane serine protease, is found on fibro- and osteo-sarcoma and on myofibroblasts in epithelial carcinoma, but rarely on other adult tissue. FAP has been demonstrated to be an excellent target for tumor imaging in clinical trials, and antibodies and other FAP-targeting drugs are in development. Here we have shown that FAP overexpression increased the growth of HT1080 fibrosarcoma cells in vitro and in vivo, and found that the expression of FAP affects response to chemotherapy. When treated with doxorubicin, expression of FAP increased susceptibility to the drug. In spite of this, FAP-HT1080 cells had fewer markers of classical apoptosis than HT1080 cells and neither necrosis nor necroptosis were enhanced. However, levels of early mitochondrial and lysosomal membrane permeability markers were increased, and autophagy switched from a protective function in HT1080 cells to part of the cell death mechanism with FAP expression. Therefore, FAP may affect how the tumor responds to chemotherapeutic drugs overall, which should be considered in targeted drug development. The overexpression of FAP also alters cell signaling and responses to the environment in this cell line. This includes cell death mechanisms, changing the response of HT1080 cells to doxorubicin from classical apoptosis to an organelle membrane permeability-dependent form of cell death.

Published
2015

26. Engineering and characterisation of chimeric monoclonal antibody 806 (ch806) for targeted immunotherapy of tumours expressing de2-7 EGFR or amplified EGFR

Author

Terrance Grant Johns, Diana Cao, Con Panousis, Andrew M. Scott, V M Rayzman, A. Kypridis, Deshou Wang, Christoph Renner, Hui K Gan, Lloyd J. Old, Glenn A Cartwright, Fook-Thean Lee, Antony W. Burgess, Zhanqi Liu, Fiona E Smyth, and Martin W. Brechbiel

Subjects
EGFRvIII, Cancer Research, medicine.drug_class, medicine.medical_treatment, EGFR, Recombinant Fusion Proteins, Transplantation, Heterologous, CHO Cells, Monoclonal antibody, Protein Engineering, Epitope, Mice, Antigen, Cricetinae, medicine, Animals, Humans, Tissue Distribution, Epidermal growth factor receptor, Mice, Inbred BALB C, biology, Antibodies, Monoclonal, Immunotherapy, Neoplasms, Experimental, Molecular biology, chimeric antibody, Transplantation, ErbB Receptors, Oncology, Monoclonal, biology.protein, Female, Antibody, Translational Therapeutics, Neoplasm Transplantation
Abstract

We report the generation of a chimeric monoclonal antibody (ch806) with specificity for an epitope on the epidermal growth factor receptor (EGFR) that is different from that targeted by all other anti-EGFR therapies. Ch806 antibody is reactive to both de2-7 and overexpressed wild-type (wt) EGFR but not native EGFR expressed in normal tissues at physiological levels. Ch806 was stably expressed in CHO (DHFR -/-) cells and purified for subsequent characterisation and validated for use in preliminary immunotherapy investigations. Ch806 retained the antigen binding specificity and affinity of the murine parental antibody. Furthermore, ch806 displayed enhanced antibody-dependent cellular cytotoxicity against target cells expressing the 806 antigen in the presence of human effector cells. Ch806 was successfully radiolabelled with both iodine-125 and indium-111 without loss of antigen binding affinity or specificity. The radioimmunoconjugates were stable in the presence of human serum at 37 degrees C for up to 9 days and displayed a terminal half-life (T(1/2beta)) of approximately 78 h in nude mice. Biodistribution studies undertaken in BALB/c nude mice bearing de2-7 EGFR-expressing or amplified EGFR-expressing xenografts revealed that (125)I-labelled ch806 failed to display any significant tumour retention. However, specific and prolonged tumour localisation of (111)In-labelled ch806 was demonstrated with uptake of 31%ID g(-1) and a tumour to blood ratio of 5 : 1 observed at 7 days postinjection. In vivo therapy studies with ch806 demonstrated significant antitumour effects on established de2-7 EGFR xenografts in BALB/c nude mice compared to control, and both murine 806 and the anti-EGFR 528 antibodies. These results support a potential therapeutic role of ch806 in the treatment of suitable EGFR-expressing tumours, and warrants further investigation of the potential of ch806 as a therapeutic agent.

Published
2005

27. Molecular imaging of death receptor 5 occupancy and saturation kinetics in vivo by humanized monoclonal antibody CS-1008

Author

Andrew M. Scott, John M. Mariadason, Robert A. Beckman, Kosaku Fujiwara, Diana Cao, Graeme O'Keefe, Reinhard von Roemeling, Ingrid Burvenich, Fook-Thean Lee, Sylvia J. Gong, Dahna Makris, Glenn A Cartwright, Martin W. Brechbiel, and Anderly C. Chueh

Subjects
Agonist, Cancer Research, Biodistribution, Pathology, medicine.medical_specialty, medicine.drug_class, Humanized antibody, Antibodies, Monoclonal, Humanized, chemistry.chemical_compound, Mice, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Tissue Distribution, Tigatuzumab, Receptor, Radionuclide Imaging, Indium Radioisotopes, Cancer, medicine.disease, Molecular Imaging, Disease Models, Animal, Kinetics, Receptors, TNF-Related Apoptosis-Inducing Ligand, Oncology, chemistry, Isotope Labeling, Monoclonal, Cancer research, Female, Protein Binding
Abstract

Purpose: CS-1008 (tigatuzumab; phase I/II), an antihuman death receptor 5 (DR5) agonist, induces apoptosis and has cytotoxic activity against human cancer cell lines. This study reports on the preclinical validation of 111In-labeled anti-DR5 humanized antibody CS-1008 as a diagnostic tool to study the DR5 occupancy in patients with cancer and establish dose ranges for receptor saturation kinetics in vivo. Experimental Design: CS-1008 was radiolabeled and characterized for DR5 binding and labeling efficiency on TRAIL-sensitive DR5–positive colorectal cancer cells (COLO 205 and WiDr). Pharmacokinetic and biodistribution studies were conducted in BALB/c nu/nu mice bearing COLO 205, WiDr, or DR5-negative CT26 colon tumors. Planar gamma camera imaging and computerized tomography (CT) images were obtained to study receptor occupancy in vivo. Results: Scatchard analysis showed high and specific binding affinity (Kd, 1.05 ± 0.12 nmol/L) of 111In-labeled CS-1008. 111In-labeled CS-1008 was specifically taken up in mice bearing COLO 205 and WiDr tumors with prolonged tumor retention (26.25 ± 2.85%ID/g vs. 12.20 ± 2.24 at 168 hours post injection; n = 5, SD), and uptake correlated both with DR5 expression on tumor cells and antitumor activity. DR5 saturation was shown in vivo via both biodistribution studies and planar gamma camera imaging/CT imaging of 111In-labeled CS-1008. Saturation of DR5 corresponded to maximal in vivo antitumor efficacy. Conclusions: Imaging of DR5 receptor occupancy in vivo correlates with tumor concentration and in vivo efficacy, and is a novel molecular imaging technique that can be used to determine receptor occupancy and effective dose levels of DR5 agonist antibodies in the clinic. Clin Cancer Res; 19(21); 5984–93. ©2013 AACR.

Published
2013

28. Radiolabelling and evaluation of novel haloethylsulfoxides as PET imaging agents for tumor hypoxia

Author

Shinn Dee Yeoh, Andrew M. Scott, Glenn A Cartwright, Jonathan M. White, Angela Rigopoulos, Evelyn Laurens, Diana Cao, Henri Tochon-Danguy, Graeme O'Keefe, and Uwe Ackermann

Subjects
Cancer Research, Stereochemistry, Chemical structure, chemistry.chemical_compound, Mice, In vivo, Cell Line, Tumor, Animals, Humans, Radiology, Nuclear Medicine and imaging, Carcinoma, Renal Cell, Fluoroethyl, Radiochemistry, Tumor hypoxia, Sulfoxide, Cell Hypoxia, Rats, Cell Transformation, Neoplastic, chemistry, Isotope Labeling, Positron-Emission Tomography, Sulfoxides, Click chemistry, Molecular Medicine, Azide, FMISO, Hydrophobic and Hydrophilic Interactions
Abstract

The significance of imaging hypoxia with the PET ligand [(18)F]FMISO has been demonstrated in a variety of cancers. However, the slow kinetics of [(18)F]FMISO require a 2-h delay between tracer administration and patient scanning. Labelled chloroethyl sulfoxides have shown faster kinetics and higher contrast than [(18)F]FMISO in a rat model of ischemic stroke. However, these nitrogen mustard analogues are unsuitable for routine production and use in humans. Here we report on the synthesis and in vitro and in vivo evaluation of two novel sulfoxides which we synthesised from a single precursor molecule via either 2-[(18)F]fluoroethyl azide click chemistry or conventional nucleophilic displacement of a chloride leaving group. The yields of the click chemistry approach were 90±5% of [(18)F]2 based on 2-[(18)F]fluoroethyl azide, and the yields for the S(N) reaction were 15±5% of [(18)F]1 based on K[(18)F]F. Both radiotracers underwent metabolism in an in vitro assay using S9 liver fractions with biological half-lives of 32.39 and 43.32 min, respectively. Imaging studies using an SK-RC-52 tumor model in BALB/c nude mice have revealed that only [(18)F]1 is retained in hypoxic tumors, whereas [(18)F]2 is cleared from those tumors at a rate similar to that of muscle tissue. [(18)F]1 has emerged as a promising new lead structure for further development of sulfoxide-based hypoxia imaging agents. In particular, the mechanism of uptake needs to be elucidated and changes to the chemical structure need to be made in order to reduce metabolism and improve radiotracer kinetics.

Published
2011

29. Comparison of warfarin pharmacogenetic dosing algorithms in a racially diverse large cohort

Author

Jaekyu Shin and Diana Cao

Subjects
Pharmacology, Databases, Factual, business.industry, Racial Groups, Warfarin, Mean absolute error, Anticoagulants, Large cohort, Cohort Studies, Therapeutic index, Pharmacogenetics, Cohort, Genetics, medicine, Molecular Medicine, Humans, Dosing, business, Pharmacogenetic Test, Algorithm, Algorithms, medicine.drug
Abstract

Aims: Multiple warfarin pharmacogenetic dosing algorithms have been reported to date. However, there is only limited information available on the performance of the algorithms that can be used with the results of a US FDA-cleared warfarin pharmacogenetic test. We compared the performance of warfarin pharmacogenetic dosing algorithms in a large racially diverse cohort. Materials & methods: Warfarin pharmacogenetic dosing algorithms were identified using the PubMed database. Patient information from the International Warfarin Pharmacogenetics Consortium database was used to predict therapeutic warfarin doses according to each algorithm. By using bootstrapping analysis, the performance of algorithms was tested by comparing the mean absolute error and mean percentage of patients whose predicted dose fell within 20% of actual dose (percentage within 20%) in the entire cohort, and by race and therapeutic dose range. Results: A total of 13 algorithms and 1940 patients were included in the study. Overall, all the algorithms had similar performances (mean absolute error: 10.3 mg/week and mean percentage within 20%–41.4%). However, algorithms derived from racially mixed populations tended to perform better than those derived from single race populations. Mixed population algorithms had the lowest mean absolute error and the highest percentage within 20% across the racial groups. Most algorithms performed better in the intermediate-dose range (between 21 and 49 mg/week) than in the low (≤21 mg/week) or high-(≥49 mg/week) range. Conclusion: Published warfarin pharmacogenetic algorithms performed similarly, although mixed population algorithms tended to perform better than race-specific algorithms.

Published
2010

30. Abstract 5318: Optimizing pharmacokinetics and targeting properties of recombinant anti-Lewis Y antibody hu3S193 in A431 tumor-bearing mice

Author

Laura Allan, Andrew M. Scott, Glenn A Cartwright, Sylvia J. Gong, Benjamin Gloria, Roger Murphy, Zhanqi Liu, Dahna Makris, Angela Rigopoulos, Ingrid Burvenich, Fook-Thean Lee, Graeme O'Keefe, Angelo Perani, Diana Cao, and Paul A. Ramsland

Subjects
Cancer Research, Biodistribution, biology, business.industry, medicine.drug_class, Monoclonal antibody, Immunoglobulin light chain, Fragment crystallizable region, Molecular biology, law.invention, Oncology, Antigen, Biochemistry, Pharmacokinetics, law, Recombinant DNA, biology.protein, Medicine, Antibody, business
Abstract

Aim: The humanized monoclonal antibody 3S193 (hu3S193) specifically binds the Lewis Y (Ley) antigen and has shown a long half-life in Phase I first-in-man trials. Previous results have shown that mutations in residues I253, H310 and H435 of the Fc region interfere with the neonatal receptor (FcRn) binding. We have generated a hu3S193 antibody with an alanine mutation in residue I253 (I253A) that shows a shorter half-life than parental hu3S193. The objective of this pilot study was to evaluate the radiolabeling properties of 89Zr-labelled hu3S193_I253A compared to its parent hu3S193 and evaluate them as small-animal positron emission tomography (PET) imaging agents. Methods: Site-directed mutagenesis was performed using a QuickChange XL II site-directed mutagenesis kit (Stratagene) to generate the hu3S193_I253A. The LONZA Glutamine Synthetase expression system was used for eukaryotic expression of antibody heavy and kappa light chain vectors. Mutants were produced in transient (Freestyle 293, Invitrogen) cells and tested for Ley binding using ELISA, FACS and BIAcore analysis. Parental hu3S193 and hu3S193_I253A were radiolabelled with 89Zr after conjugation to deferroxamine-p-SCN (Df). The 89Zr-Df-labelled antibodies were evaluated in small-animal PET studies at 4, 24, 48, and 72 hours post injection. At 72 hours after injection, animals were sacrificed. Blood samples were taken via cardiac puncture and organs were removed. Blood and organ samples were counted for radioactivity. Results: Analysis of hu3S193_I253A mutant by ELISA, BIAcore and FACS showed retention of Ley antigen binding ability. PET imaging demonstrated specific tumor uptake of both 89Zr-Df-labeled parental and hu3S193_I253A at 24 hours post injection and this uptake was maintained for 6 days after injection. Lesions as small as 16 mm3 were clearly detected with both agents. Higher uptake in the liver was detected when using 89Zr-Df-labeled hu3S193_I253A. The 72 hour biodistribution data displayed a higher non-specific uptake in the liver with hu3S193_I253A versus parental (i.e. 15 %ID/g versus 6 %ID/g respectively). For comparison, using 111In-CHX-A”-hu3S193_I253A liver uptake was 7 ± 0.3 %ID/g. This observation indicates that improvement to the 89Zr-labelling chemistry could reduce the liver uptake of faster clearing hu3S193 constructs. Conclusion: The pilot study of 89Zr-labelled hu3S193 and hu3S193_I253A demonstrated excellent tumor uptake of both agents, with high-contrast images generated of lesions as small as 16mm3. Improvements in 89Zr radiolabelling chemistry may be required to optimize imaging of fast clearing recombinant antibodies. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 102nd Annual Meeting of the American Association for Cancer Research; 2011 Apr 2-6; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2011;71(8 Suppl):Abstract nr 5318. doi:10.1158/1538-7445.AM2011-5318

Published
2011

31. CONVERGENCE.

Author

DIANA CAO

Subjects
CONVERGENCE (Poem), CAO, Diana
Published
2021

32. OLD DOGS (REMEMBER).

Author

DIANA CAO

Subjects
OLD Dogs (Remember) (Poem), CAO, Diana
Published
2021

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