Your search keyword '"Frank Loganzo"' showing total 82 results

1. Multivalent peptidic linker enables identification of preferred sites of conjugation for a potent thialanstatin antibody drug conjugate.

Author

Sujiet Puthenveetil, Haiyin He, Frank Loganzo, Sylvia Musto, Jesse Teske, Michael Green, Xingzhi Tan, Christine Hosselet, Judy Lucas, L Nathan Tumey, Puja Sapra, Chakrapani Subramanyam, Christopher J O'Donnell, and Edmund I Graziani

Subjects

Medicine, Science

Abstract

Antibody drug conjugates (ADCs) are no longer an unknown entity in the field of cancer therapy with the success of marketed ADCs like ADCETRIS and KADCYLA and numerous others advancing through clinical trials. The pursuit of novel cytotoxic payloads beyond the mictotubule inhibitors and DNA damaging agents has led us to the recent discovery of an mRNA splicing inhibitor, thailanstatin, as a potent ADC payload. In our previous work, we observed that the potency of this payload was uniquely tied to the method of conjugation, with lysine conjugates showing much superior potency as compared to cysteine conjugates. However, the ADC field is rapidly shifting towards site-specific ADCs due to their advantages in manufacturability, characterization and safety. In this work we report the identification of a highly efficacious site-specific thailanstatin ADC. The site of conjugation played a critical role on both the in vitro and in vivo potency of these ADCs. During the course of this study, we developed a novel methodology of loading a single site with multiple payloads using an in situ generated multi-drug carrying peptidic linker that allowed us to rapidly screen for optimal conjugation sites. Using this methodology, we were able to identify a double-cysteine mutant ADC delivering four-loaded thailanstatin that was very efficacious in a gastric cancer xenograft model at 3mg/kg and was also shown to be efficacious against T-DM1 resistant and MDR1 overexpressing tumor cell lines.

Published

2017

2. Data from Caveolae-Mediated Endocytosis as a Novel Mechanism of Resistance to Trastuzumab Emtansine (T-DM1)

Author

Frank Loganzo, Hans-Peter Gerber, Judy Lucas, Edward Rosfjord, Jeremy S. Myers, Russell Dushin, Dahui Zhou, Lindsay King, Laurie Tylaska, Fang Wang, Christine Hosselet, Jonathan Golas, Bingwen Lu, Xingzhi Tan, and Matthew Sung

Abstract

Trastuzumab emtansine (T-DM1) is an antibody–drug conjugate (ADC) that has demonstrated clinical benefit for patients with HER2+ metastatic breast cancer; however, its clinical activity is limited by inherent or acquired drug resistance. The molecular mechanisms that drive clinical resistance to T-DM1, especially in HER2+ tumors, are not well understood. We used HER2+ cell lines to develop models of T-DM1 resistance using a cyclical dosing schema in which cells received T-DM1 in an “on-off” routine until a T-DM1–resistant population was generated. T-DM1–resistant N87 cells (N87-TM) were cross-resistant to a panel of trastuzumab-ADCs (T-ADCs) with non–cleavable-linked auristatins. N87-TM cells do not have a decrease in HER2 protein levels or an increase in drug transporter protein (e.g., MDR1) expression compared with parental N87 cells. Intriguingly, T-ADCs using auristatin payloads attached via an enzymatically cleavable linker overcome T-DM1 resistance in N87-TM cells. Importantly, N87-TM cells implanted into athymic mice formed T-DM1 refractory tumors that remain sensitive to T-ADCs with cleavable-linked auristatin payloads. Comparative proteomic profiling suggested enrichment in proteins that mediate caveolae formation and endocytosis in the N87-TM cells. Indeed, N87-TM cells internalize T-ADCs into intracellular caveolin-1 (CAV1)–positive puncta and alter their trafficking to the lysosome compared with N87 cells. T-DM1 colocalization into intracellular CAV1-positive puncta correlated with reduced response to T-DM1 in a panel of HER2+ cell lines. Together, these data suggest that caveolae-mediated endocytosis of T-DM1 may serve as a novel predictive biomarker for patient response to T-DM1. Mol Cancer Ther; 17(1); 243–53. ©2017 AACR.

Published

2023

3. Table S5 from PF-06804103, A Site-specific Anti-HER2 Antibody–Drug Conjugate for the Treatment of HER2-expressing Breast, Gastric, and Lung Cancers

Author

Puja Sapra, Hans-Peter Gerber, Christopher J. O'Donnell, Frank Loganzo, Edward Rosfjord, Judy Lucas, Lioudmila Tchistiakova, Frank Barletta, Tracey Clark, Martin Finkelstein, Hadi Falahatpisheh, Magali Guffroy, George Hu, Cynthia M. Rohde, Christine Hosselet, Jonathon Golas, Manoj B. Charati, Eric M. Bennett, Jeffrey Casavant, Jack Bikker, L. Nathan Tumey, Sujiet Puthenveetil, Kimberly Marquette, Bitha Narayanan, Dangshe Ma, Matthew Sung, and Edmund I. Graziani

Abstract

Effects of Systemic Administration of Free Payload Compared with Conventional HER2-vc0101 on Indicators of Bone Marrow Toxicity and Bone Marrow Payload Levels in Rats

Published

2023

4. Data from PF-06804103, A Site-specific Anti-HER2 Antibody–Drug Conjugate for the Treatment of HER2-expressing Breast, Gastric, and Lung Cancers

Author

Puja Sapra, Hans-Peter Gerber, Christopher J. O'Donnell, Frank Loganzo, Edward Rosfjord, Judy Lucas, Lioudmila Tchistiakova, Frank Barletta, Tracey Clark, Martin Finkelstein, Hadi Falahatpisheh, Magali Guffroy, George Hu, Cynthia M. Rohde, Christine Hosselet, Jonathon Golas, Manoj B. Charati, Eric M. Bennett, Jeffrey Casavant, Jack Bikker, L. Nathan Tumey, Sujiet Puthenveetil, Kimberly Marquette, Bitha Narayanan, Dangshe Ma, Matthew Sung, and Edmund I. Graziani

Abstract

The approval of ado-trastuzumab emtansine (T-DM1) in HER2+ metastatic breast cancer validated HER2 as a target for HER2-specific antibody–drug conjugates (ADC). Despite its demonstrated clinical efficacy, certain inherent properties within T-DM1 hamper this compound from achieving the full potential of targeting HER2-expressing solid tumors with ADCs. Here, we detail the discovery of PF-06804103, an anti-HER2 ADC designed to have a widened therapeutic window compared with T-DM1. We utilized an empirical conjugation site screening campaign to identify the engineered ĸkK183C and K290C residues as those that maximized in vivo ADC stability, efficacy, and safety for a four drug–antibody ratio (DAR) ADC with this linker–payload combination. PF-06804103 incorporates the following novel design elements: (i) a new auristatin payload with optimized pharmacodynamic properties, (ii) a cleavable linker for optimized payload release and enhanced antitumor efficacy, and (iii) an engineered cysteine site–specific conjugation approach that overcomes the traditional safety liabilities of conventional conjugates and generates a homogenous drug product with a DAR of 4. PF-06804103 shows (i) an enhanced efficacy against low HER2-expressing breast, gastric, and lung tumor models, (ii) overcomes in vitro- and in vivo–acquired T-DM1 resistance, and (iii) an improved safety profile by enhancing ADC stability, pharmacokinetic parameters, and reducing off-target toxicities. Herein, we showcase our platform approach in optimizing ADC design, resulting in the generation of the anti-HER2 ADC, PF-06804103. The design elements of identifying novel sites of conjugation employed in this study serve as a platform for developing optimized ADCs against other tumor-specific targets.

Published

2023

5. Figure S2 from PF-06804103, A Site-specific Anti-HER2 Antibody–Drug Conjugate for the Treatment of HER2-expressing Breast, Gastric, and Lung Cancers

Author

Puja Sapra, Hans-Peter Gerber, Christopher J. O'Donnell, Frank Loganzo, Edward Rosfjord, Judy Lucas, Lioudmila Tchistiakova, Frank Barletta, Tracey Clark, Martin Finkelstein, Hadi Falahatpisheh, Magali Guffroy, George Hu, Cynthia M. Rohde, Christine Hosselet, Jonathon Golas, Manoj B. Charati, Eric M. Bennett, Jeffrey Casavant, Jack Bikker, L. Nathan Tumey, Sujiet Puthenveetil, Kimberly Marquette, Bitha Narayanan, Dangshe Ma, Matthew Sung, and Edmund I. Graziani

Abstract

Immunohistochemical evaluation of HER2 expression in vivo cell line and patient-derived xenograft models.

Published

2023

6. Supplementary Figures S1 to S11 from Tumor Cells Chronically Treated with a Trastuzumab–Maytansinoid Antibody–Drug Conjugate Develop Varied Resistance Mechanisms but Respond to Alternate Treatments

Author

Hans-Peter Gerber, Kim T. Arndt, Christopher J. O'Donnell, Andreas Maderna, Edmund Graziani, Judy Lucas, Mike Cinque, Kenny Sung Kyoo Kim, Kiran Khandke, Manoj B. Charati, William Hu, My-Hanh Lam, Sylvia Musto, Maximillian T. Follettie, Veronica Diesl, Fang Wang, Eugene Melamud, Jeremy S. Myers, Guixian Jin, Matthew Sung, Xingzhi Tan, and Frank Loganzo

Abstract

Supplementary Figures S1 to S11. Supplementary Figure S1: Schematic illustration of the approach used to create trastuzumab-maytansinoid ADC resistant cell lines. Supplementary Figure S2: Structures of payloads and ADCs. Supplementary Figure S3: 361-TM-resistant cells show differential responses to ADCs with modified linkers, payloads, and antibodies. Supplementary Figure S4: Ectoptic expression of Her2 in JIMT1-TM cells rescues sensitivity to TM-ADC. Supplementary Figure S5: Cell surface proteomic profiling of 361-TM resistant cells, with evidence of increased ABCC1. Supplementary Figure S6: Knockdown of ABCC1 (MRP1) in 361-TM cells sensitizes to ADCs. Supplementary Figure S7: Endosomal and lysosomal proteins altered in JIMT1-TM resistant cells as determined by proteomic profiling. Supplementary Figure S8: Immunoblot verification of elevated surface-associated proteins in JIMT1-TM resistant cells. Supplementary Figure S9: Co-localization analyses of ADC and lysosome via live-cell imaging. Supplementary Figure S10: Altered trafficking in JIMT1-TM cells are specific to TM-ADC and not transferrin receptor antibody. Supplementary Figure S11: LC-MRM analyses of released products from ADCs incubated with parental and resistant cell lines.

Published

2023

7. Supplementary Methods, Table S1 S2, and Figure Legends from Tumor Cells Chronically Treated with a Trastuzumab–Maytansinoid Antibody–Drug Conjugate Develop Varied Resistance Mechanisms but Respond to Alternate Treatments

Author

Hans-Peter Gerber, Kim T. Arndt, Christopher J. O'Donnell, Andreas Maderna, Edmund Graziani, Judy Lucas, Mike Cinque, Kenny Sung Kyoo Kim, Kiran Khandke, Manoj B. Charati, William Hu, My-Hanh Lam, Sylvia Musto, Maximillian T. Follettie, Veronica Diesl, Fang Wang, Eugene Melamud, Jeremy S. Myers, Guixian Jin, Matthew Sung, Xingzhi Tan, and Frank Loganzo

Abstract

Supplementary Methods, Table S1 S2, and Figure Legends. Supplementary Table S1: Properties of cell lines made resistant to TM-conjugate. Supplementary Table S2: Relative resistance of selected free payloads and Cys-capped-released species in H69 (no ABCC1) and H69AR (high ABCC1 expressing) cell lines.

Published

2023

8. Supplementary Information from PF-06804103, A Site-specific Anti-HER2 Antibody–Drug Conjugate for the Treatment of HER2-expressing Breast, Gastric, and Lung Cancers

Author

Puja Sapra, Hans-Peter Gerber, Christopher J. O'Donnell, Frank Loganzo, Edward Rosfjord, Judy Lucas, Lioudmila Tchistiakova, Frank Barletta, Tracey Clark, Martin Finkelstein, Hadi Falahatpisheh, Magali Guffroy, George Hu, Cynthia M. Rohde, Christine Hosselet, Jonathon Golas, Manoj B. Charati, Eric M. Bennett, Jeffrey Casavant, Jack Bikker, L. Nathan Tumey, Sujiet Puthenveetil, Kimberly Marquette, Bitha Narayanan, Dangshe Ma, Matthew Sung, and Edmund I. Graziani

Abstract

Includes Supplementary Materials and Methods, Data and Figure Legends

Published

2023

9. Supplementary Methods, Figures S1-S10, and Table S1 from Caveolae-Mediated Endocytosis as a Novel Mechanism of Resistance to Trastuzumab Emtansine (T-DM1)

Author

Frank Loganzo, Hans-Peter Gerber, Judy Lucas, Edward Rosfjord, Jeremy S. Myers, Russell Dushin, Dahui Zhou, Lindsay King, Laurie Tylaska, Fang Wang, Christine Hosselet, Jonathan Golas, Bingwen Lu, Xingzhi Tan, and Matthew Sung

Abstract

Supplementary Figure S1: N87 and N87-TM cells are similarly sensitive to unconjugated DM1-SMe; Supplementary Figure S2: Trastuzumab binding to N87 and N87-TM cells; Supplementary Figure S3: Generation and characterization of T-DM1-resistant HCC1954-TM and BT474-TM cells; Supplementary Figure S4: Relative resistance profiles of N87-TM to N87 cells to T-ADCs, unconjugated payloads and standard-of-care chemotherapeutics; Supplementary Figure S5: Distribution of T-ADCs in N87-TM tumors; Supplementary Figure S6: N87-TM cells are cross-resistant to a T-ADC conjugated to a cleavable linker with a cysteine-capped auristatin analog; Supplementary Figure S7: N87-TM cells internalize T-ADC into non-low pH intracellular compartments; Supplementary Figure S8: CAV1-GFP expression causes intracellular caveolae formation capable of internalizing T-ADCs in N87 cells; Supplementary Figure S9: CAV1 knockdown is not sufficient to re-sensitize N87-TM cells to T-DM1; Supplementary Figure S10: Non-cleavable and cleavable T-ADCs co-localize with CAV1 similarly in N87 and N87-TM cells; Supplementary Table S1. Cytotoxicity values of Trastuzumab and isotype-control ADCs in HT29 cells, a HER2-negative cell line

Published

2023

10. Supplementary Data from Development of Highly Optimized Antibody–Drug Conjugates against CD33 and CD123 for Acute Myeloid Leukemia

Author

Puja Sapra, Christopher J. O'Donnell, Frank Loganzo, Lioudmila Tchistiakova, Hans-Peter Gerber, Edward Rosfjord, Andreas Giannakou, Xingzhi Tan, L. Nathan Tumey, Tracey Clark, Manoj B. Charati, Nadira Prashad, Russell Dushin, Andreas Maderna, Madan Katragadda, Mauricio Leal, Fan Jiang, Stephane Thibault, Wenyue Hu, Nicole Piché-Nicholas, Jennifer Kahler, and Yoon-Chi Han

Abstract

Supplementary tables & figures

Published

2023

11. Supplementary Materials from Paclitaxel-resistant cells have a mutation in the paclitaxel-binding region of β-tubulin (Asp26Glu) and less stable microtubules

Author

Lee M. Greenberger, James P. Snyder, James H. Nettles, Daniel B. Morilla, Sylvia Musto, Xingzhi Tan, Tami Annable, Frank Loganzo, and Malathi Hari

Abstract

Supplementary Methods, Table S1, and Figure S1

Published

2023

12. Data from Development of Highly Optimized Antibody–Drug Conjugates against CD33 and CD123 for Acute Myeloid Leukemia

Author

Puja Sapra, Christopher J. O'Donnell, Frank Loganzo, Lioudmila Tchistiakova, Hans-Peter Gerber, Edward Rosfjord, Andreas Giannakou, Xingzhi Tan, L. Nathan Tumey, Tracey Clark, Manoj B. Charati, Nadira Prashad, Russell Dushin, Andreas Maderna, Madan Katragadda, Mauricio Leal, Fan Jiang, Stephane Thibault, Wenyue Hu, Nicole Piché-Nicholas, Jennifer Kahler, and Yoon-Chi Han

Abstract

Purpose:Mortality due to acute myeloid leukemia (AML) remains high, and the management of relapsed or refractory AML continues to be therapeutically challenging. The reapproval of Mylotarg, an anti-CD33–calicheamicin antibody–drug conjugate (ADC), has provided a proof of concept for an ADC-based therapeutic for AML. Several other ADCs have since entered clinical development of AML, but have met with limited success. We sought to develop a next-generation ADC for AML with a wide therapeutic index (TI) that overcomes the shortcomings of previous generations of ADCs.Experimental Design:We compared the TI of our novel CD33-targeted ADC platform with other currently available CD33-targeted ADCs in preclinical models of AML. Next, using this next-generation ADC platform, we performed a head-to-head comparison of two attractive AML antigens, CD33 and CD123.Results:Our novel ADC platform offered improved safety and TI when compared with certain currently available ADC platforms in preclinical models of AML. Differentiation between the CD33- and CD123-targeted ADCs was observed in safety studies conducted in cynomolgus monkeys. The CD33-targeted ADC produced severe hematologic toxicity, whereas minimal hematologic toxicity was observed with the CD123-targeted ADC at the same doses and exposures. The improved toxicity profile of an ADC targeting CD123 over CD33 was consistent with the more restricted expression of CD123 in normal tissues.Conclusions:We optimized all components of ADC design (i.e., leukemia antigen, antibody, and linker-payload) to develop an ADC that has the potential to translate into an effective new therapy against AML.

Published

2023

13. Data from Paclitaxel-resistant cells have a mutation in the paclitaxel-binding region of β-tubulin (Asp26Glu) and less stable microtubules

Author

Lee M. Greenberger, James P. Snyder, James H. Nettles, Daniel B. Morilla, Sylvia Musto, Xingzhi Tan, Tami Annable, Frank Loganzo, and Malathi Hari

Abstract

Resistance to paclitaxel-based therapy is frequently encountered in the clinic. The mechanisms of intrinsic or acquired paclitaxel resistance are not well understood. We sought to characterize the resistance mechanisms that develop upon chronic exposure of a cancer cell line to paclitaxel in the presence of the P-glycoprotein reversal agent, CL-347099. The epidermoid tumor line KB-3-1 was exposed to increasing concentrations of paclitaxel and 5 μmol/L CL-347099 for up to 1 year. Cells grown in 15 nmol/L paclitaxel plus CL-347099 (KB-15-PTX/099) developed 18-fold resistance to paclitaxel and were dependent upon paclitaxel for maximal growth. They grew well and retained resistance to paclitaxel when grown in athymic mice. Cross-resistance (3- to 5-fold) was observed in tissue culture to docetaxel, the novel taxane MAC-321, and epothilone B. Collateral sensitivity (∼3-fold) was observed to the depolymerizing agents vinblastine, dolastatin-10, and HTI-286. KB-15-PTX/099–resistant cells did not overexpress P-glycoprotein nor did they have an alteration of [14C]paclitaxel accumulation compared with parental cells. However, a novel point mutation (T to A) resulting in Asp26 to glutamate substitution in class I (M40) β-tubulin was found. Based on an electron crystallography structure of Zn-stabilized tubulin sheets, the phenyl ring of C-3′ NHCO-C6H5 of paclitaxel makes contact with Asp26 of β-tubulin, suggesting a ligand-induced mutation. Optimized model complexes of paclitaxel, docetaxel, and MAC-321 in β-tubulin show a novel hydrogen bonding pattern for the glutamate mutant and rationalize the observed resistance profiles. However, a mutation in the paclitaxel binding pocket does not explain the phenotype completely. KB-15-PTX/099 cells have impaired microtubule stability as determined by a reduced percentage of tubulin in microtubules and reflected by less acetylated tubulin. These results suggest that a mutation in tubulin might affect microtubule stability as well as drug binding and contribute to the observed resistance profile. [Mol Cancer Ther 2006;5(2):270–8]

Published

2023

14. Volumetric imaging of optically cleared and fluorescently labeled animal tissue (VIOLA) for quantifying the 3D biodistribution of nanoparticles at cellular resolution in tumor tissue

Author

Nikolai Rakhilin, Bing Yang, Mary E. Spilker, Lisa K. Manzuk, Mary Katherine Montgomery, Eyoung Shin, Nadira Prashad, Jungyeon Hwang, Youngho Song, Frank Loganzo, Anand Giddabasappa, and Sripad Ram

Subjects

Pharmaceutical Science

Abstract

Nanoparticle (NP) technology holds significant promise to mediate targeted drug delivery to specific organs in the body. Understanding the 3D biodistribution of NPs in heterogeneous environments such as the tumor tissue can provide crucial information on efficacy, safety and potential clinical outcomes. Here we present a novel end-to-end workflow, VIOLA, which makes use of tissue clearing methodology in conjunction with high resolution imaging and advanced 3D image processing to quantify the spatiotemporal 3D biodistribution of fluorescently labeled ACCURIN® NPs. Specifically, we investigate the spatiotemporal biodistribution of NPs in three different murine tumor models (CT26, EMT6, and KPC-GEM) of increasing complexity and translational relevance. We have developed new endpoints to characterize NP biodistribution at multiple length scales. Our observations reveal that the macroscale NP biodistribution is spatially heterogeneous and exhibits a gradient with relatively high accumulation at the tumor periphery that progressively decreases towards the tumor core in all the tumor models. Microscale analysis revealed that NP extravasation from blood vessels increases in a time dependent manner and plateaus at 72 h post injection. Volumetric analysis and pharmacokinetic modeling of NP biodistribution in the vicinity of the blood vessels revealed that the local NP density exhibits a distance dependent spatiotemporal biodistribution which provide insights into the dynamics of NP extravasation in the tumor tissue. Our data represents a comprehensive analysis of NP biodistribution at multiple length scales in different tumor models providing unique insights into their spatiotemporal dynamics. Specifically, our results show that NPs exhibit a dynamic equilibrium with macroscale heterogeneity combined with microscale homogeneity.

Published

2022

15. Anti-Extra Domain B Splice Variant of Fibronectin Antibody-Drug Conjugate Eliminates Tumors with Enhanced Efficacy When Combined with Checkpoint Blockade

Author

Andrea T. Hooper, Kimberly Marquette, Chao-Pei Betty Chang, Jonathon Golas, Sadhana Jain, My-Hanh Lam, Magali Guffroy, Mauricio Leal, Hadi Falahatpisheh, Divya Mathur, Ting Chen, Kerry Kelleher, Kiran Khandke, Elwira Muszynska, Frank Loganzo, Edward Rosfjord, Judy Lucas, Zhengyan Kan, Chakrapani Subramanyam, Christopher O'Donnell, Dario Neri, Hans-Peter Gerber, Chad May, and Puja Sapra

Subjects

Mice, Cancer Research, Immunoconjugates, Neovascularization, Pathologic, Oncology, Cell Line, Tumor, Tumor Microenvironment, Animals, Humans, Breast Neoplasms, Female, Xenograft Model Antitumor Assays, Fibronectins

Abstract

Extra domain B splice variant of fibronectin (EDB+FN) is an extracellular matrix protein (ECM) deposited by tumor-associated fibroblasts, and is associated with tumor growth, angiogenesis, and invasion. We hypothesized that EDB+FN is a safe and abundant target for therapeutic intervention with an antibody-drug conjugate (ADC). We describe the generation, pharmacology, mechanism of action, and safety profile of an ADC specific for EDB+FN (EDB-ADC). EDB+FN is broadly expressed in the stroma of pancreatic, non-small cell lung (NSCLC), breast, ovarian, head and neck cancers, whereas restricted in normal tissues. In patient -derived xenograft (PDX), cell-line xenograft (CLX), and mouse syngeneic tumor models, EDB-ADC, conjugated to auristatin Aur0101 through site-specific technology, demonstrated potent antitumor growth inhibition. Increased phospho-histone H3, a pharmacodynamic biomarker of response, was observed intumor cells distal to the target site of tumor ECM after EDB-ADC treatment. EDB-ADC potentiated infiltration of immune cells, including CD3+ T lymphocytes into the tumor, providing rationale for the combination of EDB-ADC with immune check-point therapy. EDB-ADC and anti-PD-L1 combination in a syngeneic breast tumor model led to enhanced antitumor activity with sustained tumor regressions. In nonclinical safety studies in nonhuman primates, EDB-ADC had a well-tolerated safety profile without signs of either on-target toxicity or the off -target effects typically observed with ADCs that are conjugated through conventional conjugation methods. These data highlight the potential for EDB-ADC to specifically target the tumor microenvironment, provide robust therapeutic benefits against multiple tumor types, and enhance activity antitumor in com-bination with checkpoint blockade., Molecular Cancer Therapeutics, 21 (9), ISSN:1535-7163, ISSN:1538-8514

Published

2022

16. Development of Highly Optimized Antibody-Drug Conjugates against CD33 and CD123 for Acute Myeloid Leukemia

Author

Hans-Peter Gerber, L. Nathan Tumey, Fan Jiang, Stephane Thibault, Russell Dushin, Mauricio Leal, Frank Loganzo, Puja Sapra, Jennifer Kahler, Andreas Giannakou, Xingzhi Tan, Wenyue Hu, Manoj Charati, Nadira Anarkali Prashad, Yoon-Chi Han, Madan Katragadda, Andreas Maderna, Nicole Piche-Nicholas, Tracey Clark, Lioudmila Tchistiakova, Christopher J. O’Donnell, and Edward Rosfjord

Subjects

0301 basic medicine, Oncology, Drug, Cancer Research, medicine.medical_specialty, Immunoconjugates, Cell Survival, media_common.quotation_subject, CD33, Sialic Acid Binding Ig-like Lectin 3, Interleukin-3 Receptor alpha Subunit, HL-60 Cells, 03 medical and health sciences, Mice, 0302 clinical medicine, Therapeutic index, Antineoplastic Agents, Immunological, Antigen, hemic and lymphatic diseases, Internal medicine, Cell Line, Tumor, Hardware_INTEGRATEDCIRCUITS, medicine, Animals, Humans, Hardware_ARITHMETICANDLOGICSTRUCTURES, media_common, biology, business.industry, Myeloid leukemia, medicine.disease, Gemtuzumab, Xenograft Model Antitumor Assays, Tumor Burden, body regions, Leukemia, Disease Models, Animal, Leukemia, Myeloid, Acute, Macaca fascicularis, 030104 developmental biology, 030220 oncology & carcinogenesis, Area Under Curve, biology.protein, Interleukin-3 receptor, Antibody, business

Abstract

Purpose: Mortality due to acute myeloid leukemia (AML) remains high, and the management of relapsed or refractory AML continues to be therapeutically challenging. The reapproval of Mylotarg, an anti-CD33–calicheamicin antibody–drug conjugate (ADC), has provided a proof of concept for an ADC-based therapeutic for AML. Several other ADCs have since entered clinical development of AML, but have met with limited success. We sought to develop a next-generation ADC for AML with a wide therapeutic index (TI) that overcomes the shortcomings of previous generations of ADCs. Experimental Design: We compared the TI of our novel CD33-targeted ADC platform with other currently available CD33-targeted ADCs in preclinical models of AML. Next, using this next-generation ADC platform, we performed a head-to-head comparison of two attractive AML antigens, CD33 and CD123. Results: Our novel ADC platform offered improved safety and TI when compared with certain currently available ADC platforms in preclinical models of AML. Differentiation between the CD33- and CD123-targeted ADCs was observed in safety studies conducted in cynomolgus monkeys. The CD33-targeted ADC produced severe hematologic toxicity, whereas minimal hematologic toxicity was observed with the CD123-targeted ADC at the same doses and exposures. The improved toxicity profile of an ADC targeting CD123 over CD33 was consistent with the more restricted expression of CD123 in normal tissues. Conclusions: We optimized all components of ADC design (i.e., leukemia antigen, antibody, and linker-payload) to develop an ADC that has the potential to translate into an effective new therapy against AML.

Published

2020

17. Modulation of SF3B1 in the pre-mRNA spliceosome induces a RIG-I-dependent type I IFN response

Author

Frank Loganzo, Aaron Y. Chang, Kesha M. Shah, Yu Jerry Zhou, Seng-Ryong Woo, Heather Wheeler, Paula M. Loria, Piotr W. Pobiarzyn, Pavel Tishchenko, Yue-Ming Wang, and Sharanya Iyengar

Subjects

RNA splicing, THP-1 Cells, IFN-I, type I interferon, Biochemistry, Mice, hpRNA, hairpin RNA, RNA Precursors, cytokine, MDA5, melanoma differentiation–associated protein 5, anticancer drug, Receptors, Immunologic, innate immunity, HDR, homology-directed repair, Chemistry, RIG-I, interferon, Cell biology, RIG-I-like receptor, interferon regulatory factor, Stimulator of interferon genes, Interferon Type I, MAVS, mitochondrial antiviral signaling protein, DEAD Box Protein 58, RNA Splicing Factors, Research Article, Spliceosome, Plad B, pladienolide B, mRNA, sgRNA, single-guide RNA, Mutation, Missense, TNFα, tumor necrosis factor alpha, STING, stimulator of interferon genes, Proinflammatory cytokine, alternative splicing, cDNA, complementary DNA, HEK, human embryonic kidney, SF3B1, spliceosome splicing factor 3b subunit 1, Animals, Humans, Molecular Biology, IRF3, interferon regulatory factor 3, Cell Biology, Phosphoproteins, IL, interleukin, RIG-I, retinoic acid–inducible gene I, LU, light unit, NGS, next-generation sequencing, Amino Acid Substitution, A549 Cells, ISG54, interferon-stimulated gene 54, Spliceosomes, SEAP, secreted embryonic alkaline phosphatase, spliceosome, IRF3, Interferon regulatory factors

Abstract

Nucleic acid–sensing pathways play critical roles in innate immune activation through the production of type I interferon (IFN-I) and proinflammatory cytokines. These factors are required for effective antitumor immune responses. Pharmacological modulators of the pre-mRNA spliceosome splicing factor 3b subunit 1 (SF3B1) are under clinical investigation as cancer cytotoxic agents. However, potential roles of these agents in aberrant RNA generation and subsequent RNA-sensing pathway activation have not been studied. In this study, we observed that SF3B1 pharmacological modulation using pladienolide B (Plad B) induces production of aberrant RNA species and robust IFN-I responses via engagement of the dsRNA sensor retinoic acid–inducible gene I (RIG-I) and downstream interferon regulatory factor 3. We found that Plad B synergized with canonical RIG-I agonism to induce the IFN-I response. In addition, Plad B induced NF-κB responses and secretion of proinflammatory cytokines and chemokines. Finally, we showed that cancer cells bearing the hotspot SF3B1K700E mutation, which leads to global aberrant splicing, had enhanced IFN-I response to canonical RIG-I agonism. Together, these results demonstrate that pharmacological modulation of SF3B1 in cancer cells can induce an enhanced IFN-I response dependent on RIG-I expression. The study suggests that spliceosome modulation may not only induce direct cancer cell cytotoxicity but also initiate an innate immune response via activation of RNA-sensing pathways.

Published

2021

18. PF-06804103, A Site-specific Anti-HER2 Antibody-Drug Conjugate for the Treatment of HER2-expressing Breast, Gastric, and Lung Cancers

Author

Kimberly Ann Marquette, Frank Loganzo, Puja Sapra, Dangshe Ma, George Hu, Sujiet Puthenveetil, Cynthia M. Rohde, Judy Lucas, L. Nathan Tumey, Matthew Sung, Christine Hosselet, Jonathon Golas, Manoj Charati, Edmund I. Graziani, Frank Barletta, Magali Guffroy, Martin Finkelstein, Jeffrey M. Casavant, Hadi Falahatpisheh, Bitha Narayanan, Jack A. Bikker, Hans-Peter Gerber, Eric M. Bennett, Lioudmila Tchistiakova, Tracey Clark, Edward Rosfjord, and Christopher J. O’Donnell

Subjects

0301 basic medicine, Drug, Cancer Research, Immunoconjugates, Lung Neoplasms, media_common.quotation_subject, Mice, Nude, Breast Neoplasms, 03 medical and health sciences, Mice, 0302 clinical medicine, Pharmacokinetics, In vivo, Stomach Neoplasms, medicine, Animals, Humans, Clinical efficacy, skin and connective tissue diseases, media_common, Chemistry, medicine.disease, Metastatic breast cancer, body regions, A-site, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Anti-HER2 Antibody, Cancer research, Female, Conjugate

Abstract

The approval of ado-trastuzumab emtansine (T-DM1) in HER2+ metastatic breast cancer validated HER2 as a target for HER2-specific antibody–drug conjugates (ADC). Despite its demonstrated clinical efficacy, certain inherent properties within T-DM1 hamper this compound from achieving the full potential of targeting HER2-expressing solid tumors with ADCs. Here, we detail the discovery of PF-06804103, an anti-HER2 ADC designed to have a widened therapeutic window compared with T-DM1. We utilized an empirical conjugation site screening campaign to identify the engineered ĸkK183C and K290C residues as those that maximized in vivo ADC stability, efficacy, and safety for a four drug–antibody ratio (DAR) ADC with this linker–payload combination. PF-06804103 incorporates the following novel design elements: (i) a new auristatin payload with optimized pharmacodynamic properties, (ii) a cleavable linker for optimized payload release and enhanced antitumor efficacy, and (iii) an engineered cysteine site–specific conjugation approach that overcomes the traditional safety liabilities of conventional conjugates and generates a homogenous drug product with a DAR of 4. PF-06804103 shows (i) an enhanced efficacy against low HER2-expressing breast, gastric, and lung tumor models, (ii) overcomes in vitro- and in vivo–acquired T-DM1 resistance, and (iii) an improved safety profile by enhancing ADC stability, pharmacokinetic parameters, and reducing off-target toxicities. Herein, we showcase our platform approach in optimizing ADC design, resulting in the generation of the anti-HER2 ADC, PF-06804103. The design elements of identifying novel sites of conjugation employed in this study serve as a platform for developing optimized ADCs against other tumor-specific targets.

Published

2020

19. Mechanisms of Resistance to Antibody–Drug Conjugates

Author

Frank Loganzo, Matthew Sung, and Hans-Peter Gerber

Subjects

0301 basic medicine, Drug, Cancer Research, Immunoconjugates, media_common.quotation_subject, Drug Evaluation, Preclinical, Antineoplastic Agents, Drug resistance, Pharmacology, 03 medical and health sciences, 0302 clinical medicine, Antigen, Antigens, Neoplasm, Neoplasms, medicine, Animals, Humans, Cytotoxic T cell, Molecular Targeted Therapy, Cytotoxicity, media_common, biology, Cytotoxins, Antibodies, Monoclonal, Cancer, medicine.disease, body regions, 030104 developmental biology, Gene Expression Regulation, Oncology, Drug Resistance, Neoplasm, Drug Design, 030220 oncology & carcinogenesis, Cancer cell, biology.protein, Antibody, Signal Transduction

Abstract

Drug resistance limits the effectiveness of cancer therapies. Despite attempts to develop curative anticancer treatments, tumors evolve evasive mechanisms limiting durable responses. Hence, diverse therapies are used to attack cancer, including cytotoxic and targeted agents. Antibody–drug conjugates (ADC) are biotherapeutics designed to deliver potent cytotoxins to cancer cells via tumor-specific antigens. Little is known about the clinical manifestations of drug resistance to this class of therapy; however, recent preclinical studies reveal potential mechanisms of resistance. Because ADCs are a combination of antibody and small molecule cytotoxin, multifactorial modes of resistance are emerging that are inherent to the structure and function of the ADC. Decreased cell-surface antigen reduces antibody binding, whereas elevated drug transporters such as MDR1 and MRP1 reduce effectiveness of the payload. Inherent to the uniqueness of the ADC, other novel resistance mechanisms are emerging, including altered antibody trafficking, ADC processing, and intracellular drug release. Most importantly, the modular nature of the ADC allows components to be switched and replaced, enabling development of second-generation ADCs that overcome acquired resistance. This review is intended to highlight recent progress in our understanding of ADC resistance, including approaches to create preclinical ADC-refractory models and to characterize their emerging mechanisms of resistance. Mol Cancer Ther; 15(12); 2825–34. ©2016 AACR.

Published

2016

20. Optimization of Tubulysin Antibody–Drug Conjugates: A Case Study in Addressing ADC Metabolism

Author

Judy Lucas, Guoyun Bai, Christopher J. O’Donnell, Sai Chetan K. Sukuru, Brian Rago, Sarah P. Hudson, Carolyn A. Leverett, Lioudmila Tchistiakova, Edmund I. Graziani, Anokha S. Ratnayake, Sylvia Musto, Jeffrey M. Casavant, Joseph Stock, Frank Loganzo, Christine Hosselet, Sujiet Puthenveetil, Andrew J. Bessire, Fengping Li, Xiaogang Han, Tracey Clark, Venkata Doppalapudi, Kimberly Ann Marquette, Beth C. Vetelino, Chakrapani Subramanyam, and L. Nathan Tumey

Subjects

0301 basic medicine, Drug, Heavy chain, biology, Chemistry, media_common.quotation_subject, Organic Chemistry, Metabolism, Biochemistry, body regions, 03 medical and health sciences, 030104 developmental biology, Drug Discovery, biology.protein, Antibody, media_common, Conjugate

Abstract

As part of our efforts to develop new classes of tubulin inhibitor payloads for antibody-drug conjugate (ADC) programs, we developed a tubulysin ADC that demonstrated excellent in vitro activity but suffered from rapid metabolism of a critical acetate ester. A two-pronged strategy was employed to address this metabolism. First, the hydrolytically labile ester was replaced by a carbamate functional group resulting in a more stable ADC that retained potency in cellular assays. Second, site-specific conjugation was employed in order to design ADCs with reduced metabolic liabilities. Using the later approach, we were able to identify a conjugate at the 334C position of the heavy chain that resulted in an ADC with considerably reduced metabolism and improved efficacy. The examples discussed herein provide one of the clearest demonstrations to-date that site of conjugation can play a critical role in addressing metabolic and PK liabilities of an ADC. Moreover, a clear correlation was identified between the hydrophobicity of an ADC and its susceptibility to metabolic enzymes. Importantly, this study demonstrates that traditional medicinal chemistry strategies can be effectively applied to ADC programs.

Published

2016

21. Natural Product Splicing Inhibitors: A New Class of Antibody–Drug Conjugate (ADC) Payloads

Author

Frank Loganzo, Frank Barletta, Jesse Alexander Teske, Dangshe Ma, Sylvia Musto, Chakrapani Subramanyam, Hans-Peter Gerber, L. Nathan Tumey, Ken Dirico, Christopher J. O’Donnell, Judy Lucas, Edmund I. Graziani, Puja Sapra, Michael V. Green, Brian Rago, Hadi Falahaptisheh, Haiyin He, Tracey Clark, Frank E. Koehn, Xiaogang Han, Robert Veneziale, and Sujiet Puthenveetil

Subjects

0301 basic medicine, Spliceosome, Antibody-drug conjugate, Immunoconjugates, DNA damage, Carboxylic Acids, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Maleimides, Mice, 03 medical and health sciences, chemistry.chemical_compound, Cell Line, Tumor, Animals, Humans, Cytotoxic T cell, Tissue Distribution, ATP Binding Cassette Transporter, Subfamily B, Member 1, Cysteine, Pyrans, Pharmacology, Biological Products, Natural product, biology, Chemistry, Lysine, Organic Chemistry, Combinatorial chemistry, Cell biology, Cell Transformation, Neoplastic, 030104 developmental biology, RNA splicing, biology.protein, Antibody, Biotechnology, Conjugate

Abstract

There is a considerable ongoing work to identify new cytotoxic payloads that are appropriate for antibody-based delivery, acting via mechanisms beyond DNA damage and microtubule disruption, highlighting their importance to the field of cancer therapeutics. New modes of action will allow a more diverse set of tumor types to be targeted and will allow for possible mechanisms to evade the drug resistance that will invariably develop to existing payloads. Spliceosome inhibitors are known to be potent antiproliferative agents capable of targeting both actively dividing and quiescent cells. A series of thailanstatin-antibody conjugates were prepared in order to evaluate their potential utility in the treatment of cancer. After exploring a variety of linkers, we found that the most potent antibody-drug conjugates (ADCs) were derived from direct conjugation of the carboxylic acid-containing payload to surface lysines of the antibody (a "linker-less" conjugate). Activity of these lysine conjugates was correlated to drug-loading, a feature not typically observed for other payload classes. The thailanstatin-conjugates were potent in high target expressing cells, including multidrug-resistant lines, and inactive in nontarget expressing cells. Moreover, these ADCs were shown to promote altered splicing products in N87 cells in vitro, consistent with their putative mechanism of action. In addition, the exposure of the ADCs was sufficient to result in excellent potency in a gastric cancer xenograft model at doses as low as 1.5 mg/kg that was superior to the clinically approved ADC T-DM1. The results presented herein therefore open the door to further exploring splicing inhibition as a potential new mode-of-action for novel ADCs.

Published

2016

22. Natural Product Bis-Intercalator Depsipeptides as a New Class of Payloads for Antibody-Drug Conjugates

Author

Edmund I. Graziani, Judy Lucas, L. Nathan Tumey, Frank Loganzo, Li-Ping Chang, Vlad Buklan, T. Eric Ballard, Fengping Li, Brian Rago, Christopher J. O’Donnell, Frank E. Koehn, Christine Hosselet, Jeffrey E. Janso, Anokha S. Ratnayake, Joseph A. Chemler, Xidong Feng, WeiDong Ding, Melissa Wagenaar, Sylvia Musto, and Greg L. Steele

Subjects

Immunoconjugates, Biomedical Engineering, Pharmaceutical Science, Bioengineering, 02 engineering and technology, Echinomycin, Conjugated system, 01 natural sciences, chemistry.chemical_compound, Mice, Antineoplastic Agents, Immunological, In vivo, Cell Line, Tumor, Depsipeptides, Animals, Humans, Pharmacology, Depsipeptide, Biological Products, Natural product, 010405 organic chemistry, Organic Chemistry, DNA, Genes, erbB-2, Trastuzumab, 021001 nanoscience & nanotechnology, Combinatorial chemistry, In vitro, Intercalating Agents, 0104 chemical sciences, chemistry, Heterografts, 0210 nano-technology, Linker, Biotechnology, Conjugate, Half-Life

Abstract

A potent class of DNA-damaging agents, natural product bis-intercalator depsipeptides (NPBIDs), was evaluated as ultrapotent payloads for use in antibody-drug conjugates (ADCs). Detailed investigation of potency (both in cells and via biophysical characterization of DNA binding), chemical tractability, and in vitro and in vivo stability of the compounds in this class eliminated a number of potential candidates, greatly reducing the complexity and resources required for conjugate preparation and evaluation. This effort yielded a potent, stable, and efficacious ADC, PF-06888667, consisting of the bis-intercalator, SW-163D, conjugated via an N-acetyl-lysine-valine-citrulline- p-aminobenzyl alcohol- N, N-dimethylethylenediamine (AcLysValCit-PABC-DMAE) linker to an engineered variant of the anti-Her2 mAb, trastuzumab, catalyzed by transglutaminase.

Published

2018

23. Novel PIKK inhibitor antibody-drug conjugates: Synthesis and anti-tumor activity

Author

Frank Loganzo, Dahui Zhou, Sylvia Musto, Russell Dushin, Edmund I. Graziani, Nathan Tumey, Jeffrey M. Casavant, Christopher J. O’Donnell, Haiyin He, and Jeffrey E. Janso

Subjects

Immunoconjugates, Clinical Biochemistry, Mutant, Pharmaceutical Science, Antineoplastic Agents, Conjugated system, 01 natural sciences, Biochemistry, Proof of Concept Study, chemistry.chemical_compound, Amide, Cell Line, Tumor, Drug Discovery, Humans, Pyrroles, Molecular Biology, Phosphoinositide-3 Kinase Inhibitors, biology, 010405 organic chemistry, Organic Chemistry, Acetal, Trastuzumab, Combinatorial chemistry, In vitro, 0104 chemical sciences, body regions, 010404 medicinal & biomolecular chemistry, chemistry, Mutation, biology.protein, Aminoquinolines, Molecular Medicine, Antibody, Drug Screening Assays, Antitumor, Cysteine, Conjugate

Abstract

Novel neolymphostin-based antibody-drug conjugate (ADC) precursors were synthesized either through amide couplings between both cleavable and non-cleavable linkers and neolymphostin derivatives, or through Cu(I)-catalyzed acetylene-azide click cycloadditon between non-cleavable linkers and neolymphostin acetal derivatives. These precursors were site-specifically conjugated to cysteine mutant trastuzumab-A114C to provide neolymphostin-based ADCs. Preliminary in vitro data indicated that the corresponding ADCs were active against HER2-expressing tumor cell lines, thus providing a proof-of-concept for using neolymphostin as ADC-based anticancer agents.

Published

2018

24. Caveolae-Mediated Endocytosis as a Novel Mechanism of Resistance to Trastuzumab Emtansine (T-DM1)

Author

Xingzhi Tan, Judy Lucas, Fang Wang, Bingwen Lu, Matthew Sung, Christine Hosselet, Dahui Zhou, Jeremy S. Myers, Russell Dushin, Lindsay King, Laurie Tylaska, Hans-Peter Gerber, Jonathan Golas, Edward Rosfjord, and Frank Loganzo

Subjects

musculoskeletal diseases, 0301 basic medicine, Male, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Population, Biology, Endocytosis, Caveolae, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Antineoplastic Agents, Immunological, Lysosome, medicine, Animals, Humans, education, education.field_of_study, Colocalization, Trastuzumab, Molecular biology, 030104 developmental biology, medicine.anatomical_structure, Oncology, chemistry, Trastuzumab emtansine, Cell culture, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, Female, Intracellular

Abstract

Trastuzumab emtansine (T-DM1) is an antibody–drug conjugate (ADC) that has demonstrated clinical benefit for patients with HER2+ metastatic breast cancer; however, its clinical activity is limited by inherent or acquired drug resistance. The molecular mechanisms that drive clinical resistance to T-DM1, especially in HER2+ tumors, are not well understood. We used HER2+ cell lines to develop models of T-DM1 resistance using a cyclical dosing schema in which cells received T-DM1 in an “on-off” routine until a T-DM1–resistant population was generated. T-DM1–resistant N87 cells (N87-TM) were cross-resistant to a panel of trastuzumab-ADCs (T-ADCs) with non–cleavable-linked auristatins. N87-TM cells do not have a decrease in HER2 protein levels or an increase in drug transporter protein (e.g., MDR1) expression compared with parental N87 cells. Intriguingly, T-ADCs using auristatin payloads attached via an enzymatically cleavable linker overcome T-DM1 resistance in N87-TM cells. Importantly, N87-TM cells implanted into athymic mice formed T-DM1 refractory tumors that remain sensitive to T-ADCs with cleavable-linked auristatin payloads. Comparative proteomic profiling suggested enrichment in proteins that mediate caveolae formation and endocytosis in the N87-TM cells. Indeed, N87-TM cells internalize T-ADCs into intracellular caveolin-1 (CAV1)–positive puncta and alter their trafficking to the lysosome compared with N87 cells. T-DM1 colocalization into intracellular CAV1-positive puncta correlated with reduced response to T-DM1 in a panel of HER2+ cell lines. Together, these data suggest that caveolae-mediated endocytosis of T-DM1 may serve as a novel predictive biomarker for patient response to T-DM1. Mol Cancer Ther; 17(1); 243–53. ©2017 AACR.

Published

2017

25. Borrelidin B: Isolation, Biological Activity, and Implications for Nitrile Biosynthesis

Author

Christopher J. Schulze, Roger G. Linington, Teresa Szal, Anabella Villalobos, Frank E. Koehn, Walter M. Bray, My-Hanh Lam, and Frank Loganzo

Subjects

Pharmacology, Molecular Structure, Nitrile, Stereochemistry, Metabolite, Organic Chemistry, Pharmaceutical Science, Biological activity, Biology, Analytical Chemistry, Amino Acyl-tRNA Synthetases, chemistry.chemical_compound, Polyketide, Complementary and alternative medicine, chemistry, Biosynthesis, Biochemistry, Nitriles, Drug Discovery, Transfer RNA, Threonine-tRNA Ligase, Molecular Medicine, Moiety, Fatty Alcohols, Mitosis

Abstract

Borrelidin (1) is a nitrile-containing bacterially derived polyketide that is a potent inhibitor of bacterial and eukaryotic threonyl-tRNA synthetases. We now report the discovery of borrelidin B (2), a tetrahydro-borrelidin derivative containing an aminomethyl group in place of the nitrile functionality in borrelidin. The discovery of this new metabolite has implications for both the biosynthesis of the nitrile group and the bioactivity of the borrelidin compound class. Screening in the SToPS assay for tRNA synthetase inhibition revealed that the nitrile moiety is essential for activity, while profiling using our in-house image-based cytological profiling assay demonstrated that 2 retains biological activity by causing a mitotic stall, even in the absence of the nitrile motif.

Published

2014

26. New cytotoxic benzosuberene analogs. Synthesis, molecular modeling and biological evaluation

Author

My-Hanh Lam, Christopher J. O’Donnell, Andreas Maderna, Sylvia Musto, Sai Chetan K. Sukuru, Zecheng Chen, Frank Loganzo, and Melissa Wagenaar

Subjects

Diene, Molecular model, Cell Survival, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Cell Line, chemistry.chemical_compound, Dogs, Tubulin, Drug Discovery, Benzene Derivatives, Animals, Humans, Cytotoxic T cell, Benzosuberene, Derivatization, Molecular Biology, Cell Proliferation, Biological evaluation, Binding Sites, Chemistry, Organic Chemistry, Combinatorial chemistry, Tubulin Modulators, Chemical space, Protein Structure, Tertiary, Molecular Docking Simulation, Microsomes, Liver, Molecular Medicine, Colchicine, Protein Binding, Cell based

Abstract

In this Letter we describe the synthesis and biological evaluation of new benzosuberene analogs with structural modifications on the B-ring. The focus was initially to probe the chemical space around the B-ring C-8 position. This position was readily available for derivatization chemistry using our recently developed new synthesis for this compound class. Furthermore, we describe two new B-ring analogs, one containing a diene and the other a cyclic ether group. Both new analogs show excellent potencies in tumor cell proliferation assays. In addition, we describe molecular modeling studies that provide a binding rationale for reference compound 8 in the colchicine binding site using the known colchicine crystal structure. We also examine whether the cell based potency data obtained with selected new analogs are supported by modeling results.

Published

2013

27. Site Selection: a Case Study in the Identification of Optimal Cysteine Engineered Antibody Drug Conjugates

Author

Frank Loganzo, Jack A. Bikker, Nicole Piche-Nicholas, Christopher J. O’Donnell, Tracey Clark, Lioudmila Tchistiakova, Kimberly Ann Marquette, Jeffrey M. Casavant, Sylvia Musto, Fengping Li, Amy Tam, Xiaogang Han, L. Nathan Tumey, Edmund I. Graziani, Sujiet Puthenveetil, Eric M. Bennett, Brian Rago, Hans-Peter Gerber, and Frank Barletta

Subjects

0301 basic medicine, Drug, Antibody-drug conjugate, Immunoconjugates, media_common.quotation_subject, Pharmaceutical Science, Molecular Dynamics Simulation, Cleavage (embryo), 01 natural sciences, 03 medical and health sciences, chemistry.chemical_compound, Succinimide, Amino Acid Sequence, Cysteine, media_common, biology, 010405 organic chemistry, 0104 chemical sciences, body regions, 030104 developmental biology, Biochemistry, chemistry, biology.protein, Antibody, Linker, Conjugate

Abstract

As the antibody drug conjugate (ADC) community continues to shift towards site-specific conjugation technology, there is a growing need to understand how the site of conjugation impacts the biophysical and biological properties of an ADC. In order to address this need, we prepared a carefully selected series of engineered cysteine ADCs and proceeded to systematically evaluate their potency, stability, and PK exposure. The site of conjugation did not have a significant influence on the thermal stability and in vitro cytotoxicity of the ADCs. However, we demonstrate that the rate of cathepsin-mediated linker cleavage is heavily dependent upon site and is closely correlated with ADC hydrophobicity, thus confirming other recent reports of this phenomenon. Interestingly, conjugates with high rates of cathepsin-mediated linker cleavage did not exhibit decreased plasma stability. In fact, the major source of plasma instability was shown to be retro-Michael mediated deconjugation. This process is known to be impeded by succinimide hydrolysis, and thus, we undertook a series of mutational experiments demonstrating that basic residues located nearby the site of conjugation can be a significant driver of succinimide ring opening. Finally, we show that total antibody PK exposure in rat was loosely correlated with ADC hydrophobicity. It is our hope that these observations will help the ADC community to build “design rules” that will enable more efficient prosecution of next-generation ADC discovery programs.

Published

2017

28. Establishing in vitro-in vivo correlation for antibody drug conjugate efficacy: a PK/PD modeling approach

Author

Nahor Haddish-Berhane, Sylvia Musto, Frank Barletta, Judy Lucas, Tracey Clark, Frank Loganzo, Steven Hansel, Dhaval K. Shah, Alison Betts, and Hallie S. Wald

Subjects

Antibody-drug conjugate, Immunoconjugates, Mice, Nude, Antineoplastic Agents, Pharmacology, 030226 pharmacology & pharmacy, Models, Biological, Antibodies, Correlation, 03 medical and health sciences, Mice, 0302 clinical medicine, IVIVC, In vivo, Neoplasms, Animals, Humans, Cytotoxicity, PK/PD models, Chemistry, Xenograft Model Antitumor Assays, In vitro, body regions, 030220 oncology & carcinogenesis, Female, Conjugate

Abstract

The objective of this manuscript was to establish in vitro–in vivo correlation (IVIVC) between the in vitro efficacy and in vivo efficacy of antibody drug conjugates (ADCs), using a PK/PD modeling approach. Nineteen different ADCs were used to develop IVIVC. In vitro efficacy of ADCs was evaluated using a kinetic cell cytotoxicity assay. The cytotoxicity data obtained from in vitro studies was characterized using a novel mathematical model, parameter estimates from which were used to derive an in vitro efficacy matrix for each ADC, termed as ‘in vitro tumor static concentration’ (TSCin vitro). TSCin vitro is a theoretical concentration at continuous exposure of which the number of cells will neither increase nor decrease, compared to the initial cell number in the experiment. The in vivo efficacy of ADCs was evaluated using tumor growth inhibition (TGI) studies performed on human tumor xenograft bearing mice. The TGI data obtained from in vivo studies was characterized using a PK/PD model, parameter estimates from which were used to derive an in vivo efficacy matrix for each ADC, termed as ‘in vivo tumor static concentration’ (TSCin vivo). TSCin vivo is a theoretical concentration if one were to maintain in the plasma of a tumor bearing mouse, the tumor volume will neither increase nor decrease compared to the initial tumor volume. Comparison of the TSCin vitro and TSCin vivo values from 19 ADCs provided a linear and positive IVIVC. The Spearman’s rank correlation coefficient for TSCin vitro and TSCin vivo was found to be 0.82. On average TSCin vivo was found to be ~ 27 times higher than TSCin vitro. The reasonable IVIVC for ADCs suggests that in vitro efficacy data was correctly able to differentiate ADCs for their in vivo efficacy. Thus, IVIVC can be used as a tool to triage ADC molecules in the discovery stage, thereby preventing unnecessary scaling-up of ADCs and waste of time and resources. An ability to predict the concentration of ADC that is efficacious in vivo using the in vitro data can also help in optimizing the experimental design of preclinical efficacy studies. As such, the novel PK/PD modeling method presented here to establish IVIVC for ADCs holds promise, and should be evaluated further using diverse set of cell lines and anticancer agents.

Published

2017

29. Design, Synthesis, and Cytotoxic Evaluation of Novel Tubulysin Analogues as ADC Payloads

Author

Christopher J. O’Donnell, Carolyn A. Leverett, Dingguo Liu, Beth C. Vetelino, Alison H. Varghese, Sai Chetan K. Sukuru, Sarah P. Hudson, Joseph Stock, Kevin D. Parris, Jayvardhan Pandit, Frank Loganzo, Guoyun Bai, Venkata Doppalapudi, Sylvia Musto, Bin Liu, and Chakrapani Subramanyam

Subjects

0301 basic medicine, Chemistry, medicine.medical_treatment, Organic Chemistry, Biochemistry, Small molecule, Combinatorial chemistry, Targeted therapy, 03 medical and health sciences, 030104 developmental biology, Design synthesis, Drug Discovery, medicine, Cytotoxic T cell, Human cancer

Abstract

The tubulysin class of natural products has attracted much attention from the medicinal chemistry community due to its potent cytotoxicity against a wide range of human cancer cell lines, including significant activity in multidrug-resistant carcinoma models. As a result of their potency, the tubulysins have become an important tool for use in targeted therapy, being widely pursued as payloads in the development of novel small molecule drug conjugates (SMDCs) and antibody–drug conjugates (ADCs). A structure-based and parallel medicinal chemistry approach was applied to the synthesis of novel tubulysin analogues. These efforts led to the discovery of a number of novel and potent cytotoxic tubulysin analogues, providing a framework for our simultaneous report, which highlights the discovery of tubulysin-based ADCs, including use of site-specific conjugation to address in vivo stability of the C-11 acetate functionality.

Published

2016

30. Determination of Antibody-Drug Conjugate Released Payload Species Using Directed in Vitro Assays and Mass Spectrometric Interrogation

Author

Frank Loganzo, Klaas Schildknegt, Sujiet Puthenveetil, Birte Nolting, Andrew J. Bessire, T. Eric Ballard, Lee R. Roberts, My-Hanh Lam, Chakrapani Subramanyam, Michael Eric Green, Betsy Pierce, Manoj Charati, and Justin Cohen

Subjects

0301 basic medicine, Antibody-drug conjugate, Immunoconjugates, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Nanotechnology, Mass Spectrometry, Cathepsin B, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Line, Tumor, Animals, Humans, Pharmacology, chemistry.chemical_classification, Drug Carriers, Organic Chemistry, In vitro toxicology, In vitro, Rats, Drug Liberation, 030104 developmental biology, Enzyme, chemistry, S9 fraction, Biochemistry, Targeted drug delivery, Liver, 030220 oncology & carcinogenesis, Lysosomes, Linker, Biotechnology, Conjugate

Abstract

Antibody-drug conjugates (ADC) are currently an active area of research, focused primarily on oncology therapeutics, but also to a limited extent on other areas such as infectious disease. The success of this type of targeted drug delivery is dependent upon many factors, one of which is the performance of the linker in releasing an active drug moiety under the appropriate conditions. As a tool in the development of linker/payload chemistry, we have developed an in vitro method for the identification of payload species released from ADCs in the presence of lysosomal enzymes. This method utilizes commercially available human liver S9 fraction as the source of these enzymes, and this has certain advantages over lysosomal fractions or purified enzymes. This article describes the characterization and performance of this assay with multiple ADCs composed of known and novel linkers and payloads. Additionally, we report the observation of incomplete degradation of mAb protein chains by lysosomal enzymes in vitro, believed to be the first report of this phenomenon involving an ADC therapeutic.

Published

2016

31. Depsides isolated from the Sri Lankan lichenParmotremasp. exhibit selective Plk1 inhibitory activity

Author

Maya P. Singh, Selvaluxmy Kathirgamanathar, Leonard A. McDonald, Richard Harrison, Frank Loganzo, David E. Williams, Jenny Togias, Veranja Karunaratne, Raymond J. Andersen, and Lauren Whitney

Subjects

Lichens, Molecular Sequence Data, Pharmaceutical Science, Cell Cycle Proteins, Parmotrema, Context (language use), Protein Serine-Threonine Kinases, Depsides, chemistry.chemical_compound, Ascomycota, Proto-Oncogene Proteins, Drug Discovery, Parmeliaceae, Humans, Amino Acid Sequence, Protein Kinase Inhibitors, Sri Lanka, Pharmacology, chemistry.chemical_classification, Natural product, biology, General Medicine, biology.organism_classification, In vitro, Enzyme, Complementary and alternative medicine, chemistry, Biochemistry, Molecular Medicine, Depside

Abstract

Mitotic kinase enzymes regulate critical stages of mitosis and are amenable to pharmacological inhibition. Since natural products have been a rich source of antimitotic inhibitors, we postulated that natural products would also provide effective inhibitors of mitotic kinases.To explore unique marine and terrestrial natural product sources for new anticancer drug leads, we screened our natural product extract library for polo-like kinase-1 (Plk1) kinase inhibitors.Extracts of the lichen Parmotrema sp. (Parmeliaceae) exhibited in vitro inhibitory activity. Bioassay-guided fractionation of the Parmotrema sp. extract led to the isolation of depside inhibitors.A new depside 1 has been isolated from the Sri Lankan lichen Parmotrema sp. along with the known metabolites 2 (β-collatolic acid) and 3 (β-alectoronic acid). The structure of depside 1 was elucidated by spectroscopic analysis. The three depsides 1-3 exhibited moderate inhibition of purified recombinant Plk1 kinase with IC₅₀ of 2.8, 0.7, and 1.7 µM, respectively, at 1 µM ATP. Inhibitory activity was also observed at high concentrations of ATP, suggesting the potential for activity in a cellular environment. The depsides were also tested against a panel of 23 other recombinant kinases and were found to possess up to 30-fold selectivity toward Plk1.These data suggest that the depsides 1-3 may serve as core structures that can be further explored as potential inhibitors of Plk1 and other kinases.

Published

2011

32. Abstract 1978: Antibody-drug conjugates with DNA inhibitor linker-payloads can overcome resistance in cultured tumor cells made resistant to conjugates with cleavable-linked auristatins

Author

Frank Loganzo, Xingzhi Tan, and Matthew Sung

Subjects

Drug, Cancer Research, biology, media_common.quotation_subject, Tumor cells, chemistry.chemical_compound, Oncology, chemistry, Biochemistry, biology.protein, Antibody, Linker, DNA, Conjugate, media_common

Abstract

Antibody drug conjugates (ADCs) are targeted biotherapeutics delivering cytotoxic payloads to tumor-expressed antigens. The most common class of ADC payloads are microtubule inhibitors (MTI) and DNA inhibitors, exemplified by clinically approved ado-trastuzumab emtansine (TDM1; MTI DM1), brentuximab vedotin (MTI auristatin), gemtuzumab ozogamicin and inotuzumab ozogamicin (DNA double strand breaker calicheamicin). Auristatin payloads are in active development, primarily employing proteolytically cleavable linker mcValCitPABC. There are many benefits of cleavable-linked permeable payloads, including bystander activity in a heterogeneous tumor environment. However, due to the complexity of human cancer, tumors become refractory to most drug therapies. We hypothesized that cultured tumor cells chronically treated with mcValCitPABC-auristatin ADCs would acquire varied resistance mechanisms. As model ADCs, we used trastuzumab-mcValCitPABC-mono methyl auristatin E (TvcMMAE) and trastuzumab-mcValCitPABC-Aur0101 (Tvc0101). Her2 expressing gastric carcinoma line, N87, was chronically exposed to the respective ADCs at cytotoxic doses in a cyclical fashion (3 days on; ~1 - 3 weeks off). Resistance was acquired very slowly (over ~1 year), and cells were characterized for their resistance profile. N87-TvcMMAE cells had >1000X relative resistance (RR) to T-auristatin and TDM1 ADCs compared with parental N87, and showed moderate to high resistance (~50 – 300X) to unconjugated MTIs including auristatins and DM1. The cells were cross-resistant (>100 - 1000X) to T-ADCs delivering several payload classes, including NAc-calicheamicin and cyclopropylpyrroloindolone (CPI). Her2 and MDR1 levels were unchanged in N87-TvcMMAE cells, however, a slight increase of MRP1 was observed on immunoblots. Cells made resistant to Tvc0101 ADC showed a different profile. N87-Tvc0101 cells had >1000X RR to T-auristatin ADCs and >400X to TDM1, but were sensitive ( Citation Format: Xingzhi Tan, Matthew Sung, Frank Loganzo. Antibody-drug conjugates with DNA inhibitor linker-payloads can overcome resistance in cultured tumor cells made resistant to conjugates with cleavable-linked auristatins [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 1978.

Published

2018

33. Abstract 818: NG-HER2 ADC (PF-06804103) is superior to trastuzumab emtansine in a mouse 'avatar' head-to-head clinical trial

Author

Matthew Sung, Christine Hopf, Judy Lucas, Ken Geles, Jonathon Golas, Erik Upeslacis, Manoj Charati, Frank Loganzo, Hans-Peter Gerber, Kiran Khandke, Mark Kaplan, Puja Sapra, Frank W. Kotch, and Edward Rosfjord

Subjects

Cancer Research, biology, Head to head, business.industry, Cancer, medicine.disease, Metastatic breast cancer, In vitro, Clinical trial, chemistry.chemical_compound, Oncology, chemistry, Trastuzumab emtansine, Cell culture, Cancer research, medicine, biology.protein, Antibody, business

Abstract

Patient-derived xenografts (PDXs) are resected human tumors engrafted into mice and represent personalized murine ‘avatars' of those tumors. PDXs are valuable tumor models for drug development since they recapitulate the complexity of the human tumor microenvironment more extensively than cell line xenografts (CLXs). Unlike CLXs, PDXs are never passaged in vitro, and therefore they more faithfully recapitulate native tumor biology and response to therapeutics. Thus, PDXs may more accurately predict clinical activity of therapeutic compounds than traditional CLXs. We are developing a next generation (NG)-HER2 antibody-drug conjugate (ADC), PF-06804103, that employs a proprietary site-specific conjugation technology that chemically links the clinically-validated linker-payload “ValCit-Aur0101” to an anti-HER2 antibody. The site-specific conjugation enables enhanced exposures and reduced off-target toxicities as previously described. We utilized our PDX collection to evaluate the breadth-of-efficacy of PF-06804103 versus trastuzumab emtansine (T-DM1), an FDA-approved ADC for metastatic breast cancer patients with high HER2 expression. Efficient cleavage of the ‘ValCit' linker and payload release in the early endosome is not impacted by the rapid recycling properties of the HER2 receptor, unlike T-DM1 which requires catabolism in the within the lysosomal milieu to efficiently release its payload. To date, we have enrolled >20 HER2-expressing breast, gastric and non-small cell lung cancer PDXs, with varying low to high HER2 expression levels, in a head-to-head ‘mouse avatar clinical trial' comparing activity of a single cycle of T-DM1 (6 mg/kg) to PF-06804103 (3 mg/kg). Impressively, PF-06804103 had more durable complete responses and a higher objective response rate (ORR) than T-DM1 (84% vs. 4%), including in low-moderate HER2 expressers. PF-06804103 prolonged median overall survival (OS) of mice with HER2-expressing tumors compared to T-DM1 (100 vs 45 days). Biomarker analysis showed that tumors at all levels of HER2 expression were more likely to receive more benefit with PF-06804103 than T-DM1 (HR < 0.45). By leveraging our novel PDX ‘avatar' clinic, we were able to demonstrate that PF-06804103 displays superior in vivo breadth-of-efficacy compared to T-DM1. Citation Format: Matthew S. Sung, Christine Hopf, Erik Upeslacis, Jonathon Golas, Mark Kaplan, Kiran Khandke, Manoj Charati, Frank Kotch, Frank Loganzo, Ken Geles, Judy Lucas, Hans-Peter Gerber, Puja Sapra, Edward Rosfjord. NG-HER2 ADC (PF-06804103) is superior to trastuzumab emtansine in a mouse 'avatar' head-to-head clinical trial [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 818.

Published

2018

34. Opportunities posed by novel patient selection biomarker approaches in oncology drug development: going beyond the cytotoxics

Author

John Alvarez, Christina Marie Coughlin, Richat Abbas, Michael E. Burczynski, Fred Immermann, Grant Sellar, Frank Loganzo, Maha Karnoub, and Giora Feuerstein

Subjects

Drug, Clinical Oncology, medicine.medical_specialty, business.industry, media_common.quotation_subject, Biochemistry (medical), Clinical Biochemistry, Bioinformatics, Drug development, Drug Discovery, medicine, Biomarker (medicine), Oncology drug, Biomarker discovery, Intensive care medicine, business, media_common

Abstract

An area of unmet medical need in clinical oncology has been optimizing patient selection for a given therapeutic with the goal of getting the right drug to the right patient. Recent studies have developed preclinical approaches to identifying molecular ‘signatures of resistance’ for cytotoxic therapies and prospective validation of this strategy is ongoing in the clinic. New challenges in this setting include identifying approaches to patient selection for cytostatic compounds such as signaling pathway inhibitors and stem cell targets. Here, we discuss the biomarker methodologies developed using traditional cytotoxic drugs and how these approaches can be adapted to identify biomarkers of patient selection for novel signaling inhibitors and other novel targets. It has become increasingly clear that such biomarker discovery and validation needs to begin early and continue throughout the drug development process.

Published

2008

35. Development of Solid-Phase Site-Specific Conjugation and Its Application toward Generation of Dual Labeled Antibody and Fab Drug Conjugates

Author

Sylvia Musto, Frank Loganzo, L. Nathan Tumey, Edmund I. Graziani, Sujiet Puthenveetil, and Christopher J. O’Donnell

Subjects

0301 basic medicine, Drug, Immunoconjugates, media_common.quotation_subject, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Nanotechnology, Antibodies, 03 medical and health sciences, Immunoglobulin Fab Fragments, Purification methods, media_common, Pharmacology, biology, Chemistry, Organic Chemistry, A protein, Combinatorial chemistry, body regions, 030104 developmental biology, biology.protein, Antibody, Linker, Biotechnology, Conjugate

Abstract

The focus of the antibody-drug conjugate (ADC) field is shifting toward development of site-specific, next-generation ADCs to address the issue of heterogeneity, metabolic instability, conjugatability, and less than ideal therapeutic index associated with the conventional (heterogeneous) ADCs. It is evident from the recent literature that the site of conjugation, the structure of the linker, and the physicochemical properties of the linker-payload all have a significant impact on the safety and efficacy of the resulting ADCs. Screening multiple linker-payloads on multiple sites of an antibody presents a combinatorial problem that necessitates high-throughput conjugation and purification methodology to identify ADCs with the best combination of site and payload. Toward this end, we developed a protein A/L-based solid-phase, site-specific conjugation and purification method that can be used to generate site-specific ADCs in a 96-well plate format. This solid-phase method has been shown to be versatile because of its compatibility with various conjugation functional handles such as maleimides, haloacetamides, copper free click substrates, and transglutaminase substrates. The application of this methodology was further expanded to generate dual labeled, site-specific antibody and Fab conjugates.

Published

2016

36. Dual irreversible kinase inhibitors: Quinazoline-based inhibitors incorporating two independent reactive centers with each targeting different cysteine residues in the kinase domains of EGFR and VEGFR-2

Author

Frank Loganzo, Charles Ingalls, Thomas Nittoli, Xingzhi Tan, M. Brawner Floyd, Heidi L. Fraser, Kinwang Cheung, Allan Wissner, Russell Dushin, and Malini Ravi

Subjects

Models, Molecular, Tertiary amine, Protein Conformation, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Inhibitory Concentration 50, chemistry.chemical_compound, Adenosine Triphosphate, Growth factor receptor, Drug Discovery, Quinazoline, Humans, Epidermal growth factor receptor, Protein Kinase Inhibitors, Molecular Biology, Reactive center, Cells, Cultured, chemistry.chemical_classification, Binding Sites, Molecular Structure, biology, Kinase, Chemistry, Organic Chemistry, Vascular Endothelial Growth Factor Receptor-2, ErbB Receptors, Enzyme, Enzyme inhibitor, Quinazolines, biology.protein, Molecular Medicine, Biological Assay

Abstract

A series of 4-dimethylamino-but-2-enoic acid [4-(3,6-dioxo-cyclohexa-1,4-dienylamino)-7-ethoxy-quinazolin-6-yl]-amide derivatives were prepared. These compounds have two independent reactive centers and were designed to function as dual irreversible inhibitors of the kinase domains of both Epidermal Growth Factor Receptor (EGFR) and Vascular Endothelial Growth Factor Receptor-2 (VEGFR-2) where each reactive center targets a different, non-conserved, cysteine residue located in the ATP binding pocket of these enzymes. The compounds contain a 6-(4-(dimethylamino) crotonamide) Michael acceptor group that targets Cys-773 in EGFR and a 4-(amino-[1,4]benzoquinone) moiety that targets Cys-1045 in VEGFR-2. In vitro studies indicated that most of these compounds are relatively potent inhibitors of each enzyme. These inhibitors were compared with reference compounds that lack one or both of the reactive centers. The relative dependence of the IC50 values on the concentration of ATP used in the assays suggests that these compounds appear to function as irreversible inhibitors of each kinase.

Published

2007

37. Combining antibody-drug conjugates and immune-mediated cancer therapy: What to expect?

Author

Puja Sapra, Frank Loganzo, Chad May, and Hans-Peter Gerber

Subjects

0301 basic medicine, Antibody-drug conjugate, Antineoplastic Agents, Pharmacology, Biology, CD8-Positive T-Lymphocytes, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigens, Neoplasm, Neoplasms, medicine, Cytotoxic T cell, Animals, Humans, Immunologic Factors, Cancer, Antibodies, Monoclonal, Dendritic cell, medicine.disease, Combined Modality Therapy, Blockade, 030104 developmental biology, 030220 oncology & carcinogenesis, biology.protein, Immunogenic cell death, Immunotherapy, Antibody

Abstract

Blockade of immune-checkpoints has emerged as one of the most promising approaches to improve the durability of anti-tumor responses in cancer patients. However, the fraction of patients experiencing durable responses to single agent immune checkpoint inhibitor treatment remains limited. Recent clinical reports suggest that patients responding best to checkpoint blockade therapies display higher levels of CD8(+) T-cells in the tumor prior to treatment. Therefore, combination treatments of immune-checkpoint inhibitors with compounds that increase the number of tumor infiltrating CD8(+) T cells may expand the therapeutic benefit of immuno-oncology (IO) drugs. Immunogenic cell death (ICD) of tumor cells is induced by certain classes of cytotoxic compounds and represents a potent stimulator of effector T-cell recruitment to tumors. In addition, several cytotoxics directly stimulate dendritic cell activation and maturation, resulting in improved anti-tumor immune responses when combined with IO compounds. Among them, several cytotoxic agents are currently utilized as payloads for antibody-drug conjugates (ADCs). Therefore, identification of optimal combination regimens between ADC- and IO compounds holds strong promise to overcome the current limitations of immune checkpoint inhibitors, by increasing the recruitment of CD8(+) effector T-cells to the tumor core. Here we review the emerging field of ADC/IO combination research, with a focus on how to optimally combine both modalities. The answer to this question may have a broader impact on oncology drug development, as synergistic activities between IO compounds and ADCs may increase the formation of tumor specific immunological memory, ultimately leading to durable responses in a larger fraction of cancer patients.

Published

2015

38. The process of designing and developing spliceostatin class of splicing inhibitors as payloads for antibody drug conjugates

Author

Frank E. Koehn, Frank Loganzo, Edmund I. Graziani, Christopher J. O’Donnell, Chakrapani Subramanyam, Anokha S. Ratnayake, Sujiet Puthenveetil, Kenneth J. DiRico, Alessandra S. Eustáquio, LP Chang, JE Janso, H He, Jesse Alexander Teske, and N Tumey

Subjects

Pharmacology, Drug, biology, Chemistry, media_common.quotation_subject, Organic Chemistry, Pharmaceutical Science, Computational biology, Analytical Chemistry, Complementary and alternative medicine, Drug Discovery, RNA splicing, biology.protein, Molecular Medicine, Antibody, media_common, Conjugate

Published

2015

39. Paclitaxel-resistant cells have a mutation in the paclitaxel-binding region of β-tubulin (Asp26Glu) and less stable microtubules

Author

Lee M. Greenberger, Frank Loganzo, James H. Nettles, Tami Annable, Malathi Hari, Xingzhi Tan, Daniel B. Morilla, Sylvia Musto, and James P. Snyder

Subjects

Cancer Research, Paclitaxel, Protein Conformation, Glutamic Acid, Mice, Nude, Docetaxel, Pharmacology, Biology, Epothilone, Microtubules, Mice, chemistry.chemical_compound, Tubulin, Microtubule, Cell Line, Tumor, medicine, Animals, Humans, Point Mutation, ATP Binding Cassette Transporter, Subfamily B, Member 1, Aspartic Acid, Taxane, Antineoplastic Agents, Phytogenic, Molecular biology, Vinblastine, Amino Acid Substitution, Verapamil, Oncology, chemistry, Drug Resistance, Neoplasm, Epothilones, Acetylation, Carcinoma, Squamous Cell, biology.protein, Taxoids, medicine.drug

Abstract

Resistance to paclitaxel-based therapy is frequently encountered in the clinic. The mechanisms of intrinsic or acquired paclitaxel resistance are not well understood. We sought to characterize the resistance mechanisms that develop upon chronic exposure of a cancer cell line to paclitaxel in the presence of the P-glycoprotein reversal agent, CL-347099. The epidermoid tumor line KB-3-1 was exposed to increasing concentrations of paclitaxel and 5 μmol/L CL-347099 for up to 1 year. Cells grown in 15 nmol/L paclitaxel plus CL-347099 (KB-15-PTX/099) developed 18-fold resistance to paclitaxel and were dependent upon paclitaxel for maximal growth. They grew well and retained resistance to paclitaxel when grown in athymic mice. Cross-resistance (3- to 5-fold) was observed in tissue culture to docetaxel, the novel taxane MAC-321, and epothilone B. Collateral sensitivity (∼3-fold) was observed to the depolymerizing agents vinblastine, dolastatin-10, and HTI-286. KB-15-PTX/099–resistant cells did not overexpress P-glycoprotein nor did they have an alteration of [14C]paclitaxel accumulation compared with parental cells. However, a novel point mutation (T to A) resulting in Asp26 to glutamate substitution in class I (M40) β-tubulin was found. Based on an electron crystallography structure of Zn-stabilized tubulin sheets, the phenyl ring of C-3′ NHCO-C6H5 of paclitaxel makes contact with Asp26 of β-tubulin, suggesting a ligand-induced mutation. Optimized model complexes of paclitaxel, docetaxel, and MAC-321 in β-tubulin show a novel hydrogen bonding pattern for the glutamate mutant and rationalize the observed resistance profiles. However, a mutation in the paclitaxel binding pocket does not explain the phenotype completely. KB-15-PTX/099 cells have impaired microtubule stability as determined by a reduced percentage of tubulin in microtubules and reflected by less acetylated tubulin. These results suggest that a mutation in tubulin might affect microtubule stability as well as drug binding and contribute to the observed resistance profile. [Mol Cancer Ther 2006;5(2):270–8]

Published

2006

40. Hybrids of the Hemiasterlin Analogue Taltobulin and the Dolastatins Are Potent Antimicrotubule Agents

Author

Arie Zask, Joshua Kaplan, Sylvia Musto, and Frank Loganzo

Subjects

Models, Molecular, Vinca, Protein Conformation, Stereochemistry, Taltobulin, Antineoplastic Agents, Tripeptide, Biochemistry, KB Cells, Catalysis, Tubulin binding, Structure-Activity Relationship, Colloid and Surface Chemistry, Microtubule, Cell Line, Tumor, Depsipeptides, Humans, Binding site, biology, Chemistry, Transporter, General Chemistry, biology.organism_classification, Tubulin Modulators, Tubulin, biology.protein, Thermodynamics, Drug Screening Assays, Antitumor, Oligopeptides

Abstract

The targeting of microtubules is an important mechanism for cancer chemotherapy. However, there is still a need for improved antimicrotubule agents. A number of seemingly structurally disparate peptidic natural products inhibit tubulin polymerization by binding to a region of the tubulin heterodimer close to the vinca binding site. An analogue of the naturally occurring tripeptide hemiasterlin, taltobulin (HTI-286, 3), has advanced to clinical trials. Structure-activity relationship studies of 3 have revealed critical structural elements necessary for antimicrotubule activity that correspond to comparable groups in the amino terminus tripeptide region of the dolastatins. To investigate the structural relationship between the hemiasterlins and the more complex dolastatins, hybrid compounds composed of 3 and the carboxy terminus dipeptides of dolastatin 10, or the dolastatin 15 analogue cemadotin, were synthesized. The resulting hybrid compounds were potent antimicrotubule agents, thus establishing a structural relationship between the hemiasterlins and the dolastatins. This relationship may be useful in the design of analogues having improved activity in resistant cell lines expressing the P-glycoprotein transporter, for establishing structural relationships with other classes of peptidic antimicrotubule agents, or for modeling studies of the tubulin binding site of these agents.

Published

2005

41. Synthesis and activity of novel analogs of hemiasterlin as inhibitors of tubulin polymerization: modification of the A segment

Author

Sylvia Musto, Arie Zask, Chuan Niu, Carolyn Discafani, Frank Loganzo, Tami Annable, Richard Hernandez, Emily B. Norton, Semiramis Ayral-Kaloustian, Carl Beyer, Ayako Yamashita, and Joshua Kaplan

Subjects

Stereochemistry, Clinical Biochemistry, Melanoma, Experimental, Mice, Nude, Pharmaceutical Science, Antineoplastic Agents, macromolecular substances, Ring (chemistry), Biochemistry, Hemiasterlin, KB Cells, Mice, Structure-Activity Relationship, Biopolymers, Tubulin, Drug Discovery, Animals, Humans, Tubulin polymerization, Molecular Biology, Cell Proliferation, Cell growth, Chemistry, Organic Chemistry, Stereoisomerism, Aromaticity, Xenograft Model Antitumor Assays, Tubulin Modulators, Molecular Medicine, Oligopeptides

Abstract

Analogs of hemiasterlin (1) and HTI-286 (2), which contain various aromatic rings in the A segment, were synthesized as potential inhibitors of tubulin polymerization. The structure-activity relationships related to stereo- and regio-chemical effects of substituents on the aromatic ring in the A segment were studied. Analogs, which carry a meta-substituted phenyl ring in the A segment show comparable activity for inhibition of tubulin polymerization to 2, as well as in the cell proliferation assay using KB cells containing P-glycoprotein, compared to those of 1 and 2.

Published

2004

42. Tumor Cells Resistant to a Microtubule-Depolymerizing Hemiasterlin Analogue, HTI-286, Have Mutations in α- or β-Tubulin and Increased Microtubule Stability

Author

Dan L. Sackett, Tami Annable, Frank Loganzo, Jong-Hyeok Kim, Tito Fojo, Lee M. Greenberger, Eva Nogales, and Marianne S. Poruchynsky

Subjects

Mutation, education.field_of_study, Cell growth, Population, Cell, macromolecular substances, Biology, medicine.disease_cause, Biochemistry, Molecular biology, Cell biology, chemistry.chemical_compound, medicine.anatomical_structure, Tubulin, Paclitaxel, chemistry, Microtubule, Acetylation, medicine, biology.protein, education

Abstract

Hemiasterlins are sponge-derived tripeptides that inhibit cell growth by depolymerizing existing microtubules and inhibiting microtubule assembly. Since hemiasterlins are poor substrates for P-glycoprotein, they are attractive candidates for cancer therapy and have been undergoing clinical trials. The basis of resistance to a synthetic analogue of hemiasterlin, HTI-286 (HTI), was examined in cell populations derived from ovarian carcinoma (A2780/1A9) cells selected in HTI-286. 1A9-HTI-resistant cells (1A9-HTI(R) series) were 57-89-fold resistant to HTI. Cross-resistance (3-186-fold) was observed to other tubulin depolymerizing drugs, with collateral sensitivity (2-14-fold) to tubulin polymerizing agents. Evaluation of the percentage of polymerized and soluble tubulin in 1A9 parental and 1A9-HTI(R) cells corroborated the HTI cytotoxicity data. At 22 degrees C or 37 degrees C, in the absence of any drug, the percentage of polymerized microtubules for each of the 1A9-HTI(R) populations was greater than that in the 1A9 parental cells, consistent with more stable microtubules. Furthermore, microtubules in the 1A9-HTI(R) populations were also more resistant to depolymerization at 4 degrees C and had more acetylated and detyrosinated (Glu-tubulin) alpha-tubulin, all characteristic of more stable microtubules. The 1A9-HTI(R) cell populations exhibited either a single nucleotide change in the M40 beta-tubulin isotype, S172A, or in two cell populations where no beta-tubulin mutation was detected, mutations in the Kalpha-1 alpha-tubulin isotype, S165P and R221H in one resistant cell population and I384V in another. Unlike reports of mutations resulting in reduced drug affinity, the experimental data and location of mutations are consistent with resistance to HTI-286 mediated by microtubule-stabilizing mutations in beta- or alpha-tubulin.

Published

2004

43. Synthesis and Biological Activity of Analogues of the Antimicrotubule Agent N,β,β-Trimethyl-<scp>l</scp>-phenylalanyl-N-[(1S,2E)-3-carboxy-1-isopropylbut-2-enyl]- N1,3-dimethyl-<scp>l</scp>-valinamide (HTI-286)

Author

Richard Hernandez, Girija Krishnamurthy, Frank Loganzo, Arie Zask, Ayako Yamashita, Gary Harold Birnberg, Lee M. Greenberger, Zhilian Tang, Sylvia Musto, Tami Annable, Derek C. Cole, Xiaoran Yang, Robert Williamson, Semiramis Ayral-Kaloustian, Gulnaz Khafizova, Carolyn Discafani, Emily B. Norton, Katherine Cheung, Chuan Niu, Ronald Suayan, Joshua Kaplan, and Carl Beyer

Subjects

Antimicrotubule agent, Chemistry, Stereochemistry, Biological activity, Tripeptide, Chemical synthesis, In vitro, Microtubule polymerization, chemistry.chemical_compound, Biochemistry, Paclitaxel, In vivo, Drug Discovery, Molecular Medicine

Abstract

Hemiasterlin (1), a tripeptide isolated from marine sponges, induces microtubule depolymerization and mitotic arrest in cells. HTI-286 (2), an analogue from an initial study of the hemiasterlins, is presently in clinical trials. In addition to its potent antitumor effects, 2 has the advantage of circumventing the P-glycoprotein-mediated resistance that hampers the efficacy of other antimicrotubule agents such as paclitaxel and vincristine in animal models. This paper describes an in-depth study of the structure−activity relationships of analogues of 2, their effects on microtubule polymerization, and their in vitro and in vivo anticancer activity. Regions of the molecule necessary for potent activity are identified. Groups tolerant of modification, leading to novel analogues, are reported. Potent analogues identified through in vivo studies in tumor xenograft models include one superior analogue, HTI-042 (48).

Published

2004

44. Biophysical Characterization of the Interactions of HTI-286 with Tubulin Heterodimer and Microtubules

Author

Frank Loganzo, Wendy Cheng, Girija Krishnamurthy, and Arie Zask, Weidong Ding, Mei-Chu Lo, George A. Ellestad, Ann Aulabaugh, and Vladimir I. Razinkov

Subjects

Glycerol, Circular dichroism, Paclitaxel, macromolecular substances, Calorimetry, Microtubules, Biochemistry, chemistry.chemical_compound, Tubulin, Microtubule, Animals, biology, Tubulin Modulators, Circular Dichroism, Titrimetry, Isothermal titration calorimetry, Dissociation constant, Kinetics, Crystallography, Spectrometry, Fluorescence, Monomer, Microscopy, Fluorescence, chemistry, Sedimentation equilibrium, Chromatography, Gel, biology.protein, Biophysics, Thermodynamics, Cattle, Dimerization, Oligopeptides, Ultracentrifugation

Abstract

HTI-286 is a synthetic analogue of the natural product hemiasterlin and is a potent antimitotic agent. HTI-286 inhibits the proliferation of tumor cells during mitosis. The observed antimitotic activity is due to the binding of HTI-286 to tubulin. This report details the effects of HTI-286 on soluble tubulin and preassembled microtubules. HTI-286 binds tubulin monomer and oligomerizes it to an 18.5 S species corresponding to a discrete ring structure consisting of about 13 tubulin units as determined by sedimentation equilibrium analyses. The rate of formation of the oligomers is dependent on the concentration of HTI-286 and the time of incubation. Tubulin oligomers, specifically the 18.5 S species, form slowly. The interactions of HTI-286 with tubulin were studied by isothermal titration calorimetry. HTI-286 binds tubulin rapidly, and the initial association of HTI-286 with tubulin is enthalpically driven with a DeltaH value of -14 kcal/mol at 25 degrees C and a dissociation constant of ca. 100 nM. However, the accompanying tubulin oligomerization event does not produce measurable heats at 25 degrees C. The dissociation constant estimated from the changes in the intrinsic fluorescence of tubulin was found to be consistent with the calorimetric results. Both HTI-286 and hemiasterlin bind tubulin with nearly equal potency. However, the stability of the tubulin oligomers is not identical under size-exclusion column chromatographic conditions. The tubulin oligomers formed in the presence of HTI-286 dissociate on the column, while the corresponding oligomers formed in the presence of hemiasterlin are stable. Tubulin undergoes a change in the secondary structure in the presence of HTI-286, which is evidenced by changes in the circular dichroic absorption spectrum of tubulin. In contrast to the microtubule-stabilizing effects of paclitaxel, both HTI-286 and hemiasterlin depolymerize preassembled microtubules at micromolar concentrations.

Published

2003

45. Anticancer Agents from Unique Natural Products Sources

Author

Chris Ireland, William Aalbersberg, Raymond Andersen, Semiramis Ayral-Kaloustian, Roberto Berlinck, Valerie Bernan, Guy Carter, Alice Churchill, Jon Clardy, Gisela Concepcion, E. De Silva, Carolyn Discafani, Tito Fojo, Philip Frost, Donna Gibson, Lee Greenberger, Michael Greenstein, Mary Kay Harper, Robert Mallon, Frank Loganzo, Maria Nunes, Marianne Poruchynsky, and Arie Zask

Subjects

Pharmacology, chemistry.chemical_classification, Natural product, Drug discovery, Pharmaceutical Science, General Medicine, Computational biology, Biology, Combinatorial chemistry, Hemiasterlin, Natural (archaeology), chemistry.chemical_compound, Polyketide, Austocystin D, Complementary and alternative medicine, chemistry, Nonribosomal peptide, Drug Discovery, Molecular Medicine, Antimitotic Agent

Abstract

The National Cooperative Natural Products Drug Discovery Group (NCNPDDG) “Anticancer Agents from Unique Natural Products Sources, CA 67786” was first awarded in September 1995. The goal of the project is to discover and develop novel anticancer agents from a variety of natural products sources. The key accomplishments of this NCDDG which will be highlighted in this manuscript include:Development of tools to probe fungi for the production of novel natural products by DNA-based probes. Discovery that the majority of these fungi can produce natural products via nonribosomal peptide synthetases, polyketide synthases, or both – a much larger percentage than current culturing techniques reveal.Identification of the MDR-selective cytotoxic agent austocystin D, and use of a novel yeast deletion strain approach to help identify its molecular target(s).Identification of hemiasterlin and other naturally occurring analogs as potent antimitotic agents with excellent in vivo activity against human solid tumors in mouse...

Published

2003

46. Discovery of cytotoxic dolastatin 10 analogues with N-terminal modifications

Author

Chakrapani Subramanyam, Alison H. Varghese, Christopher J. O’Donnell, Michael J. Shapiro, Suman Shanker, Andreas Maderna, Cynthia Song, Beth C. Vetelino, My-Hanh Lam, Matthew David Doroski, Frank Loganzo, Hud Lawrence Risley, Kathleen A. Farley, Zecheng Chen, Melissa Wagenaar, Carolyn A. Leverett, Jayvardhan Pandit, Alexander M. Porte, Kevin D. Parris, Sylvia Musto, and Sai Chetan K. Sukuru

Subjects

Male, Models, Molecular, Stereochemistry, Protein Conformation, Antineoplastic Agents, Crystallography, X-Ray, Cocrystal, chemistry.chemical_compound, Structure-Activity Relationship, Microtubule, Tandem Mass Spectrometry, Tubulin, Depsipeptides, Neoplasms, Drug Discovery, Peptide bond, Animals, Humans, Rats, Wistar, Cells, Cultured, ADME, Cell Proliferation, chemistry.chemical_classification, Natural product, biology, Molecular Structure, Combinatorial chemistry, Amino acid, Rats, chemistry, Area Under Curve, biology.protein, Hepatocytes, Microsomes, Liver, Molecular Medicine, Drug Screening Assays, Antitumor, Conjugate

Abstract

Auristatins, synthetic analogues of the antineoplastic natural product Dolastatin 10, are ultrapotent cytotoxic microtubule inhibitors that are clinically used as payloads in antibody-drug conjugates (ADCs). The design and synthesis of several new auristatin analogues with N-terminal modifications that include amino acids with α,α-disubstituted carbon atoms are described, including the discovery of our lead auristatin, PF-06380101. This modification of the peptide structure is unprecedented and led to analogues with excellent potencies in tumor cell proliferation assays and differential ADME properties when compared to other synthetic auristatin analogues that are used in the preparation of ADCs. In addition, auristatin cocrystal structures with tubulin are being presented that allow for the detailed examination of their binding modes. A surprising finding is that all analyzed analogues have a cis-configuration at the Val-Dil amide bond in their functionally relevant tubulin bound state, whereas in solution this bond is exclusively in the trans-configuration. This remarkable observation shines light onto the preferred binding mode of auristatins and serves as a valuable tool for structure-based drug design.

Published

2014

47. Synthesis, molecular editing, and biological assessment of the potent cytotoxin leiodermatolide

Author

Maik Schuler, Sylvia Musto, Frank Loganzo, Jens Willwacher, Nina Kausch-Busies, Damien Mailhol, Zhanna Sobol, Andreas Maderna, Elizabeith E. Rubitski, Alois Fürstner, and My-Hanh Lam

Subjects

Natural product, biology, Molecular Structure, Cell growth, Chemistry, Total synthesis, General Chemistry, Biochemistry, Catalysis, Tubulin binding, chemistry.chemical_compound, Colloid and Surface Chemistry, Tubulin, Mechanism of action, Cell culture, Centrosome, biology.protein, medicine, Macrolides, medicine.symptom

Abstract

It was by way of total synthesis that the issues concerning the stereostructure of leiodermatolide (1) have recently been solved; with the target now being unambiguously defined, the mission of synthesis changes as to secure a meaningful supply of this exceedingly scarce natural product derived from a deep-sea sponge. To this end, a scalable route of 19 steps (longest linear sequence) has been developed, which features a catalytic asymmetric propargylation of a highly enolizable β-keto-lactone, a ring closing alkyne metathesis and a modified Stille coupling as the key transformations. Deliberate digression from this robust blueprint brought a first set of analogues into reach, which allowed the lead qualities of 1 to be assessed. The acquired biodata show that 1 is a potent cytotoxin in human tumor cell proliferation assays, distinguished by GI50 values in the ≤3 nM range even for cell lines expressing the Pgp efflux transporter. Studies with human U2OS cells revealed that 1 causes mitotic arrest, micronucleus induction, centrosome amplification and tubulin disruption, even though no evidence for direct tubulin binding has been found in cell-free assays; moreover, the compound does not seem to act through kinase inhibition. Indirect evidence points at centrosome declustering as a possible mechanism of action, which provides a potentially rewarding outlook in that centrosome declustering agents hold promise of being inherently selective for malignant over healthy human tissue.

Published

2014

48. Tumor cells chronically treated with a trastuzumab-maytansinoid antibody-drug conjugate develop varied resistance mechanisms but respond to alternate treatments

Author

Edmund I. Graziani, Jeremy S. Myers, Xingzhi Tan, Veronica Diesl, Andreas Maderna, My-Hanh Lam, Eugene Melamud, Judy Lucas, Sylvia Musto, Frank Loganzo, Kim Arndt, Mike Cinque, William T. Hu, Fang Wang, Kiran Khandke, Kenny Sung Kyoo Kim, Guixian Jin, Maximillian T. Follettie, Christopher J. O’Donnell, Matthew Sung, Hans-Peter Gerber, and Manoj Charati

Subjects

Cancer Research, Antibody-drug conjugate, Immunoconjugates, Proteome, Cell Survival, Receptor, ErbB-2, Antineoplastic Agents, Drug resistance, Biology, Pharmacology, Maytansinoid, Mertansine, chemistry.chemical_compound, Inhibitory Concentration 50, Mice, Antigen, Cell Line, Tumor, Animals, Humans, Gene Expression Profiling, Trastuzumab, Xenograft Model Antitumor Assays, Immunoconjugate, Tumor Burden, body regions, Disease Models, Animal, Protein Transport, Oncology, chemistry, Cell culture, Drug Resistance, Neoplasm, Cancer cell, Antigens, Surface, Female, Multidrug Resistance-Associated Proteins, Transcriptome, Signal Transduction

Abstract

Antibody–drug conjugates (ADC) are emerging as clinically effective therapy. We hypothesized that cancers treated with ADCs would acquire resistance mechanisms unique to immunoconjugate therapy and that changing ADC components may overcome resistance. Breast cancer cell lines were exposed to multiple cycles of anti-Her2 trastuzumab–maytansinoid ADC (TM-ADC) at IC80 concentrations followed by recovery. The resistant cells, 361-TM and JIMT1-TM, were characterized by cytotoxicity, proteomic, transcriptional, and other profiling. Approximately 250-fold resistance to TM-ADC developed in 361-TM cells, and cross-resistance was observed to other non–cleavable-linked ADCs. Strikingly, these 361-TM cells retained sensitivity to ADCs containing cleavable mcValCitPABC-linked auristatins. In JIMT1-TM cells, 16-fold resistance to TM-ADC developed, with cross-resistance to other trastuzumab-ADCs. Both 361-TM and JIMT1-TM cells showed minimal resistance to unconjugated mertansine (DM1) and other chemotherapeutics. Proteomics and immunoblots detected increased ABCC1 (MRP1) drug efflux protein in 361-TM cells, and decreased Her2 (ErbB2) in JIMT1-TM cells. Proteomics also showed alterations in various pathways upon chronic exposure to the drug in both cell models. Tumors derived from 361-TM cells grew in mice and were refractory to TM-ADC compared with parental cells. Hence, acquired resistance to trastuzumab–maytansinoid ADC was generated in cultured cancer cells by chronic drug treatment, and either increased ABCC1 protein or reduced Her2 antigen were primary mediators of resistance. These ADC-resistant cell models retain sensitivity to other ADCs or standard-of-care chemotherapeutics, suggesting that alternate therapies may overcome acquired ADC resistance. Mol Cancer Ther; 14(4); 952–63. ©2015 AACR.

Published

2014

49. Mild method for succinimide hydrolysis on ADCs: impact on ADC potency, stability, exposure, and efficacy

Author

Xiaogang Han, Manoj Charati, Jeff Casavant, Eric Sousa, Judy Lucas, Tracey Clark, L. Nathan Tumey, Edmund I. Graziani, Tao He, Frank Loganzo, Dangshe Ma, and Frank Barletta

Subjects

Stereochemistry, Biomedical Engineering, Pharmaceutical Science, Succinimides, Bioengineering, Sulfides, chemistry.chemical_compound, Hydrolysis, Mice, Protein stability, Succinimide, Drug Stability, Cell Line, Tumor, Neoplasms, Potency, Animals, Humans, Cytotoxicity, Maleimide, Pharmacology, Chemistry, Protein Stability, Immunotoxins, Organic Chemistry, Combinatorial chemistry, body regions, Linker, Biotechnology

Abstract

The stability of the connection between the antibody and the toxin can have a profound impact on ADC safety and efficacy. There has been increasing evidence in recent years that maleimide-based ADCs are prone to payload loss via a retro-Michael type reaction. Herein, we report a mild method for the hydrolysis of the succinimide-thioether ring which results in a “ring-opened” linker. ADCs containing this hydrolyzed succinimide linker show equivalent cytotoxicity, improved in vitro stability, improved PK exposure, and improved efficacy as compared to their nonhydrolyzed counterparts. This method offers a simple way to improve the stability, exposure, and efficacy of maleimide-based ADCs.

Published

2014

50. Cytotoxic Spliceostatins from Burkholderia sp. and Their Semisynthetic Analogues

Author

Frank Loganzo, Frank E. Koehn, Haiyin He, Christopher J. O’Donnell, Jeffrey E. Janso, Min He, Anokha S. Ratnayake, Boris Shor, and Hui Y. Yang

Subjects

Spliceosome, Stereochemistry, Burkholderia, Pharmaceutical Science, Antineoplastic Agents, Biology, Analytical Chemistry, chemistry.chemical_compound, Structure-Activity Relationship, Biosynthesis, Amide, Drug Discovery, Cytotoxic T cell, Humans, Spiro Compounds, RNA, Messenger, Cytotoxicity, Mode of action, Pyrans, Pharmacology, Molecular Structure, Organic Chemistry, Semisynthesis, In vitro, Complementary and alternative medicine, Biochemistry, chemistry, Molecular Medicine, Drug Screening Assays, Antitumor

Abstract

The spliceostatin class of natural products was reported to be potent cytotoxic agents via inhibition of the spliceosome, a key protein complex in the biosynthesis of mature mRNA. As part of an effort to discover novel leads for cancer chemotherapy, we re-examined this class of compounds from several angles, including fermentation of the producing strains, isolation and structure determination of new analogues, and semisynthetic modification. Accordingly, a group of spliceostatins were isolated from a culture broth of Burkholderia sp. FERM BP-3421, and their structures identified by analysis of spectroscopic data. Semisynthesis was performed on the major components 4 and 5 to generate ester and amide derivatives with improved in vitro potency. With their potent activity against tumor cells and unique mode of action, spliceostatins can be considered potential leads for development of cancer drugs.

Published

2014