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A homogeneous high-DAR antibody–drug conjugate platform combining THIOMAB antibodies and XTEN polypeptides

The antibody–drug conjugate (ADC) is a well-validated modality for the cell-specific delivery of small molecules with impact expanding rapidly beyond their originally-intended purpose of treating cancer. However, antibody-mediated delivery (AMD) remains inefficient, limiting its applicability to tar...

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Autores principales: Zacharias, Neelie, Podust, Vladimir N., Kajihara, Kimberly K., Leipold, Douglas, Del Rosario, Geoffrey, Thayer, Desiree, Dong, Emily, Paluch, Maciej, Fischer, David, Zheng, Kai, Lei, Corinna, He, Jintang, Ng, Carl, Su, Dian, Liu, Luna, Masih, Shabkhaiz, Sawyer, William, Tinianow, Jeff, Marik, Jan, Yip, Victor, Li, Guangmin, Chuh, Josefa, Morisaki, J. Hiroshi, Park, Summer, Zheng, Bing, Hernandez-Barry, Hilda, Loyet, Kelly M., Xu, Min, Kozak, Katherine R., Phillips, Gail Lewis, Shen, Ben-Quan, Wu, Cong, Xu, Keyang, Yu, Shang-Fan, Kamath, Amrita, Rowntree, Rebecca K., Reilly, Dorothea, Pillow, Thomas, Polson, Andrew, Schellenberger, Volker, Hazenbos, Wouter L. W., Sadowsky, Jack
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8926172/
https://www.ncbi.nlm.nih.gov/pubmed/35414872
http://dx.doi.org/10.1039/d1sc05243h
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author Zacharias, Neelie
Podust, Vladimir N.
Kajihara, Kimberly K.
Leipold, Douglas
Del Rosario, Geoffrey
Thayer, Desiree
Dong, Emily
Paluch, Maciej
Fischer, David
Zheng, Kai
Lei, Corinna
He, Jintang
Ng, Carl
Su, Dian
Liu, Luna
Masih, Shabkhaiz
Sawyer, William
Tinianow, Jeff
Marik, Jan
Yip, Victor
Li, Guangmin
Chuh, Josefa
Morisaki, J. Hiroshi
Park, Summer
Zheng, Bing
Hernandez-Barry, Hilda
Loyet, Kelly M.
Xu, Min
Kozak, Katherine R.
Phillips, Gail Lewis
Shen, Ben-Quan
Wu, Cong
Xu, Keyang
Yu, Shang-Fan
Kamath, Amrita
Rowntree, Rebecca K.
Reilly, Dorothea
Pillow, Thomas
Polson, Andrew
Schellenberger, Volker
Hazenbos, Wouter L. W.
Sadowsky, Jack
author_facet Zacharias, Neelie
Podust, Vladimir N.
Kajihara, Kimberly K.
Leipold, Douglas
Del Rosario, Geoffrey
Thayer, Desiree
Dong, Emily
Paluch, Maciej
Fischer, David
Zheng, Kai
Lei, Corinna
He, Jintang
Ng, Carl
Su, Dian
Liu, Luna
Masih, Shabkhaiz
Sawyer, William
Tinianow, Jeff
Marik, Jan
Yip, Victor
Li, Guangmin
Chuh, Josefa
Morisaki, J. Hiroshi
Park, Summer
Zheng, Bing
Hernandez-Barry, Hilda
Loyet, Kelly M.
Xu, Min
Kozak, Katherine R.
Phillips, Gail Lewis
Shen, Ben-Quan
Wu, Cong
Xu, Keyang
Yu, Shang-Fan
Kamath, Amrita
Rowntree, Rebecca K.
Reilly, Dorothea
Pillow, Thomas
Polson, Andrew
Schellenberger, Volker
Hazenbos, Wouter L. W.
Sadowsky, Jack
author_sort Zacharias, Neelie
collection PubMed
description The antibody–drug conjugate (ADC) is a well-validated modality for the cell-specific delivery of small molecules with impact expanding rapidly beyond their originally-intended purpose of treating cancer. However, antibody-mediated delivery (AMD) remains inefficient, limiting its applicability to targeting highly potent payloads to cells with high antigen expression. Maximizing the number of payloads delivered per antibody is one key way in which delivery efficiency can be improved, although this has been challenging to carry out; with few exceptions, increasing the drug-to-antibody ratio (DAR) above ∼4 typically destroys the biophysical properties and in vivo efficacy for ADCs. Herein, we describe the development of a novel bioconjugation platform combining cysteine-engineered (THIOMAB) antibodies and recombinant XTEN polypeptides for the unprecedented generation of homogeneous, stable “TXCs” with DAR of up to 18. Across three different bioactive payloads, we demonstrated improved AMD to tumors and Staphylococcus aureus bacteria for high-DAR TXCs relative to conventional low-DAR ADCs.
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spelling pubmed-89261722022-04-11 A homogeneous high-DAR antibody–drug conjugate platform combining THIOMAB antibodies and XTEN polypeptides Zacharias, Neelie Podust, Vladimir N. Kajihara, Kimberly K. Leipold, Douglas Del Rosario, Geoffrey Thayer, Desiree Dong, Emily Paluch, Maciej Fischer, David Zheng, Kai Lei, Corinna He, Jintang Ng, Carl Su, Dian Liu, Luna Masih, Shabkhaiz Sawyer, William Tinianow, Jeff Marik, Jan Yip, Victor Li, Guangmin Chuh, Josefa Morisaki, J. Hiroshi Park, Summer Zheng, Bing Hernandez-Barry, Hilda Loyet, Kelly M. Xu, Min Kozak, Katherine R. Phillips, Gail Lewis Shen, Ben-Quan Wu, Cong Xu, Keyang Yu, Shang-Fan Kamath, Amrita Rowntree, Rebecca K. Reilly, Dorothea Pillow, Thomas Polson, Andrew Schellenberger, Volker Hazenbos, Wouter L. W. Sadowsky, Jack Chem Sci Chemistry The antibody–drug conjugate (ADC) is a well-validated modality for the cell-specific delivery of small molecules with impact expanding rapidly beyond their originally-intended purpose of treating cancer. However, antibody-mediated delivery (AMD) remains inefficient, limiting its applicability to targeting highly potent payloads to cells with high antigen expression. Maximizing the number of payloads delivered per antibody is one key way in which delivery efficiency can be improved, although this has been challenging to carry out; with few exceptions, increasing the drug-to-antibody ratio (DAR) above ∼4 typically destroys the biophysical properties and in vivo efficacy for ADCs. Herein, we describe the development of a novel bioconjugation platform combining cysteine-engineered (THIOMAB) antibodies and recombinant XTEN polypeptides for the unprecedented generation of homogeneous, stable “TXCs” with DAR of up to 18. Across three different bioactive payloads, we demonstrated improved AMD to tumors and Staphylococcus aureus bacteria for high-DAR TXCs relative to conventional low-DAR ADCs. The Royal Society of Chemistry 2022-01-28 /pmc/articles/PMC8926172/ /pubmed/35414872 http://dx.doi.org/10.1039/d1sc05243h Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Zacharias, Neelie
Podust, Vladimir N.
Kajihara, Kimberly K.
Leipold, Douglas
Del Rosario, Geoffrey
Thayer, Desiree
Dong, Emily
Paluch, Maciej
Fischer, David
Zheng, Kai
Lei, Corinna
He, Jintang
Ng, Carl
Su, Dian
Liu, Luna
Masih, Shabkhaiz
Sawyer, William
Tinianow, Jeff
Marik, Jan
Yip, Victor
Li, Guangmin
Chuh, Josefa
Morisaki, J. Hiroshi
Park, Summer
Zheng, Bing
Hernandez-Barry, Hilda
Loyet, Kelly M.
Xu, Min
Kozak, Katherine R.
Phillips, Gail Lewis
Shen, Ben-Quan
Wu, Cong
Xu, Keyang
Yu, Shang-Fan
Kamath, Amrita
Rowntree, Rebecca K.
Reilly, Dorothea
Pillow, Thomas
Polson, Andrew
Schellenberger, Volker
Hazenbos, Wouter L. W.
Sadowsky, Jack
A homogeneous high-DAR antibody–drug conjugate platform combining THIOMAB antibodies and XTEN polypeptides
title A homogeneous high-DAR antibody–drug conjugate platform combining THIOMAB antibodies and XTEN polypeptides
title_full A homogeneous high-DAR antibody–drug conjugate platform combining THIOMAB antibodies and XTEN polypeptides
title_fullStr A homogeneous high-DAR antibody–drug conjugate platform combining THIOMAB antibodies and XTEN polypeptides
title_full_unstemmed A homogeneous high-DAR antibody–drug conjugate platform combining THIOMAB antibodies and XTEN polypeptides
title_short A homogeneous high-DAR antibody–drug conjugate platform combining THIOMAB antibodies and XTEN polypeptides
title_sort homogeneous high-dar antibody–drug conjugate platform combining thiomab antibodies and xten polypeptides
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8926172/
https://www.ncbi.nlm.nih.gov/pubmed/35414872
http://dx.doi.org/10.1039/d1sc05243h
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