Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells

A number of agents designed for immunotherapy of Acute Myeloid Leukemia (AML) are in preclinical and early clinical development. Most of them target a single antigen on the surface of AML cells. Here we describe the development and key biological properties of a tri-specific agent, the dual-targetin...

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Autores principales: Braciak, Todd A., Roskopf, Claudia C., Wildenhain, Sarah, Fenn, Nadja C., Schiller, Christian B., Schubert, Ingo A., Jacob, Uwe, Honegger, Annemarie, Krupka, Christina, Subklewe, Marion, Spiekermann, Karsten, Hopfner, Karl-Peter, Fey, Georg H., Aigner, Michael, Krause, Stefan, Mackensen, Andreas, Oduncu, Fuat S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2018
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6140553/
https://www.ncbi.nlm.nih.gov/pubmed/30228941
http://dx.doi.org/10.1080/2162402X.2018.1472195
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author Braciak, Todd A.
Roskopf, Claudia C.
Wildenhain, Sarah
Fenn, Nadja C.
Schiller, Christian B.
Schubert, Ingo A.
Jacob, Uwe
Honegger, Annemarie
Krupka, Christina
Subklewe, Marion
Spiekermann, Karsten
Hopfner, Karl-Peter
Fey, Georg H.
Aigner, Michael
Krause, Stefan
Mackensen, Andreas
Oduncu, Fuat S.
author_facet Braciak, Todd A.
Roskopf, Claudia C.
Wildenhain, Sarah
Fenn, Nadja C.
Schiller, Christian B.
Schubert, Ingo A.
Jacob, Uwe
Honegger, Annemarie
Krupka, Christina
Subklewe, Marion
Spiekermann, Karsten
Hopfner, Karl-Peter
Fey, Georg H.
Aigner, Michael
Krause, Stefan
Mackensen, Andreas
Oduncu, Fuat S.
author_sort Braciak, Todd A.
collection PubMed
description A number of agents designed for immunotherapy of Acute Myeloid Leukemia (AML) are in preclinical and early clinical development. Most of them target a single antigen on the surface of AML cells. Here we describe the development and key biological properties of a tri-specific agent, the dual-targeting triplebody SPM-2, with binding sites for target antigens CD33 and CD123, and for CD16 to engage NK cells as cytolytic effectors. Primary blasts of nearly all AML patients carry at least one of these target antigens and the pair is particularly promising for the elimination of blasts and leukemia stem cells (LSCs) from a majority of AML patients by dual-targeting agents. The cytolytic activity of NK cells mediated by SPM-2 was analyzed in vitro for primary leukemic cells from 29 patients with a broad range of AML-subtypes. Blasts from all 29 patients, including patients with genomic alterations associated with an unfavorable genetic subtype, were lysed at nanomolar concentrations of SPM-2. Maximum susceptibility was observed for cells with a combined density of CD33 and CD123 above 10,000 copies/cell. Cell populations enriched for AML-LSCs (CD34pos and CD34pos CD38neg cells) from 2 AML patients carried an increased combined antigen density and were lysed at correspondingly lower concentrations of SPM-2 than unsorted blasts. These initial findings raise the expectation that SPM-2 may also be capable of eliminating AML-LSCs and thus of prolonging survival. In the future, patients with a broad range of AML subtypes may benefit from treatment with SPM-2.
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spelling pubmed-61405532018-10-29 Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells Braciak, Todd A. Roskopf, Claudia C. Wildenhain, Sarah Fenn, Nadja C. Schiller, Christian B. Schubert, Ingo A. Jacob, Uwe Honegger, Annemarie Krupka, Christina Subklewe, Marion Spiekermann, Karsten Hopfner, Karl-Peter Fey, Georg H. Aigner, Michael Krause, Stefan Mackensen, Andreas Oduncu, Fuat S. Oncoimmunology Original Research A number of agents designed for immunotherapy of Acute Myeloid Leukemia (AML) are in preclinical and early clinical development. Most of them target a single antigen on the surface of AML cells. Here we describe the development and key biological properties of a tri-specific agent, the dual-targeting triplebody SPM-2, with binding sites for target antigens CD33 and CD123, and for CD16 to engage NK cells as cytolytic effectors. Primary blasts of nearly all AML patients carry at least one of these target antigens and the pair is particularly promising for the elimination of blasts and leukemia stem cells (LSCs) from a majority of AML patients by dual-targeting agents. The cytolytic activity of NK cells mediated by SPM-2 was analyzed in vitro for primary leukemic cells from 29 patients with a broad range of AML-subtypes. Blasts from all 29 patients, including patients with genomic alterations associated with an unfavorable genetic subtype, were lysed at nanomolar concentrations of SPM-2. Maximum susceptibility was observed for cells with a combined density of CD33 and CD123 above 10,000 copies/cell. Cell populations enriched for AML-LSCs (CD34pos and CD34pos CD38neg cells) from 2 AML patients carried an increased combined antigen density and were lysed at correspondingly lower concentrations of SPM-2 than unsorted blasts. These initial findings raise the expectation that SPM-2 may also be capable of eliminating AML-LSCs and thus of prolonging survival. In the future, patients with a broad range of AML subtypes may benefit from treatment with SPM-2. Taylor & Francis 2018-07-30 /pmc/articles/PMC6140553/ /pubmed/30228941 http://dx.doi.org/10.1080/2162402X.2018.1472195 Text en Published with license by Taylor & Francis. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivatives License (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited, and is not altered, transformed, or built upon in any way.
spellingShingle Original Research
Braciak, Todd A.
Roskopf, Claudia C.
Wildenhain, Sarah
Fenn, Nadja C.
Schiller, Christian B.
Schubert, Ingo A.
Jacob, Uwe
Honegger, Annemarie
Krupka, Christina
Subklewe, Marion
Spiekermann, Karsten
Hopfner, Karl-Peter
Fey, Georg H.
Aigner, Michael
Krause, Stefan
Mackensen, Andreas
Oduncu, Fuat S.
Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells
title Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells
title_full Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells
title_fullStr Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells
title_full_unstemmed Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells
title_short Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells
title_sort dual-targeting triplebody 33-16-123 (spm-2) mediates effective redirected lysis of primary blasts from patients with a broad range of aml subtypes in combination with natural killer cells
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6140553/
https://www.ncbi.nlm.nih.gov/pubmed/30228941
http://dx.doi.org/10.1080/2162402X.2018.1472195
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