α-Radioimmunotherapy with (213)Bi-anti-CD38 immunoconjugates is effective in a mouse model of human multiple myeloma

In spite of development of molecular therapeutics, multiple myeloma (MM) is fatal in most cases. CD38 is a promising target for selective treatment of MM. We tested radioimmunoconjugates consisting of the α-emitter (213)Bi coupled to an anti-CD38 MAb in preclinical treatment of MM. Efficacy of (213)...

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Autores principales: Teiluf, Katharina, Seidl, Christof, Blechert, Birgit, Gaertner, Florian C., Gilbertz, Klaus-Peter, Fernandez, Vanesa, Bassermann, Florian, Endell, Jan, Boxhammer, Rainer, Leclair, Stephane, Vallon, Mario, Aichler, Michaela, Feuchtinger, Annette, Bruchertseifer, Frank, Morgenstern, Alfred, Essler, Markus
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2014
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4467108/
https://www.ncbi.nlm.nih.gov/pubmed/25576914
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author Teiluf, Katharina
Seidl, Christof
Blechert, Birgit
Gaertner, Florian C.
Gilbertz, Klaus-Peter
Fernandez, Vanesa
Bassermann, Florian
Endell, Jan
Boxhammer, Rainer
Leclair, Stephane
Vallon, Mario
Aichler, Michaela
Feuchtinger, Annette
Bruchertseifer, Frank
Morgenstern, Alfred
Essler, Markus
author_facet Teiluf, Katharina
Seidl, Christof
Blechert, Birgit
Gaertner, Florian C.
Gilbertz, Klaus-Peter
Fernandez, Vanesa
Bassermann, Florian
Endell, Jan
Boxhammer, Rainer
Leclair, Stephane
Vallon, Mario
Aichler, Michaela
Feuchtinger, Annette
Bruchertseifer, Frank
Morgenstern, Alfred
Essler, Markus
author_sort Teiluf, Katharina
collection PubMed
description In spite of development of molecular therapeutics, multiple myeloma (MM) is fatal in most cases. CD38 is a promising target for selective treatment of MM. We tested radioimmunoconjugates consisting of the α-emitter (213)Bi coupled to an anti-CD38 MAb in preclinical treatment of MM. Efficacy of (213)Bi-anti-CD38-MAb was assayed towards different MM cell lines with regard to induction of DNA double-strand breaks, induction of apoptosis and initiation of cell cycle arrest. Moreover, mice bearing luciferase-expressing MM xenografts were treated with (213)Bi-anti-CD38-MAb. Therapeutic efficacy was monitored by bioluminescence imaging, overall survival and histology. (213)Bi-anti-CD38-MAb treatment induced DNA damage which did not result in activation of the G2 DNA-damage-response checkpoint, but instead in mitotic arrest and subsequent mitotic catastrophe. The anti-tumor effect of (213)Bi-anti-CD38-MAb correlated with the expression level of CD38 in each MM cell line. In myeloma xenografts, treatment with (213)Bi-anti-CD38-MAb suppressed tumor growth via induction of apoptosis in tumor tissue and significantly prolonged survival compared to controls. The major organ systems did not show any signs of (213)Bi-induced toxicity. Preclinical treatment of MM with (213)Bi-anti-CD38-MAb turned out as an effective therapeutic option.
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spelling pubmed-44671082015-06-22 α-Radioimmunotherapy with (213)Bi-anti-CD38 immunoconjugates is effective in a mouse model of human multiple myeloma Teiluf, Katharina Seidl, Christof Blechert, Birgit Gaertner, Florian C. Gilbertz, Klaus-Peter Fernandez, Vanesa Bassermann, Florian Endell, Jan Boxhammer, Rainer Leclair, Stephane Vallon, Mario Aichler, Michaela Feuchtinger, Annette Bruchertseifer, Frank Morgenstern, Alfred Essler, Markus Oncotarget Research Paper In spite of development of molecular therapeutics, multiple myeloma (MM) is fatal in most cases. CD38 is a promising target for selective treatment of MM. We tested radioimmunoconjugates consisting of the α-emitter (213)Bi coupled to an anti-CD38 MAb in preclinical treatment of MM. Efficacy of (213)Bi-anti-CD38-MAb was assayed towards different MM cell lines with regard to induction of DNA double-strand breaks, induction of apoptosis and initiation of cell cycle arrest. Moreover, mice bearing luciferase-expressing MM xenografts were treated with (213)Bi-anti-CD38-MAb. Therapeutic efficacy was monitored by bioluminescence imaging, overall survival and histology. (213)Bi-anti-CD38-MAb treatment induced DNA damage which did not result in activation of the G2 DNA-damage-response checkpoint, but instead in mitotic arrest and subsequent mitotic catastrophe. The anti-tumor effect of (213)Bi-anti-CD38-MAb correlated with the expression level of CD38 in each MM cell line. In myeloma xenografts, treatment with (213)Bi-anti-CD38-MAb suppressed tumor growth via induction of apoptosis in tumor tissue and significantly prolonged survival compared to controls. The major organ systems did not show any signs of (213)Bi-induced toxicity. Preclinical treatment of MM with (213)Bi-anti-CD38-MAb turned out as an effective therapeutic option. Impact Journals LLC 2014-12-10 /pmc/articles/PMC4467108/ /pubmed/25576914 Text en Copyright: © 2015 Teiluf et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Teiluf, Katharina
Seidl, Christof
Blechert, Birgit
Gaertner, Florian C.
Gilbertz, Klaus-Peter
Fernandez, Vanesa
Bassermann, Florian
Endell, Jan
Boxhammer, Rainer
Leclair, Stephane
Vallon, Mario
Aichler, Michaela
Feuchtinger, Annette
Bruchertseifer, Frank
Morgenstern, Alfred
Essler, Markus
α-Radioimmunotherapy with (213)Bi-anti-CD38 immunoconjugates is effective in a mouse model of human multiple myeloma
title α-Radioimmunotherapy with (213)Bi-anti-CD38 immunoconjugates is effective in a mouse model of human multiple myeloma
title_full α-Radioimmunotherapy with (213)Bi-anti-CD38 immunoconjugates is effective in a mouse model of human multiple myeloma
title_fullStr α-Radioimmunotherapy with (213)Bi-anti-CD38 immunoconjugates is effective in a mouse model of human multiple myeloma
title_full_unstemmed α-Radioimmunotherapy with (213)Bi-anti-CD38 immunoconjugates is effective in a mouse model of human multiple myeloma
title_short α-Radioimmunotherapy with (213)Bi-anti-CD38 immunoconjugates is effective in a mouse model of human multiple myeloma
title_sort α-radioimmunotherapy with (213)bi-anti-cd38 immunoconjugates is effective in a mouse model of human multiple myeloma
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4467108/
https://www.ncbi.nlm.nih.gov/pubmed/25576914
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