Anti-CD45 Radioimmunotherapy with .sup.90Y but Not .sup.177Lu Is Effective Treatment in a Syngeneic Murine Leukemia Model

Radioimmunotherapy (RIT) for treatment of hematologic malignancies has primarily employed monoclonal antibodies (Ab) labeled with .sup.131 I or .sup.90 Y which have limitations, and alternative radionuclides are needed to facilitate wider adoption of RIT. We therefore compared the relative therapeut...

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Veröffentlicht in:PloS one 2014-12, Vol.9 (12)
Hauptverfasser: Orozco, Johnnie J, Balkin, Ethan R, Gooley, Ted A, Kenoyer, Aimee, Hamlin, Donald K, Wilbur, D. Scott, Fisher, Darrell R, Hylarides, Mark D, Shadman, Mazyar, Green, Damian J, Gopal, Ajay K, Press, Oliver W, Pagel, John M
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container_issue 12
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container_title PloS one
container_volume 9
creator Orozco, Johnnie J
Balkin, Ethan R
Gooley, Ted A
Kenoyer, Aimee
Hamlin, Donald K
Wilbur, D. Scott
Fisher, Darrell R
Hylarides, Mark D
Shadman, Mazyar
Green, Damian J
Gopal, Ajay K
Press, Oliver W
Pagel, John M
description Radioimmunotherapy (RIT) for treatment of hematologic malignancies has primarily employed monoclonal antibodies (Ab) labeled with .sup.131 I or .sup.90 Y which have limitations, and alternative radionuclides are needed to facilitate wider adoption of RIT. We therefore compared the relative therapeutic efficacy and toxicity of anti-CD45 RIT employing .sup.90 Y and .sup.177 Lu in a syngeneic, disseminated murine myeloid leukemia (B6SJLF1/J) model. Biodistribution studies showed that both .sup.90 Y- and .sup.177 Lu-anti-murine CD45 Ab conjugates (DOTA-30F11) targeted hematologic tissues, as at 24 hours 48.8±21.2 and 156±14.6% injected dose per gram of tissue (% ID/g) of .sup.90 Y-DOTA-30F11 and 54.2±9.5 and 199±11.7% ID/g of .sup.177 Lu-DOTA-30F11 accumulated in bone marrow (BM) and spleen, respectively. However, .sup.90 Y-DOTA-30F11 RIT demonstrated a dose-dependent survival benefit: 60% of mice treated with 300 [micro]Ci .sup.90 Y-DOTA-30F11 lived over 180 days after therapy, and mice treated with 100 [micro]Ci .sup.90 Y-DOTA-30F11 had a median survival 66 days. .sup.90 Y-anti-CD45 RIT was associated with transient, mild myelotoxicity without hepatic or renal toxicity. Conversely, .sup.177 Lu- anti-CD45 RIT yielded no long-term survivors. Thus, .sup.90 Y was more effective than .sup.177 Lu for anti-CD45 RIT of AML in this murine leukemia model.
doi_str_mv 10.1371/journal.pone.0113601
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Scott ; Fisher, Darrell R ; Hylarides, Mark D ; Shadman, Mazyar ; Green, Damian J ; Gopal, Ajay K ; Press, Oliver W ; Pagel, John M</creator><creatorcontrib>Orozco, Johnnie J ; Balkin, Ethan R ; Gooley, Ted A ; Kenoyer, Aimee ; Hamlin, Donald K ; Wilbur, D. Scott ; Fisher, Darrell R ; Hylarides, Mark D ; Shadman, Mazyar ; Green, Damian J ; Gopal, Ajay K ; Press, Oliver W ; Pagel, John M</creatorcontrib><description>Radioimmunotherapy (RIT) for treatment of hematologic malignancies has primarily employed monoclonal antibodies (Ab) labeled with .sup.131 I or .sup.90 Y which have limitations, and alternative radionuclides are needed to facilitate wider adoption of RIT. We therefore compared the relative therapeutic efficacy and toxicity of anti-CD45 RIT employing .sup.90 Y and .sup.177 Lu in a syngeneic, disseminated murine myeloid leukemia (B6SJLF1/J) model. Biodistribution studies showed that both .sup.90 Y- and .sup.177 Lu-anti-murine CD45 Ab conjugates (DOTA-30F11) targeted hematologic tissues, as at 24 hours 48.8±21.2 and 156±14.6% injected dose per gram of tissue (% ID/g) of .sup.90 Y-DOTA-30F11 and 54.2±9.5 and 199±11.7% ID/g of .sup.177 Lu-DOTA-30F11 accumulated in bone marrow (BM) and spleen, respectively. However, .sup.90 Y-DOTA-30F11 RIT demonstrated a dose-dependent survival benefit: 60% of mice treated with 300 [micro]Ci .sup.90 Y-DOTA-30F11 lived over 180 days after therapy, and mice treated with 100 [micro]Ci .sup.90 Y-DOTA-30F11 had a median survival 66 days. .sup.90 Y-anti-CD45 RIT was associated with transient, mild myelotoxicity without hepatic or renal toxicity. Conversely, .sup.177 Lu- anti-CD45 RIT yielded no long-term survivors. 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Biodistribution studies showed that both .sup.90 Y- and .sup.177 Lu-anti-murine CD45 Ab conjugates (DOTA-30F11) targeted hematologic tissues, as at 24 hours 48.8±21.2 and 156±14.6% injected dose per gram of tissue (% ID/g) of .sup.90 Y-DOTA-30F11 and 54.2±9.5 and 199±11.7% ID/g of .sup.177 Lu-DOTA-30F11 accumulated in bone marrow (BM) and spleen, respectively. However, .sup.90 Y-DOTA-30F11 RIT demonstrated a dose-dependent survival benefit: 60% of mice treated with 300 [micro]Ci .sup.90 Y-DOTA-30F11 lived over 180 days after therapy, and mice treated with 100 [micro]Ci .sup.90 Y-DOTA-30F11 had a median survival 66 days. .sup.90 Y-anti-CD45 RIT was associated with transient, mild myelotoxicity without hepatic or renal toxicity. Conversely, .sup.177 Lu- anti-CD45 RIT yielded no long-term survivors. 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Scott</au><au>Fisher, Darrell R</au><au>Hylarides, Mark D</au><au>Shadman, Mazyar</au><au>Green, Damian J</au><au>Gopal, Ajay K</au><au>Press, Oliver W</au><au>Pagel, John M</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Anti-CD45 Radioimmunotherapy with .sup.90Y but Not .sup.177Lu Is Effective Treatment in a Syngeneic Murine Leukemia Model</atitle><jtitle>PloS one</jtitle><date>2014-12-02</date><risdate>2014</risdate><volume>9</volume><issue>12</issue><issn>1932-6203</issn><eissn>1932-6203</eissn><abstract>Radioimmunotherapy (RIT) for treatment of hematologic malignancies has primarily employed monoclonal antibodies (Ab) labeled with .sup.131 I or .sup.90 Y which have limitations, and alternative radionuclides are needed to facilitate wider adoption of RIT. We therefore compared the relative therapeutic efficacy and toxicity of anti-CD45 RIT employing .sup.90 Y and .sup.177 Lu in a syngeneic, disseminated murine myeloid leukemia (B6SJLF1/J) model. 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subjects Comparative analysis
Health aspects
Mouse leukemia complex
Radioimmunotherapy
title Anti-CD45 Radioimmunotherapy with .sup.90Y but Not .sup.177Lu Is Effective Treatment in a Syngeneic Murine Leukemia Model
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