Joseph J Grudzinski1, Reinier Hernandez2, Ian Marsh3, Ravi B Patel4, Eduardo Aluicio-Sarduy3, Jon Engle3,2, Zachary Morris4, Bryan Bednarz3,2,4, Jamey Weichert3,2,5. 1. Department of Medical Physics, University of Wisconsin-Madison, Madison, Wisconsin grudzinski@wisc.edu. 2. Department of Radiology, University of Wisconsin, Madison, Wisconsin. 3. Department of Medical Physics, University of Wisconsin-Madison, Madison, Wisconsin. 4. Department of Human Oncology, University of Wisconsin-Madison, Madison, Wisconsin; and. 5. University of Wisconsin Carbone Cancer Center, Madison, Wisconsin.
Abstract
We characterize the in vivo biodistribution and tumor selectivity of 86Y-NM600, a theranostic alkylphosphocholine radiometal chelate with broad tumor selectivity, in a variety of preclinical cancer models. Methods: Mice bearing flank tumors (representative of lung, pancreatic, prostate, liver, skin, and lymphoid cancers) were injected intravenously with 9.25 MBq of 86Y-NM600 and imaged longitudinally over 4-5 d using small-animal PET/CT. Percentage injected activity per gram (%IA/g) for each volume of interest was measured at each time point for the organs of interest. Mice were euthanized after the final time point, and the tumor and organs of interest were counted with an automatic γ-counter. Absorbed doses delivered by 90Y-NM600 per injected activity (Gy/MBq) were estimated. Mice bearing B78 flank tumors were injected with a prescription of 90Y-NM600 that delivered 2.5 Gy of absorbed tumor dose and was compared with an equivalent absorbed dose delivered via external-beam radiotherapy using tumor volume as a measure of response. Histology and complete blood counts were analyzed in naïve C57BL/6 mice that were injected with 9.25 MBq of 90Y-NM600 at 5, 10, and 28 d after injection. Results: PET imaging showed consistent tumor accumulation and retention across all tumor models investigated, with little off-target retention of NM600 except in the liver, as is characteristic of hepatobiliary metabolism. The tumor uptake was highest in the pancreatic and lymphoid cancer models, reaching peak concentrations of 9.34 ± 2.66 %IA/g (n = 3) and 9.10 ± 0.13 %IA/g (n = 3), respectively, at approximately 40-48 h after injection. These corresponded to tumor dose estimates of 2.72 ± 0.33 Gy/MBq and 2.67 ± 0.32 Gy/MBq, respectively. In the toxicity study, there were no visible signs of acute toxicity by histology, and perturbation of hematologic parameters was transient when observed, returning to pretherapy levels after 28 d. Conclusion: NM600 is a theranostic agent with a unique ability to selectively target a variety of cancer types, presenting a unique opportunity for PET image-guided targeted radionuclide therapy and combination with immunotherapies.
We characterize the in vivo biodistribution and tumor selectivity of 86Y-NM600, a theranostic alkylphosphocholine radiometal chelate with broad tumor selectivity, in a variety of preclinical cancer models. Methods:Mice bearing flank tumors (representative of lung, pancreatic, prostate, liver, skin, and lymphoid cancers) were injected intravenously with 9.25 MBq of 86Y-NM600 and imaged longitudinally over 4-5 d using small-animal PET/CT. Percentage injected activity per gram (%IA/g) for each volume of interest was measured at each time point for the organs of interest. Mice were euthanized after the final time point, and the tumor and organs of interest were counted with an automatic γ-counter. Absorbed doses delivered by 90Y-NM600 per injected activity (Gy/MBq) were estimated. Mice bearing B78 flank tumors were injected with a prescription of 90Y-NM600 that delivered 2.5 Gy of absorbed tumor dose and was compared with an equivalent absorbed dose delivered via external-beam radiotherapy using tumor volume as a measure of response. Histology and complete blood counts were analyzed in naïve C57BL/6 mice that were injected with 9.25 MBq of 90Y-NM600 at 5, 10, and 28 d after injection. Results: PET imaging showed consistent tumor accumulation and retention across all tumor models investigated, with little off-target retention of NM600 except in the liver, as is characteristic of hepatobiliary metabolism. The tumor uptake was highest in the pancreatic and lymphoid cancer models, reaching peak concentrations of 9.34 ± 2.66 %IA/g (n = 3) and 9.10 ± 0.13 %IA/g (n = 3), respectively, at approximately 40-48 h after injection. These corresponded to tumor dose estimates of 2.72 ± 0.33 Gy/MBq and 2.67 ± 0.32 Gy/MBq, respectively. In the toxicity study, there were no visible signs of acute toxicity by histology, and perturbation of hematologic parameters was transient when observed, returning to pretherapy levels after 28 d. Conclusion:NM600 is a theranostic agent with a unique ability to selectively target a variety of cancer types, presenting a unique opportunity for PET image-guided targeted radionuclide therapy and combination with immunotherapies.
Authors: Paul A Clark; Raghava N Sriramaneni; Amber M Bates; Won Jong Jin; Justin C Jagodinsky; Reinier Hernandez; Trang Le; Justin J Jeffery; Ian R Marsh; Joseph J Grudzinski; Eduardo Aluicio-Sarduy; Todd E Barnhart; Bryce R Anderson; Ishan Chakravarty; Ian S Arthur; KyungMann Kim; Jonathan W Engle; Bryan P Bednarz; Jamey P Weichert; Zachary S Morris Journal: Radiat Res Date: 2021-06-01 Impact factor: 2.841
Authors: Ray R Zhang; Cynthia Choi; Christina L Brunnquell; Reinier Hernandez; Anatoly N Pinchuk; Joseph G Grudzinski; Paul A Clark; Alan B McMillan; Anjon Audhya; Justin Jeffrey; John S Kuo; Jamey P Weichert Journal: Invest Radiol Date: 2022-06-22 Impact factor: 10.065
Authors: Megan M Dacek; Darren R Veach; Sarah M Cheal; Lukas M Carter; Michael R McDevitt; Blesida Punzalan; Daniela Burnes Vargas; Thomas Z Kubik; Sebastien Monette; Brian H Santich; Guangbin Yang; Ouathek Ouerfelli; Adam L Kesner; Nai-Kong V Cheung; David A Scheinberg; Steven M Larson; Simone Krebs Journal: Bioconjug Chem Date: 2021-04-05 Impact factor: 4.774
Authors: Justin C Jagodinsky; Won Jong Jin; Amber M Bates; Reinier Hernandez; Joseph J Grudzinski; Ian R Marsh; Ishan Chakravarty; Ian S Arthur; Luke M Zangl; Ryan J Brown; Erin J Nystuen; Sarah E Emma; Caroline Kerr; Peter M Carlson; Raghava N Sriramaneni; Jonathan W Engle; Eduardo Aluicio-Sarduy; Todd E Barnhart; Trang Le; KyungMann Kim; Bryan P Bednarz; Jamey P Weichert; Ravi B Patel; Zachary S Morris Journal: Theranostics Date: 2021-04-15 Impact factor: 11.600
Authors: Kara Magee; Ian R Marsh; Michelle M Turek; Joseph Grudzinski; Eduardo Aluicio-Sarduy; Jonathan W Engle; Ilene D Kurzman; Cindy L Zuleger; Elizabeth A Oseid; Christine Jaskowiak; Mark R Albertini; Karla Esbona; Bryan Bednarz; Paul M Sondel; Jamey P Weichert; Zachary S Morris; Reinier Hernandez; David M Vail Journal: PLoS One Date: 2021-08-12 Impact factor: 3.752
Authors: Hemanth K Potluri; Carolina A Ferreira; Joseph Grudzinski; Christopher Massey; Eduardo Aluicio-Sarduy; Jonathan W Engle; Ohyun Kwon; Ian R Marsh; Bryan P Bednarz; Reinier Hernandez; Jamey P Weichert; Douglas G McNeel Journal: J Immunother Cancer Date: 2022-08 Impact factor: 12.469
Authors: Reinier Hernandez; Joseph J Grudzinski; Eduardo Aluicio-Sarduy; Christopher F Massey; Anatoly N Pinchuk; Ariana N Bitton; Ravi Patel; Ray Zhang; Aakarsha V Rao; Gopal Iyer; Jonathan W Engle; Jamey P Weichert Journal: J Nucl Med Date: 2019-12-20 Impact factor: 10.057