Pre-clinical investigation of astatine-211-parthanatine for high-risk neuroblastoma

Author:

Makvandi Mehran,Samanta Minu,Martorano Paul,Lee Hwan,Gitto Sarah B.,Patel Khushbu,Groff DavidORCID,Pogoriler JenniferORCID,Martinez Daniel,Riad Aladdin,Dabagian Hannah,Zaleski MichaelORCID,Taghvaee Tara,Xu Kuiying,Lee Ji Youn,Hou CatherineORCID,Farrel Alvin,Batra Vandana,Carlin Sean D.,Powell Daniel J.ORCID,Mach Robert H.,Pryma Daniel A.ORCID,Maris John M.ORCID

Abstract

AbstractAstatine-211-parthanatine ([211At]PTT) is an alpha-emitting radiopharmaceutical therapeutic that targets poly(adenosine-diphosphate-ribose) polymerase 1 (PARP1) in cancer cells. High-risk neuroblastomas exhibit among the highest PARP1 expression across solid tumors. In this study, we evaluated the efficacy of [211At]PTT using 11 patient-derived xenograft (PDX) mouse models of high-risk neuroblastoma, and assessed hematological and marrow toxicity in a CB57/BL6 healthy mouse model. We observed broad efficacy in PDX models treated with [211At]PTT at the maximum tolerated dose (MTD 36 MBq/kg/fraction x4) administered as a fractionated regimen. For the MTD, complete tumor response was observed in 81.8% (18 of 22) of tumors and the median event free survival was 72 days with 30% (6/20) of mice showing no measurable tumor >95 days. Reversible hematological and marrow toxicity was observed 72 hours post-treatment at the MTD, however full recovery was evident by 4 weeks post-therapy. These data support clinical development of [211At]PTT for high-risk neuroblastoma.

Funder

U.S. Department of Health & Human Services | NIH | National Cancer Institute

U.S. Department of Energy

Publisher

Springer Science and Business Media LLC

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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