Pre-clinical Investigation of Astatine-211-parthanatine for High-risk Neuroblastoma

Overview

Journal Commun Biol

Specialty Biology

Date 2022 Nov 18

PMID 36396952

Authors

Mehran Makvandi

Minu Samanta

Paul Martorano

Hwan Lee

Sarah B Gitto

Khushbu Patel

David Groff

Jennifer Pogoriler

Daniel Martinez

Aladdin Riad

Hannah Dabagian

Michael Zaleski

Tara Taghvaee

Kuiying Xu

Ji Youn Lee

Catherine Hou

Alvin Farrel

Vandana Batra

Sean D Carlin

Daniel J Powell Jr

Robert H Mach

Daniel A Pryma

John M Maris

Affiliations

Soon will be listed here.

Abstract

Astatine-211-parthanatine ([At]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 [At]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 [At]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 [At]PTT for high-risk neuroblastoma.

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