Initial testing of the replication competent Seneca Valley virus (NTX‐010) by the pediatric preclinical testing program

CL Morton, PJ Houghton, EA Kolb… - Pediatric blood & …, 2010 - Wiley Online Library
CL Morton, PJ Houghton, EA Kolb, R Gorlick, CP Reynolds, MH Kang, JM Maris, ST Keir
Pediatric blood & cancer, 2010Wiley Online Library
Abstract Background Seneca Valley virus (NTX‐010) is a non‐recombinant, replication
competent RNA virus that is undergoing phase 1 clinical trials in adults for tumors with
neuroendocrine characteristics. Here we have evaluated the antitumor activity of NTX‐010
administered systemically. Procedures In vitro NTX‐010 was tested against 23 cell lines
exposed for 96 hr at 1× 10− 4 to 104 viral particles (vp)/cell. In vivo NTX‐010 was
administered intravenously once at 3× 1012 vp/kg. Three measures of antitumor activity …
Background
Seneca Valley virus (NTX‐010) is a non‐recombinant, replication competent RNA virus that is undergoing phase 1 clinical trials in adults for tumors with neuroendocrine characteristics. Here we have evaluated the antitumor activity of NTX‐010 administered systemically.
Procedures
In vitro NTX‐010 was tested against 23 cell lines exposed for 96 hr at 1 × 10−4 to 104 viral particles (vp)/cell. In vivo NTX‐010 was administered intravenously once at 3 × 1012 vp/kg. Three measures of antitumor activity were used: (1) an objective response measure modeled after the clinical setting; (2) a treated to control (T/C) tumor volume measure; and (3) a time to event (fourfold increase in tumor volume for solid tumor models), measure based on the median event‐free survival (EFS) of treated and control animals for each xenograft.
Results
In vitro NTX‐010 demonstrated a marked cytotoxic effect in a subset of the cell lines from the neuroblastoma, Ewing sarcoma, and rhabdomyosarcoma panels. In vivo the most consistent activity was observed for the rhabdomyosarcoma and the neuroblastoma panels, with all four of the alveolar rhabdomyosarcoma xenografts and four of five neuroblastoma xenografts achieving CR or maintained CR. Objective responses were also observed in the rhabdoid tumor, Wilms tumor, and glioblastoma panels.
Conclusions
NTX‐010 demonstrated a high level of activity both in vitro and in vivo. Further analysis of existing testing and molecular characterization data may help define the biological characteristics of cancer cells that are associated with response to NTX‐010. Pediatr Blood Cancer. 2010;55:295–303. © 2010 Wiley–Liss, Inc.
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