Angiogenesis inhibitor TNP-470 during bone marrow transplant: safety in a preclinical model.
Publication/Presentation Date
4-1-2001
Abstract
High-dose therapy with stem cell rescue is a treatment option for patients with advanced solid tumors. Although this approach has promise for some pediatric cancers, especially neuroblastoma, it is limited by the risk of relapse posttransplant as well as concern about possible reinfused tumor cells in autologous stem cell products. Antiangiogenic agents given during and after recovery from high-dose therapy with stem cell rescue may decrease the risk of relapse. TNP-470 is an antiangiogenic agent now in clinical trials. Although it inhibits the growth of bone marrow (BM) colony-forming cells in vitro, no significant hematological toxicity has been seen in Phase I trials. To assess the feasibility of using antiangiogenic agents during the period of posttransplant hematopoietic engraftment, we have developed a model of stem cell transplant in mice. Mice were lethally irradiated and then rescued with stem cells containing a transgene expressed in the hematopoietic lineage. Mice were then treated with TNP-470 or placebo, and assessed for survival, successful engraftment, and kinetics of engraftment. Both treated and control mice demonstrated reliable multilineage engraftment as well as normal lymphoid maturation with no excess mortality in the treated group. WBCs were lower but still within the normal range at d+28 in mice treated with bolus TNP-470, but not in those treated with continuous infusion TNP-470, compared with controls. These data indicate that inhibitors of angiogenesis do not adversely impact engraftment after stem cell transplantation.
Volume
7
Issue
4
First Page
1026
Last Page
1032
ISSN
1078-0432
Published In/Presented At
Stern, J. W., Fang, J., Shusterman, S., Pierson, G., Barr, R., Pawel, B., Diller, L., & Grupp, S. A. (2001). Angiogenesis inhibitor TNP-470 during bone marrow transplant: safety in a preclinical model. Clinical cancer research : an official journal of the American Association for Cancer Research, 7(4), 1026–1032.
Disciplines
Medicine and Health Sciences | Pediatrics
PubMedID
11309354
Department(s)
Department of Pediatrics
Document Type
Article