Effectiveness of two different dose administration regimens of an IL-15 superagonist complex (ALT-803) in an orthotopic bladder cancer mouse model

Hideki Furuya; Owen T. M. Chan; Ian Pagano; Chengjun Zhu; Nari Kim; Rafael Peres; Kanani Hokutan; Sarah Alter; Peter Rhode; Charles J. Rosser

doi:10.1186/s12967-019-1778-6

Journal of Translational Medicine (Jan 2019)

Effectiveness of two different dose administration regimens of an IL-15 superagonist complex (ALT-803) in an orthotopic bladder cancer mouse model

Hideki Furuya,
Owen T. M. Chan,
Ian Pagano,
Chengjun Zhu,
Nari Kim,
Rafael Peres,
Kanani Hokutan,
Sarah Alter,
Peter Rhode,
Charles J. Rosser

Affiliations

Hideki Furuya: Translational and Clinical Research Program, University of Hawaii Cancer Center
Owen T. M. Chan: Pathology Shared Resource, University of Hawaii Cancer Center
Ian Pagano: Cancer Prevention in the Pacific Program, University of Hawaii Cancer Center
Chengjun Zhu: Translational and Clinical Research Program, University of Hawaii Cancer Center
Nari Kim: Translational and Clinical Research Program, University of Hawaii Cancer Center
Rafael Peres: Translational and Clinical Research Program, University of Hawaii Cancer Center
Kanani Hokutan: Translational and Clinical Research Program, University of Hawaii Cancer Center
Sarah Alter: Altor Bioscience Corp
Peter Rhode: Altor Bioscience Corp
Charles J. Rosser: Translational and Clinical Research Program, University of Hawaii Cancer Center

DOI: https://doi.org/10.1186/s12967-019-1778-6
Journal volume & issue: Vol. 17, no. 1
pp. 1 – 12

Abstract

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Abstract Background We set out to determine if the administration of subcutaneous (SQ) ALT-803 was non-inferior to standard intravesical BCG treatment in a carcinogen induced mouse (C57BL/6J) bladder cancer model. Methods Using this well-established carcinogen induced mouse model, we studied the effects of various dosing schemas of ALT-803 (SQ alone, SQ with intravesical BCG, intravesical alone, intravesical with intravesical BCG) compared to intravesical BCG alone (positive control) and PBS (negative control). The non-inferiority margin for the difference in bladder weight, as a surrogate for tumor mass, was defined as 7%. Results All treatment groups (i.e., ALT-803 SQ alone, ALT-803 SQ with intravesical BCG, ALT-803 intravesical alone, ALT-803 intravesical with intravesical BCG and intravesical BCG alone) demonstrated a significant reduction in tumor burden as evident by bladder weights and H&E stain (p < 0.005). Non-inferiority tests between the intravesical BCG alone group and the additional treatment groups showed that SQ ALT-803 alone (p = 0.04) and BCG plus SQ ALT-803 (p = 0.009) were non-inferior to intravesical BCG alone. In this model, we did not see an appreciable infiltration of CD4+ T, CD8+ T or CD161/KLRB1+ natural killer (NK) cells in the bladder/tumor. When assessing peripheral blood mononuclear cells, SQ ALT-803 alone resulted in a robust induction of CD8+ T cells (p < 0.01), NKG2D+ NK cells (p < 0.005) and CD3+/NKG2D+ NKT cells (p < 0.005) compared to other groups, while in splenic tissue, SQ ALT-803 alone resulted in a robust induction of CD3+/NKG2D+ NKT cells (p < 0.005) compared to other groups. Conclusion Subcutaneous ALT-803 treatment alone or in combination with intravesical BCG was well tolerated and was not inferior to intravesical BCG alone. CD8+ T, NKG2D+ NK and CD3+/NKG2D+ NKT cell induction along with induction of key cytokines remain steadfast mechanisms behind ALT-803. The enhanced therapeutic index seen with BCG and ALT-803, administered SQ or intravesically, provides a powerful justification for the further development of these regimens.

Published in Journal of Translational Medicine

ISSN: 1479-5876 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://translational-medicine.biomedcentral.com/

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