Literature DB >> 31069130

Order of administration of combination cytokine therapies can decouple toxicity from efficacy in syngeneic mouse tumor models.

Adrienne Rothschilds1,2, Alice Tzeng1,2, Naveen K Mehta1,2, Kelly D Moynihan1,2,3, Darrell J Irvine1,2,3,4,5, K Dane Wittrup1,2,6.   

Abstract

In combination cancer immunotherapies, consideration should be given to designing treatment schedules that harmonize with the immune system's natural timing. An efficacious temporally programmed combination therapy of extended half-life interleukin 2 (eIL2), tumor targeting antibody, and interferon (IFN) α was recently reported; however, tumor-ablative efficacy was associated with significant toxicity. In the current work, altering the order and timing of the three agents is shown to decouple toxicity from efficacy. Delaying the administration of eIL2 to be concurrent with or after IFNα eliminates toxicity without affecting efficacy in multiple syngeneic tumor models and mouse strains. The toxicity resulting from eIL2 administration before IFNα is dependent on multiple systemic inflammatory cytokines including IL6, IL10, IFNγ, and tumor necrosis factor α. Natural killer (NK) cells are the main cellular contributor to toxicity, but are not essential for tumor control in this system. When pre-conditioned with eIL2, splenic NK cells became hyper-activated and upregulate IFNα signaling proteins that cause an excessive, toxic response to subsequent IFNα exposure. This work illustrates an example where accounting for the temporal dynamics of the immune system in combination therapy treatment schedule can favorably decouple efficacy and toxicity.

Entities:  

Keywords:  Dose scheduling; cytokines; timing; toxicity

Year:  2019        PMID: 31069130      PMCID: PMC6492973          DOI: 10.1080/2162402X.2018.1558678

Source DB:  PubMed          Journal:  Oncoimmunology        ISSN: 2162-4011            Impact factor:   8.110


  60 in total

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7.  High- and low-dose interferon alfa-2b in high-risk melanoma: first analysis of intergroup trial E1690/S9111/C9190.

Authors:  J M Kirkwood; J G Ibrahim; V K Sondak; J Richards; L E Flaherty; M S Ernstoff; T J Smith; U Rao; M Steele; R H Blum
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Authors:  S A Rosenberg; J C Yang; D J Schwartzentruber; P Hwu; F M Marincola; S L Topalian; C A Seipp; J H Einhorn; D E White; S M Steinberg
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9.  High-dose interferon alfa-2b significantly prolongs relapse-free and overall survival compared with the GM2-KLH/QS-21 vaccine in patients with resected stage IIB-III melanoma: results of intergroup trial E1694/S9512/C509801.

Authors:  J M Kirkwood; J G Ibrahim; J A Sosman; V K Sondak; S S Agarwala; M S Ernstoff; U Rao
Journal:  J Clin Oncol       Date:  2001-05-01       Impact factor: 44.544

10.  Randomized study of high-dose and low-dose interleukin-2 in patients with metastatic renal cancer.

Authors:  James C Yang; Richard M Sherry; Seth M Steinberg; Suzanne L Topalian; Douglas J Schwartzentruber; Patrick Hwu; Claudia A Seipp; Linda Rogers-Freezer; Kathleen E Morton; Donald E White; David J Liewehr; Maria J Merino; Steven A Rosenberg
Journal:  J Clin Oncol       Date:  2003-08-15       Impact factor: 44.544

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Journal:  Mol Cancer Ther       Date:  2022-04-01       Impact factor: 6.009

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Review 5.  Improving cancer immunotherapy through nanotechnology.

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Authors:  Lawrence Fong; Michael J Morris; Andrew J Armstrong; Daniel P Petrylak; Oliver Sartor; Celestia S Higano; Lance Pagliaro; Ajjai Alva; Leonard J Appleman; Winston Tan; Ulka Vaishampayan; Raphaelle Porcu; Darren Tayama; Edward E Kadel; Kobe C Yuen; Asim Datye
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7.  Immuno-priming durvalumab with bevacizumab in HER2-negative advanced breast cancer: a pilot clinical trial.

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  7 in total

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