Meeting
2017 ASCO Annual Meeting
Effect of a novel IL-2 cytokine immune agonist (NKTR-214) on proliferating CD8+T cells and PD-1 expression on immune cells in the tumor microenvironment in patients with prior checkpoint therapy.
Authors
Chantale Bernatchez
The University of Texas MD Anderson Cancer Center, Houston, TX
Chantale Bernatchez , Cara L. Haymaker , Michael E. Hurwitz , Harriet M. Kluger , Michael T. Tetzlaff , Natalie Jackson , Ivan Gergel , Mary Ann Tagliaferri , Jonathan Zalevsky , Ute Hoch , Christie Fanton , Ernesto Iacucci , Sandra Aung , Michael Imperiale , Ej Liao , Salah E Bentebibel , Nizar M. Tannir , Patrick Hwu , Mario Sznol , Adi Diab
Organizations
The University of Texas MD Anderson Cancer Center, Houston, TX, Yale School of Medicine, New Haven, CT, MD Anderson Cancer Center, Houston, TX, Nektar Therapeutics, San Francisco, CA, Kanglaite Inc., San Anselmo, CA, Yale School of Medicine and Yale Cancer Center, New Haven, CT
Research Funding
Pharmaceutical/Biotech Company
Background: NKTR-214 is a CD122-biased agonist designed to provide sustained signaling through the heterodimeric IL-2 receptor pathway (IL-2Rβɣ) to preferentially activate and expand effector CD8+ T and NK cells over T regulatory cells in the tumor microenvironment. Immune changes in the tumor microenvironment after NKTR-214 treatment was assessed in patients with locally advanced or metastatic solid tumors. Methods: NKTR-214 was administered IV in an outpatient setting q2w or q3w. Serial blood and tumor tissue samples were collected to measure immune activation using immunophenotyping including flow cytometry, immunohistochemistry (IHC), T cell clonality and gene expression analyses. Results: 26 patients (pts) have been treated with NKTR-214 at q3w, 4@0.003, 9@0.006, 6@0.009 and 1@0.012 mg/kg. Six pts received 0.006 mg/kg q2w. 58% of pts had prior immunotherapy. The most common Gr1-2 TRAEs were fatigue (73%) and pruritus (65%), and decreased appetite (46%). One pt experienced Gr3 syncope and hypotension at the highest dose tested and continued treatment at a lower dose. No drug-related AEs led to study discontinuation. No immune-related AEs or capillary leak syndrome were observed. 6 pts (23%) experienced tumor shrinkage from 10-30%. Three immunotherapy naïve pts receiving sequential anti-PD1 therapy, after ending treatment with NKTR-214, experienced significant tumor regression at first scan. In all pts evaluated, blood samples showed increases in newly proliferating (Ki67+) T and NK cells 8 days post dose. Flow cytometry and/or IHC revealed an up to 10-fold increase from baseline in tumor CD8+T and NK cells in the tumor microenvironment, with minimal changes to Tregs. PD-1 expression increased 2-fold in TILs. Gene expression analysis of tumor tissue showed increases in several immune checkpoint genes, cytotoxic markers (IFNg, PRF1, and GZMB), as well as a dynamic change in T cell clonality. Conclusions: Based on a favorable safety profile and strong correlative biomarker data, a phase 1/2 trial combining NKTR-214 and nivolumab is currently enrolling. Clinical trial information: NCT02869295
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Abstract Details
Session Type
Poster Session
Session Title
Developmental Therapeutics—Clinical Pharmacology and Experimental Therapeutics
Track
Developmental Therapeutics and Translational Research
Sub Track
Immunoconjugates
Clinical Trial Registration Number
NCT02869295
Citation
J Clin Oncol 35, 2017 (suppl; abstr 2545)
DOI
10.1200/JCO.2017.35.15_suppl.2545
Abstract #
2545
Poster Bd #
37
Abstract Disclosures
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