Tion on CD8 T Cells and NK Cells Tanya Robinson, PhD1, Shweta Hegde, Investigation Assistant1, Sarai Rivas, BS1, Takahiro Miyazaki, MS2, Kimberly S. Schluns, PhD1 1 University of Texas MD Anderson Cancer Center, Houston, TX, USA; two Nektar Therapeutics, San Francisco, CA, USA Correspondence: Tanya Robinson ([email protected]); Kimberly S. Schluns Journal for ImmunoTherapy of Cancer 2018, 6(Suppl 1):P422 Background IL-15 has anti-tumor activity but with restricted efficacy as a result of its unfavorable pharmacokinetic properties and tolerability. Nektar Therapeutics has Dual-Specificity Phosphatase 1 (DUSP1) Proteins Storage & Stability developed a polymer-conjugated human IL-15 (NKTR255) that exhibits a prolonged in vivo half-life and enhanced potency, which can be currently getting examined as a prospective cancer immunotherapeutic agent. Because responses by IL-15 is often mediated by transpresentation via the IL-15R, as soluble IL-15/IL-15R complexes, or by cis-presentation, we investigated the part of IL-15R in driving NKTR-255 responses by na e and memory CD8 T cells and NK cells in mice. Techniques The effects of NKTR-255 were examined by the adoptive transfer of CFSE-labeled na e ovalbumin-specific CD8 T cells (OT-I) orestablished memory OT-I T cells followed by systemic administration of NKTR-255. To assess responses by central and effector memory T cell subsets, sorted CD44hi memory phenotype CD8 T cells had been transferred into wild-type (Wt) recipients followed by NKTR-255 treatment. Moreover, NK cell responses to NKTR-255 had been analyzed in IL-15R bone marrow (BM) chimeras by BrdU incorporation. Outcomes Na e CD8 OT-I T cells transferred into Wt and IL-15R-/- mice proliferated at equivalent levels and acquired a central memory phenotype in response to NKTR-255. Interestingly, naive IL-15R-/- OT-I T cells had a deficient response to NKTR-255 but to not rhIL-15 or soluble IL-15 complexes. Additionally, proliferation by memory IL-15R-/- OT- I T cells in response to NKTR-255 was partially impaired in comparison with Wt OT-I cells. Sorted memory CD8 T cells maintained their proportion of CD62L+ and – subsets following NKTR-255-stimulated proliferation. Considering that IL-15R expression is crucial for NK cell improvement, BM chimeras had been generated with either IL-15R-/- or Wt BM in Wt recipients. In this model system, comparable levels of BrdU had been incorporated in IL15R-/- and Wt NK cells immediately after therapy with NKTR-255. Conclusions These PTPN2 Proteins Source findings suggest naive CD8 T cells are critically dependent on cis-presentation of NKTR-255, whilst memory CD8 T cells are only partially dependent. For both naive or memory CD8 T cells, transpresentation of NKTR-255 was not needed. In contrast to CD8 T cells, NK cell responses to NKTR-255 usually are not dependent on cis-presentation. All round, these findings highlight the prospective of polymerized IL-15 to modify IL-15R dependency leading to unique mechanisms of action on CD8 T cells and NK cells and one of a kind therapeutic effects. Ethics Approval All animal procedures have been conducted in accordance using the animal care and use protocols (00000851-RN01) approved by the IACUC at the UT MD Anderson Cancer Center.P423 Security, pharmacokinetics and pharmacodynamic effects of ALKS 4230 in sufferers with sophisticated strong tumors from the ongoing dose escalation portion of a initial in human (FIH) study Ulka Vaishampayan, MD1, Vamsidhar Velcheti, MD FACP2, David McDermott, MD3, Mayer Fishman, MD, PhD4, Chris Hoimes, MD5, Daniel Cho, MD6, Lei Sun, Ph.D7, Juan Alvarez, PhD8, Heather Losey, PhD7, Rose Marino, MD7, Emily Putiri, PhD7, Sean R.