Litcius/Paper detail

Physical- and Chemical-Dually ROS-Responsive Nano-in-Gel Platforms with Sequential Release of OX40 Agonist and PD-1 Inhibitor for Augmented Combination Immunotherapy

Yu Fu, Yulan Huang, Pingrong Li, Luyao Wang, Zhongjie Tang, Xinlong Liu, Xufei Bian, Shuang Wu, Xiaoyou Wang, Biyue Zhu, Yang Yu, Jiayun Jiang, Chong Li

2023Nano Letters11 citationsDOI

Abstract

Combination immunotherapy synergizing the PD-1 blockade with OX40 agonism has become a research hotspot, due to its enormous potential to overcome the restricted clinical objective response suffered by monotherapy. Questions of timing and sequence have been important aspects of immunotherapies when considering immunologic mechanisms; however, most of the time the straightforward additive approach was taken. Herein, our work is the first to investigate an alternative timing of aOX40 and aPD-1 treatment in melanoma-bearing mice, and it demonstrates that sequential administration (aOX40 first, then aPD-1 following) provided superior antitumor benefits than concurrent treatment. Based on that, to further avoid the limits suffered by solution forms, we adopted pharmaceutical technologies to construct an in situ -formed physical- and chemical-dually ROS-responsive nano-in-gel platform to implement sequential and prolonged release of aPD-1 and aOX40. Equipped with these advantages, the as-prepared (aPD-1NCs&aOX40)@Gels elicited augmented combination immunity and achieved great eradication of both primary and distant melanoma tumors in vivo .

Topics & Concepts

ImmunotherapyAgonistMelanomaIn vivoPharmacologyMedicineCancer researchImmune systemImmunologyInternal medicineBiologyReceptorBiotechnologyNanoplatforms for cancer theranosticsImmunotherapy and Immune ResponsesPeptidase Inhibition and Analysis