Systemic Delivery of a STING Agonist‐Loaded Positively Charged Liposome Selectively Targets Tumor Immune Microenvironment and Suppresses Tumor Angiogenesis

Author:

Go Eun‐Jin12ORCID,Yang Hannah12ORCID,Park Wooram3ORCID,Lee Seung Joon12,Han Jun‐Hyeok3,Kong So Jung12,Lee Won Suk12ORCID,Han Dong Keun4ORCID,Chon Hong Jae12ORCID,Kim Chan12ORCID

Affiliation:

1. Medical Oncology CHA Bundang Medical Center CHA University School of Medicine Seongnam Gyeonggi 13496 Republic of Korea

2. Laboratory of Translational Immuno‐Oncology CHA University School of Medicine Seongnam Gyeonggi 13496 Republic of Korea

3. Department of Integrative Biotechnology College of Biotechnology and Bioengineering Sungkyunkwan University Seoburo 2066 Suwon Gyeonggi 16419 Republic of Korea

4. Department of Biomedical Science CHA University Seongnam Gyeonggi 13496 Republic of Korea

Abstract

AbstractAlthough stimulator of interferon genes (STING) agonists has shown great promise in preclinical studies, the clinical development of STING agonist therapy is challenged by its limited systemic delivery. Here, positively charged fusogenic liposomes loaded with a STING agonist (PoSTING) are designed for systemic delivery and to preferentially target the tumor microenvironment. When PoSTING is administered intravenously, it selectively targets not only tumor cells but also immune and tumor endothelial cells (ECs). In particular, delivery of STING agonists to tumor ECs normalizes abnormal tumor vasculatures, induces intratumoral STING activation, and elicits robust anti‐tumor T cell immunity within the tumor microenvironment. Therefore, PoSTING can be used as a systemic delivery platform to overcome the limitations of using STING agonists in clinical trials.

Funder

National Research Foundation of Korea

Publisher

Wiley

Subject

Biomaterials,Biotechnology,General Materials Science,General Chemistry

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