Enhancing CAR‐NK Cells Against Solid Tumors Through Chemical and Genetic Fortification with DOTAP‐Functionalized Lipid Nanoparticles

Author:

Shin Ha Eun1,Han Jun‐Hyeok12,Park Joo Dong1,Park Minji3,Han Jieun14,Kang Min‐Ho5,Lee Jung Seung267,Park Chun Gwon268,Park Juwon9,Kim Hyun‐Young10,Cho Duck31011,Park Wooram1478ORCID

Affiliation:

1. Department of Integrative Biotechnology College of Biotechnology and Bioengineering Sungkyunkwan University (SKKU) Seobu‐ro 2066, Jangan‐gu Suwon Gyeonggi 16419 Republic of Korea

2. Department of Intelligent Precision Healthcare Convergence SKKU Institute for Convergence SKKU Seobu‐ro 2066, Jangan‐gu Suwon Gyeonggi 16419 Republic of Korea

3. Department of Health Sciences and Technology Samsung Advanced Institute for Health Sciences and Technology (SAIHST) SKKU 115 Irwon‐ro, Gangnam‐gu Seoul 06355 Republic of Korea

4. Institute of Biotechnology and Bioengineering College of Biotechnology and Bioengineering SKKU Seobu‐ro 2066 Suwon Gyeonggi 16419 Republic of Korea

5. Biomedical and Chemical Engineering Department of Biotechnology The Catholic University of Korea 43 Jibong‐ro, Wonmi‐gu Bucheon Gyeonggi 14662 Republic of Korea

6. Department of Biomedical Engineering SKKU Seobu‐ro 2066, Jangan‐gu Suwon Gyeonggi 16419 Republic of Korea

7. Department of MetaBioHealth SKKU Institute for Convergence SKKU Seobu‐ro 2066, Jangan‐gu Suwon Gyeonggi 16419 Republic of Korea

8. Korea Institute of Science and Technology (KIST) 5 Hwarang‐ro 14‐gil, Seongbuk‐g Seoul 02792 Republic of Korea

9. Department of Tropical Medicine Medical Microbiology and Pharmacology John A. Burns School Medicine University of Hawai'i at Manoa Honolulu 96813 USA

10. Department of Laboratory Medicine and Genetics Samsung Medical Center SKKU School of Medicine SKKU 115 Irwon‐ro, Gangnam‐gu Seoul 06351 Republic of Korea

11. Department of Biopharmaceutical Convergence SKKU Seobu‐ro 2066, Jangan‐gu Suwon Gyeonggi 16419 Republic of Korea

Abstract

AbstractNatural killer (NK) cells are crucial in the innate immune response and show promise in cancer immunotherapy, but face challenges in activation and targeted gene delivery. In this study, bifunctional lipid nanoparticles (DLNPs) containing 1,2‐dioleoyl‐3‐trimethylammonium‐propane (DOTAP), designed to bolster the antitumor efficacy of chimeric antigen receptor‐modified NK (CAR‐NK) cells by facilitating activation and efficient CAR mRNA delivery are introduced. The DLNPs, created by functionalizing FDA‐approved LNP compositions, exhibit excellent mRNA encapsulation and colloidal stability. NK cells primed with DLNPs show increased cytotoxicity against cancer cells via extracellular signal‐regulated kinase/Mitogen‐Activated Protein Kinase pathway modulation and mitochondrial dynamics changes. The DLNPs enter NK cells predominantly through clathrin‐mediated endocytosis, boosting mRNA delivery and overcoming NK cells' resistance to genetic manipulation. CAR‐NK cells targeting glypican‐3, prevalent in hepatocellular carcinoma, show significant therapeutic effects in an orthotopic mouse model. These findings underscore the potential of DLNPs in enhancing CAR‐NK cell therapy for solid tumors, marking a significant stride in NK cell‐based cancer immunotherapy and broadening prospects for NK cell‐related disease interventions.

Funder

National Research Foundation of Korea

Korea Health Industry Development Institute

Publisher

Wiley

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