Improvement of Therapeutic Effect via Inducing Non-Apoptotic Cell Death Using mRNA-Protection Nanocage

Authors
Kim, SeoyoungKim, SeongchanKim, SojinLee, Nan-EeLee, Soo-HwanKim, HyunkyungLee, Hyojin
Issue Date
2024-10
Publisher
Wiley-Blackwell
Citation
Advanced Healthcare Materials, v.13, no.27
Abstract
Necroptosis, a cell death mechanism with the characteristics of both apoptosis and necrosis, is proposed as a promising therapeutic approach for cancer therapy. Induction of necroptosis for cancer therapy may be possible through the regulation of the expression of a key factor gene receptor-interacting protein kinase-3 (RIPK3) via in vitro transcription (IVT) mRNA delivery. However, mRNA is susceptible to degradation and has a low delivery efficiency, which highlights the requirement of a proper delivery vehicle for intracellular delivery. Therefore, a new mRNA delivery system based on the nanostructured silica nanoparticles, termed mRNA-protective nanocage (mPN) has been developed. High-efficiency expression of RIPK3 and induction of necroptosis is achieved through delivery of RIPK3 IVT mRNA with mPN in vitro and in vivo models. Importantly, the mPN carrying RIPK3 mRNA distributed locally in tumors upon intravascular injection, and successfully induced necroptosis and immune cell infiltration, a hallmark of necroptosis. the suppression of tumor growth in a murine cancer model, demonstrating the synergistic effect of RIPK3 mRNA- and immune cell-mediated therapy is also observed. These findings suggest the potential for anticancer therapy through necroptosis induction and provide a strategy for the development of mRNA-based nanomedicine. This study develops a nanocage-based mRNA delivery platform to induce necroptosis, non-apoptotic cell death. Delivery of necroptosis-induced mRNA using mRNA protective nanoparticles suppresses tumor growth and promotes immune cell infiltration in hepatocellular carcinoma. image
Keywords
NECROPTOSIS; DELIVERY; VACCINES; cancer therapy; in vitro transcription mRNA; mRNA-protective nanocage; necroptosis; receptor-interacting protein kinase-3
ISSN
2192-2640
URI
https://pubs.kist.re.kr/handle/201004/150393
DOI
10.1002/adhm.202400240
Appears in Collections:
KIST Article > 2024
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