PDL1-binding peptide/anti-miRNA21 conjugate as a therapeutic modality for PD-L1high tumors and TAMs

Authors
Kim, Eun HyeLee, JongwonKwak, GijungJang, HochungKim, HyosukCho, HaeunJang, YeongjiChoi, JiwoongChi, Sung GilKim, KwangmeyungKwon, Ick ChanYang, YoosooKim, Sun Hwa
Issue Date
2022-05
Publisher
Elsevier BV
Citation
Journal of Controlled Release, v.345, pp.62 - 74
Abstract
Upregulation of oncogenic miRNA21 (miR-21) plays a pivotal role in proliferation, migration and invasion of cancer cells. In addition to cancer cells, tumor-associated macrophages (TAMs) also have high abundance of miR21, which accelerates malignant progression of tumors in the late stages of carcinogenesis. Despite of the protumorigenic functions of miR-21 in TAMs and cancer cells, reliable therapeutic strategies to simultaneously inhibit miR-21 activity in both types of cell have not yet been developed. In this study, we designed a dualtargeting drug delivery system of miR-21 inhibitors that could bind to both tumor cells and macrophages with overexpressed PD-L1 receptors. This peptide-oligonucleotide conjugate (Pep-21) consists of a PDL1-binding peptide covalently linked with an anti-miR-21 inhibitor via click chemistry. Pep-21 was preferentially internalized in both cell types, consequently depleting endogenous miR-21. Our studies found that Pep-21 treatment reduced tumor cell migration, reprogrammed immunosuppressive M2-type TAMs into M1-type macrophages, and restrained tumor progression. Collectively, neutralization of miR-21 activity in both cancer cells and TAMs can be a promising strategy for effective antitumor responses.
Keywords
IN-VIVO; CANCER; MICRORNAS; OLIGONUCLEOTIDES; anti-miRNA delivery; PD-L1; miR-21; B16 melanoma; Tumor-associated macrophage
ISSN
0168-3659
URI
https://pubs.kist.re.kr/handle/201004/115232
DOI
10.1016/j.jconrel.2022.02.031
Appears in Collections:
KIST Article > 2022
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