Dual-Action Protein-siRNA Conjugates for Targeted Disruption of CD47-Signal Regulatory Protein α Axis in Cancer Therapy

Authors
Lee, Jong WonYoon, Hong YeolKo, Young JiKim, Eun HyeSong, SukyungHue, SeungmiGupta, NilakshMalin, DmitryKim, JayKong, ByoungjaeKim, SehoonKim, In-SanKwon, Ick ChanYang, YoosooKim, Sun Hwa
Issue Date
2024-08
Publisher
American Chemical Society
Citation
ACS Nano, v.18, no.33, pp.22298 - 22315
Abstract
A series of successes in RNA interference (RNAi) therapies for liver diseases using lipid nanoparticles and N-acetylgalactosamine have heralded a current era of RNA therapeutics. However, alternative delivery strategies are required to take RNAi out of the comfort zone of hepatocytes. Here we report SIRP alpha IgV/anti-CD47 siRNA (vS-siCD47) conjugates that selectively and persistently disrupt the antiphagocytic CD47/SIRP alpha axis in solid tumors. Conjugation of the SIRP alpha IgV domain protein to siRNAs enables tumor dash through CD47-mediated erythrocyte piggyback, primarily blocking the physical interaction between CD47 on cancer cells and SIRP alpha on phagocytes. After internalization of the vS-siCD47 conjugates within cancer cells, the detached free-standing anti-CD47 siRNAs subsequently attack CD47 through the RNAi mechanism. The dual-action approach of the vS-siCD47 conjugate effectively overcomes the "don't eat me" barrier and stimulates phagocyte-mediated tumor destruction, demonstrating a highly selective and potent CD47-blocking immunotherapy. This delivery strategy, employing IgV domain protein-siRNA conjugates with a dual mode of target suppression, holds promise for expanding RNAi applications beyond hepatocytes and advancing RNAi-based cancer immunotherapies for solid tumors.
Keywords
IMMUNE CHECKPOINT BLOCKADE; CD47; DELIVERY; PHARMACOKINETICS; RNA interference; siRNA delivery; protein-RNAbioconjugate; RBC-hitchhiking; cancer immunotherapy
ISSN
1936-0851
URI
https://pubs.kist.re.kr/handle/201004/150475
DOI
10.1021/acsnano.4c06471
Appears in Collections:
KIST Article > 2024
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