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iRGD-modified exosomes-delivered BCL6 siRNA inhibit the progression of diffuse large B-cell lymphoma

Qinhua Liu, Dai Guanrong, Yi Wu, Mingxia Zhang, Mingya Yang, Xiaonan Wang, Mingyue Song, Xiaodan Li, Ruixiang Xia, Zhengsheng Wu

2022Frontiers in Oncology38 citationsDOIOpen Access PDF

Abstract

Clinical applications of siRNA therapeutics have been limited by the immunogenicity of the siRNA and low efficiency of siRNA delivery to target cells. Recently, evidence have shown that exosomes, endogenous nano-vesicles, can deliver siRNA to the tumor tissues in mice. Here, to reduce immunogenicity, we selected immature dendritic cells (DCs) to produce exosomes. In addition, tumor targeting was achieved by engineering the DCs to express exosomal membrane protein (Lamp2b), fused to av integrin-specific iRGD peptide (CRGDKGPDC). Next, iRGD targeted exosomes (iRGD-Exo) were isolated from the transfected DCs, and then the isolated exosomes were loaded with BCL6 siRNA by electroporation. Our results found that integrin (αvβ3) receptors were highly expressed on OCI-Ly8 cells. In addition, iRGD-Exo showed high targeting ability with avβ3 integrins positive OCI-Ly8 cells. Significantly, iRGD-Exo loaded with BCL6 siRNA suppressed DLBCL cell proliferation in vitro . Furthermore, intravenously injected iRGD-Exo delivered BCL6 siRNA to tumor tissues, resulting in inhibition of tumor growth in DLBCL. Meanwhile, exosomes mediated BCL6 siRNA delivery did not exhibit appreciable toxicity in mice. Collectively, our study demonstrates a therapeutic potential of exosomes as a promising vehicle for RNAi delivery to treat DLBCL.

Topics & Concepts

MicrovesiclesCancer researchSmall interfering RNATransfectionImmunogenicityChemistryExosomeBCL6Cell biologyBiologyCell cultureImmune systemImmunologymicroRNAB cellBiochemistryAntibodyGeneGeneticsGerminal centerExtracellular vesicles in diseaseRNA Interference and Gene DeliveryImmunotherapy and Immune Responses