2011
DOI: 10.1021/cb200176v
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Humanized Lewis-Y Specific Antibody Based Delivery of STAT3 siRNA

Abstract: The clinical application of siRNA is limited largely by the lack of efficient, cell-specific delivery systems. Antibodies are attractive delivery vehicles for targeted therapy due to their high specificity. In this study we describe the use of a humanized monoclonal antibody (mAb), hu3S193, against Lewis-Y (Ley), as a delivery vehicle for STAT3 siRNA. This mAb is rapidly internalized into Ley expressing cancer cells via antigen recognition, and when coupled to STAT3 siRNA, a potentially powerful molecularly ta… Show more

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Cited by 41 publications
(35 citation statements)
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“…Previously developed siRNA-delivery strategies used antibodies, oligonucleotides, or RNA aptamers specific to surface receptors on tumor cells. 16,36,42 In contrast, our approach used a ligand to intracellular TLR9 receptor that is ubiquitously expressed in B-cell malignancies and AML. [25][26][27] Dicer RNase, which is critical for uncoupling of CpG-siRNA conjugates, is also commonly expressed in normal and transformed B cells and in the majority of clinical AML samples.…”
Section: Discussionmentioning
confidence: 99%
See 1 more Smart Citation
“…Previously developed siRNA-delivery strategies used antibodies, oligonucleotides, or RNA aptamers specific to surface receptors on tumor cells. 16,36,42 In contrast, our approach used a ligand to intracellular TLR9 receptor that is ubiquitously expressed in B-cell malignancies and AML. [25][26][27] Dicer RNase, which is critical for uncoupling of CpG-siRNA conjugates, is also commonly expressed in normal and transformed B cells and in the majority of clinical AML samples.…”
Section: Discussionmentioning
confidence: 99%
“…For the design of the human cell-specific CpG-siRNA (Figure 2A), we used a 25/27mer Dicersubstrate STAT3 siRNA selected from more than 20 sequences based on the high silencing efficacy (Ͼ 95%). 36 The 25/27mer siRNA sequence was selected to enable intracellular uncoupling of both parts of the molecule by Dicer endonuclease. 20 We conjugated STAT3 siRNA to both type-B (CpG7909) and type-A (D19) CpG-ODNs.…”
Section: Cpg(a)-sirna-mediated Target Gene Silencing In Human Immune mentioning
confidence: 99%
“…Monoclonal antibodies targeted against specific cell types can also be used to deliver siRNAs enclosed in liposomes. A recent study has utilized humanized Lewis-Y monoclonal antibody to selectively deliver STAT3 siRNA to Lewis-Y protein expressing cancer cells via antigen recognition (171). Pirollo and colleagues employed cationic immunoliposomes decorated with antitransferrin receptor antibody.…”
Section: Bioconjugationmentioning
confidence: 99%
“…A variety of linkages have been used to conjugate ligands and ONs including amide, thioether, thiol-maleimide, ester, and disulfide [23, 28, 29]. Some linkages are readily cleavable inside the cells, including disulfide, some peptides, and hydrazone, and they are needed to attain biological activity of ONs when large ligands such as antibody [30] or carrier proteins such as albumin [31] are linked the ONs.…”
Section: Molecular Conjugatesmentioning
confidence: 99%
“…This approach of direct conjugation has been extended to ON delivery; however, direct antibody-ONs conjugates haven't accomplished similar success as antibody-drug conjugates. In one study, a humanized monoclonal antibody was linked to siRNA via a reductive disulfide bond that is cleavable within cells [30]. Although antigen-specific binding and internalization of the antibody-ON conjugates were observed, single treatment of the conjugates failed to produce significant gene silencing.…”
Section: Molecular Conjugatesmentioning
confidence: 99%