Abstract

The NF-KB signaling pathway represents an attractive therapeutic target for chronic inflammation as it regulates many gene products that control the inflammatory response. However, generalized suppression of this pathway can result in serious host toxicity, as NF-KB is a major mediator of both innate and adaptive immunity. We have formulated, characterized, and evaluated a novel peptide-siRNA construct that is self-condensing, stable in serum, and delivers oligonucleotides to the cell cytoplasm with an intrinsic endosomal releasing mechanism based on a modified version of the amphipathic cationic peptide melittin, a component of bee venom that normally forms pores in membrane by oligomerization. We showed that the modified melittin could be conjugated to myriad cargos and transport materials rapidly into the cell cytoplasm for efficient gene silencing: The peptide-siRNA complexes targeting the NF-KB p65 canonical subunit homed to the inflamed paws through leaky vasculature and potently suppressed ongoing inflammation in a murine model of RA. Extensive in vivo and ex vivo studies also suggest that the platform has a favorable toxicity profile and did not elicit immunogenicity after repeated dosing. In this proposal we will use the peptide-siRNA platform to explore the hypothesis that a dual approach (targeting both NF-KB canonical and non-canonical pathways) will have synergistic or additive benefits in the treatment of RA. To that end we will formulate and optimize peptide- siRNA constructs containing NF-KB-p65 (canonical), p52/100 (non-canonical), or a combination of both and test their efficiency for NF-KB signaling pathway knockdown in vitro in human/murine cell lines and in vivo in two murine models of inflammatory arthritis. The results will provide in vivo proof-of-concept for this new peptide- siRNA platform and the success will justify further development of this system for other disease processes that are amenable to RNA interference therapy.

Public Health Relevance

Rheumatoid arthritis is a chronic inflammatory disease affecting 1% of the general population. Unabated the disease often leads to severe joint destruction and other morbidities. Despite recent advances, a large number of patients fail to respond to existing therapeutics or stop responding to them altogether. In addition, systemic side effects often limit the use of many therapies. In this proposal, we propose to develop new nanomedicines that can safely modulate the inflammation in the host and preserve joint integrity without compromising the immune system.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR067491-04
Application #
9458102
Study Section
Nanotechnology Study Section (NANO)
Program Officer
Mao, Su-Yau
Project Start
2015-04-01
Project End
2020-03-31
Budget Start
2018-04-01
Budget End
2019-03-31
Support Year
4
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Moore, Jeremy K; Chen, Junjie; Pan, Hua et al. (2018) Quantification of vascular damage in acute kidney injury with fluorine magnetic resonance imaging and spectroscopy. Magn Reson Med 79:3144-3153
Kabir, Ashraf Ul; Lee, Tae-Jin; Pan, Hua et al. (2018) Requisite endothelial reactivation and effective siRNA nanoparticle targeting of Etv2/Er71 in tumor angiogenesis. JCI Insight 3:
Pan, Hua; Palekar, Rohun U; Hou, Kirk K et al. (2018) Anti-JNK2 peptide-siRNA nanostructures improve plaque endothelium and reduce thrombotic risk in atherosclerotic mice. Int J Nanomedicine 13:5187-5205
Wu, Xiaobo; Hutson, Irina; Akk, Antonina M et al. (2018) Contribution of Adipose-Derived Factor D/Adipsin to Complement Alternative Pathway Activation: Lessons from Lipodystrophy. J Immunol 200:2786-2797
Rai, Muhammad Farooq; Pham, Christine Tn (2018) Intra-articular drug delivery systems for joint diseases. Curr Opin Pharmacol 40:67-73
Dai, Rujuan; Cowan, Catharine; Heid, Bettina et al. (2017) Neutrophils and neutrophil serine proteases are increased in the spleens of estrogen-treated C57BL/6 mice and several strains of spontaneous lupus-prone mice. PLoS One 12:e0172105
Hourcade, Dennis E; Akk, Antonina M; Mitchell, Lynne M et al. (2016) Anti-complement activity of the Ixodes scapularis salivary protein Salp20. Mol Immunol 69:62-9
Toonen, Erik J M; Mirea, Andreea-Manuela; Tack, Cees J et al. (2016) Activation of proteinase 3 contributes to Non-alcoholic Fatty Liver Disease (NAFLD) and insulin resistance. Mol Med 22:
Ortega-Gomez, Almudena; Salvermoser, Melanie; Rossaint, Jan et al. (2016) Cathepsin G Controls Arterial But Not Venular Myeloid Cell Recruitment. Circulation 134:1176-1188
Esser, Alison K; Schmieder, Anne H; Ross, Michael H et al. (2016) Dual-therapy with ?v?3-targeted Sn2 lipase-labile fumagillin-prodrug nanoparticles and zoledronic acid in the Vx2 rabbit tumor model. Nanomedicine 12:201-11

Showing the most recent 10 out of 23 publications