Literature DB >> 28092646

Ex vivo nonviral gene delivery of μ-opioid receptor to attenuate cancer-induced pain.

Seiichi Yamano1, Chi T Viet2,3, Dongmin Dang2,3, Jisen Dai1, Shigeru Hanatani1, Tadahiro Takayama1, Hironori Kasai1, Kentaro Imamura1, Ron Campbell2,3, Yi Ye2,3, John C Dolan2,3, William Myung Kwon2,3, Stefan D Schneider2,3, Brian L Schmidt2,3.   

Abstract

Virus-mediated gene delivery shows promise for the treatment of chronic pain. However, viral vectors have cytotoxicity. To avoid toxicities and limitations of virus-mediated gene delivery, we developed a novel nonviral hybrid vector: HIV-1 Tat peptide sequence modified with histidine and cysteine residues combined with a cationic lipid. The vector has high transfection efficiency with little cytotoxicity in cancer cell lines including HSC-3 (human tongue squamous cell carcinoma) and exhibits differential expression in HSC-3 (∼45-fold) relative to HGF-1 (human gingival fibroblasts) cells. We used the nonviral vector to transfect cancer with OPRM1, the μ-opioid receptor gene, as a novel method for treating cancer-induced pain. After HSC-3 cells were transfected with OPRM1, a cancer mouse model was created by inoculating the transfected HSC-3 cells into the hind paw or tongue of athymic mice to determine the analgesic potential of OPRM1 transfection. Mice with HSC-3 tumors expressing OPRM1 demonstrated significant antinociception compared with control mice. The effect was reversible with local naloxone administration. We quantified β-endorphin secretion from HSC-3 cells and showed that HSC-3 cells transfected with OPRM1 secreted significantly more β-endorphin than control HSC-3 cells. These findings indicate that nonviral delivery of the OPRM1 gene targeted to the cancer microenvironment has an analgesic effect in a preclinical cancer model, and nonviral gene delivery is a potential treatment for cancer pain.

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Year:  2017        PMID: 28092646      PMCID: PMC5584564          DOI: 10.1097/j.pain.0000000000000750

Source DB:  PubMed          Journal:  Pain        ISSN: 0304-3959            Impact factor:   7.926


  59 in total

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Authors:  K Hargreaves; R Dubner; F Brown; C Flores; J Joris
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Review 4.  Non-viral gene transfer: applications in developmental biology and gene therapy.

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5.  Modified Tat peptide with cationic lipids enhances gene transfection efficiency via temperature-dependent and caveolae-mediated endocytosis.

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7.  Repeated intrathecal administration of plasmid DNA complexed with polyethylene glycol-grafted polyethylenimine led to prolonged transgene expression in the spinal cord.

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  10 in total

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6.  Neutrophil-Mediated Endogenous Analgesia Contributes to Sex Differences in Oral Cancer Pain.

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7.  Targeting the endothelin axis as a therapeutic strategy for oral cancer metastasis and pain.

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8.  Cathepsin S Evokes PAR2-Dependent Pain in Oral Squamous Cell Carcinoma Patients and Preclinical Mouse Models.

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9.  Cell-penetrating Peptide-modified Targeted Drug-loaded Phase-transformation Lipid Nanoparticles Combined with Low-intensity Focused Ultrasound for Precision Theranostics against Hepatocellular Carcinoma.

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  10 in total

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