Literature DB >> 30702897

The Development of a Macromolecular Analgesic for Arthritic Pain.

Laura Weber, Xiaobei Wang, Rongguo Ren, Xin Wei, Gang Zhao, Junxiao Yang, Hongjiang Yuan, Huiling Pang, Hanjun Wang, Dong Wang.   

Abstract

The addictive potential of clinically used opioids as a result of their direct action on the dopaminergic reward system in the brain has limited their application. In an attempt to reduce negative side effects as well as to improve the overall effectiveness of these analgesics, we have designed, synthesized, and evaluated an N-(2-hydroxypropyl)methacrylamide (HPMA)-based macromolecular prodrug of hydromorphone (HMP), a commonly used opioid. To this end, P-HMP was synthesized via RAFT polymerization and a subsequent polymer analogous reaction. Its interaction with inflammatory cells in arthritic joints was evaluated in vitro using a RAW 264.7 cell culture, and subsequent confocal microscopy analysis confirmed that P-HMP could be internalized by the cells via endocytosis. In vivo imaging studies indicated that the prodrug can passively target the arthritic joint after systemic administration in a rodent model of monoarticular adjuvant-induced arthritis (MAA). The inflammatory pain-alleviating properties of the prodrug were assessed in MAA rats using the incapacitance test and were observed to be similar to dose-equivalent HMP. Analgesia through mechanisms at the spinal cord level was further measured using the tail flick test, and it was determined that the prodrug significantly reduced spinal cord analgesia versus free HMP, further validating the peripheral restriction of the macromolecular prodrug. Immunohistochemical analysis of cellular uptake of the P-HMP within the MAA knee joint proved the internalization of the prodrug by phagocytic synoviocytes, colocalized with HMP's target receptor as well as with pain-modulating ion channels. Therefore, it can be concluded that the novel inflammation-targeting polymeric prodrug of HMP (P-HMP) has the potential to be developed as an effective and safe analgesic agent for musculoskeletal pain.

Entities:  

Keywords:  ELVIS mechanism; HPMA copolymer; analgesic; opioid; rheumatoid arthritis

Mesh:

Substances:

Year:  2019        PMID: 30702897      PMCID: PMC6413733          DOI: 10.1021/acs.molpharmaceut.8b01197

Source DB:  PubMed          Journal:  Mol Pharm        ISSN: 1543-8384            Impact factor:   4.939


  44 in total

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Review 3.  The role of opioids in cancer pain.

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Review 5.  Understanding opioid reward.

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Review 6.  Modulation of peripheral sensory neurons by the immune system: implications for pain therapy.

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8.  A pain research agenda for the 21st century.

Authors:  Robert W Gereau; Kathleen A Sluka; William Maixner; Seddon R Savage; Theodore J Price; Beth B Murinson; Mark D Sullivan; Roger B Fillingim
Journal:  J Pain       Date:  2014-10-29       Impact factor: 5.820

Review 9.  Diagnosis and Treatment of Inflammatory Joint Disease.

Authors:  Yeesuk Kim; Hyun-Cheol Oh; Jang Won Park; In-Sung Kim; Jun-Young Kim; Ki-Choul Kim; Dong-Sik Chae; Woo-Lam Jo; Joo-Hyoun Song
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10.  Intrathecal Trialing of Continuous Infusion Combination Therapy With Hydromorphone and Bupivacaine in Failed Back Surgery Patients.

Authors:  Ryan J Galica; Salim M Hayek; Elias Veizi; Matthew T McEwan; Sivakanth Katta; Omar Ali; Nida Aziz; Nidhi Sondhi
Journal:  Neuromodulation       Date:  2017-12-05
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  2 in total

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Journal:  J Control Release       Date:  2021-10-12       Impact factor: 9.776

2.  Triptolide and l-ascorbate palmitate co-loaded micelles for combination therapy of rheumatoid arthritis and side effect attenuation.

Authors:  Man Li; Guoqiang Wang; Yinyin Yan; Mengyuan Jiang; Zhirong Wang; Zhenqiang Zhang; Xiangxiang Wu; Huahui Zeng
Journal:  Drug Deliv       Date:  2022-12       Impact factor: 6.819

  2 in total

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