Literature DB >> 29578946

Bivalent ligand MCC22 potently attenuates nociception in a murine model of sickle cell disease.

Giuseppe Cataldo1, Mary M Lunzer2, Julie K Olson1, Eyup Akgün2, John D Belcher3, Gregory M Vercellotti3, Philip S Portoghese2, Donald A Simone1.   

Abstract

Sickle cell disease (SCD) is a chronic inflammatory disorder accompanied by chronic pain. In addition to ongoing pain and hyperalgesia, vaso-occlusive crises-induced pain can be chronic or episodic. Because analgesics typically used to treat pain are not very effective in SCD, opioids, including morphine, are a primary treatment for managing pain in SCD but are associated with many serious side effects, including constipation, tolerance, addiction, and respiratory depression. Thus, there is a need for the development of novel treatments for pain in SCD. In this study, we used the Townes transgenic mouse model of SCD to investigate the antinociceptive efficacy of the bivalent ligand, MCC22, and compared its effectiveness with morphine. MCC22 consists of a mu-opioid receptor agonist and a chemokine receptor-5 (CCR5) antagonist that are linked through a 22-atom spacer. Our results show that intraperitoneal administration of MCC22 produced exceptionally potent dose-dependent antihyperalgesia as compared to morphine, dramatically decreased evoked responses of nociceptive dorsal horn neurons, and decreased expression of proinflammatory cytokines in the spinal cord. Moreover, tolerance did not develop to its analgesic effects after repeated administration. In view of the extraordinary potency of MCC22 without tolerance, MCC22 and similar compounds may vastly improve the management of pain associated with SCD.

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Year:  2018        PMID: 29578946      PMCID: PMC6008209          DOI: 10.1097/j.pain.0000000000001225

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


  77 in total

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6.  Transient receptor potential vanilloid 1 mediates pain in mice with severe sickle cell disease.

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Journal:  ACS Chem Neurosci       Date:  2017-07-26       Impact factor: 4.418

8.  Sensitization of nociceptive spinal neurons contributes to pain in a transgenic model of sickle cell disease.

Authors:  Giuseppe Cataldo; Sugandha Rajput; Kalpna Gupta; Donald A Simone
Journal:  Pain       Date:  2015-04       Impact factor: 7.926

Review 9.  Role of TNF-alpha during central sensitization in preclinical studies.

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10.  Controlling neuropathic pain by adeno-associated virus driven production of the anti-inflammatory cytokine, interleukin-10.

Authors:  Erin D Milligan; Evan M Sloane; Stephen J Langer; Pedro E Cruz; Marucia Chacur; Leah Spataro; Julie Wieseler-Frank; Sayamwong E Hammack; Steven F Maier; Terence R Flotte; John R Forsayeth; Leslie A Leinwand; Raymond Chavez; Linda R Watkins
Journal:  Mol Pain       Date:  2005-02-25       Impact factor: 3.395

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  4 in total

1.  The bivalent ligand MCC22 potently attenuates hyperalgesia in a mouse model of cisplatin-evoked neuropathic pain without tolerance or reward.

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Journal:  Neuropharmacology       Date:  2019-04-07       Impact factor: 5.250

2.  End points for sickle cell disease clinical trials: patient-reported outcomes, pain, and the brain.

Authors:  Ann T Farrell; Julie Panepinto; C Patrick Carroll; Deepika S Darbari; Ankit A Desai; Allison A King; Robert J Adams; Tabitha D Barber; Amanda M Brandow; Michael R DeBaun; Manus J Donahue; Kalpna Gupta; Jane S Hankins; Michelle Kameka; Fenella J Kirkham; Harvey Luksenburg; Shirley Miller; Patricia Ann Oneal; David C Rees; Rosanna Setse; Vivien A Sheehan; John Strouse; Cheryl L Stucky; Ellen M Werner; John C Wood; William T Zempsky
Journal:  Blood Adv       Date:  2019-12-10

3.  Children and adolescents with sickle cell disease have worse cold and mechanical hypersensitivity during acute painful events.

Authors:  Amanda M Brandow; Karla Hansen; Melodee Nugent; Amy Pan; Julie A Panepinto; Cheryl L Stucky
Journal:  Pain       Date:  2019-02       Impact factor: 7.926

Review 4.  Targeting Chemokines and Chemokine GPCRs to Enhance Strong Opioid Efficacy in Neuropathic Pain.

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  4 in total

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