| Literature DB >> 28323403 |
Young-Hwan Jung1, Yeo Ok Kim, Hai Lin, Joong-Heui Cho2, Jin-Hee Park2, So-Deok Lee1, Jinsu Bae3, Koon Mook Kang1, Yoon-Gyoon Kim4, Ae Nim Pae5, Hyojin Ko1, Chul-Seung Park1, Myung Ha Yoon, Yong-Chul Kim1,3.
Abstract
Antagonism of the P2X3 receptor is one of the potential therapeutic strategies for the management of neuropathic pain because P2X3 receptors are predominantly localized on small to medium diameter C- and Aδ-fiber primary afferent neurons, which are related to the pain-sensing system. In this study, 5-hydroxy pyridine derivatives were designed, synthesized, and evaluated for their in vitro biological activities by two-electrode voltage clamp assay at hP2X3 receptors. Among the novel hP2X3 receptor antagonists, intrathecal treatment of compound 29 showed parallel efficacy with pregabalin (calcium channel modulator) and higher efficacy than AF353 (P2X3 receptor antagonist) in the evaluation of its antiallodynic effects in spinal nerve ligation rats. However, because compound 29 was inactive by intraperitoneal administration in neuropathic pain animal models due to low cell permeability, the corresponding methyl ester analogue, 28, which could be converted to compound 29 in vivo, was investigated as a prodrug concept. Intravenous injection of compound 28 resulted in potent antiallodynic effects, with ED50 values of 2.62 and 2.93 mg/kg in spinal nerve ligation and chemotherapy-induced peripheral neuropathy rats, respectively, indicating that new drug development targeting the P2X3 receptor could be promising for neuropathic pain, a disease with high unmet medical needs.Entities:
Keywords: Neuropathic pain; P2X3 receptor; adenosine 5′-triphosphate; antagonist; antiallodynic effect; structure−activity relationship
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Year: 2017 PMID: 28323403 DOI: 10.1021/acschemneuro.6b00401
Source DB: PubMed Journal: ACS Chem Neurosci ISSN: 1948-7193 Impact factor: 4.418