The regulatory role and mechanism of CP-25 on OAT1 in rats with collagen-induced arthritis

Fei DUAN; Jin-Zhang GAO; Yong WANG; Bin WANG; Wei WEI; Chun WANG

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The regulatory role and mechanism of CP-25 on OAT1 in rats with collagen-induced arthritis

VernacularTitle:CP-25对大鼠胶原性关节炎OAT1的调控作用及机制
Author: Fei DUAN ¹ ; Jin-Zhang GAO ; Yong WANG ; Bin WANG ; Wei WEI ; Chun WANG
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1. 安徽医科大学临床药理研究所,抗炎免疫药物教育部重点实验室,安徽省抗炎免疫药物协同创新中心,安徽合肥 230032
Keywords: rheumatoid arthritis; CP-25; OAT1; PGE2; EP4; PKA; GRK2
From: Chinese Pharmacological Bulletin 2024;40(12):2295-2302
CountryChina
Language:Chinese
Abstract: Aim The present study was conducted to investigate the expression of organic anion transporter 1(OAT1)in synovial tissue of collagen-induced arthritis(CIA)rats and the effect of paeoniflorin-6'-O-benzene sulfonate(CP-25),and meanwhile reveal its potential regulatory mechanism.Methods The rat CIA model was established and treated with CP-25(50 mg·kg-1·d-1),paroxetine(15 mg·kg-1·d-),prosta-glandin E receptor 4(EP4)antagonist(3 mg·kg-1·d-1),or a combination of CP-25(50 mg·kg-1·d-1)plus EP4 antagonist(3 mg·kg-1·d-1),while methotrexate(0.5 mg·kg-1·3d-1)was used as the positive control drug.Clinical manifestation of CIA rats,including arthritis index,numbers of swollen joints,paw volume of non-injected hind and clinical scores was measured.Moreover,X-ray imaging of paw,pathological examination of the ankle joint and quantitative assessment were conducted.The concen-tration of serum prostaglandin E2(PGE2)was quanti-fied using the ELISA.Western blot analysis was em-ployed to assess the levels of phospho-G protein-cou-pled receptor kinase 2(p-GRK2),protein kinase A(PKA),EP4 and OAT1 membrane proteins of rat syn-ovial tissues following CP-25 treatment.Results The administration of CP-25 resulted in a reduction in foot swelling,global score,arthritis index,paw volume of non-injected,and numbers of swollen joints in CIA rats.Pathological examination and X-ray analysis re-vealed that CP-25 significantly ameliorated the patho-logical changes and bone erosion degree of CIA rats.CP-25 significantly lowered PGE2 concentration in the serum of CIA rats.In the CIA model group,membrane expression of OAT1 and EP4 in synovial tissues of rats was significantly downregulated.Treatment with CP-25 or paroxetine resulted in a significant upregulation of OAT1 and EP4 expression and the effect of CP-25 on OAT1 was blocked when EP4 antagonist was used to-gether.Furthermore,the expression of p-GRK2 in syn-ovial tissue from CIA rats was significantly upregulat-ed,and however,CP-25 or paroxetine interventions led to a significant reduction in p-GRK2 expression.The expression trend of PKA was similar to that of OAT1.Conclusion OAT1 membrane expression is reduced in the synovial tissue of CIA rats,and CP-25 treatment increases OAT1 membrane expression.The PGE2-EP4-PKA pathway may be involved in the regu-lation of OAT1 by CP-25.