Romero Miguel, Toral Marta, Robles-Vera Iñaki, Sánchez Manuel, Jiménez Rosario, O'Valle Francisco, Rodriguez-Nogales Alba, Pérez-Vizcaino Francisco, Gálvez Julio, Duarte Juan
From the Department of Pharmacology, School of Pharmacy (M.R., M.T., I.R.-V., M.S., R.J., A.R.-N., F.P.-V., J.G., J.D.), Department of Pathology, School of Medicine (F.O.), and CIBER-EHD, Center for Biomedical Research (CIBM) (J.G.), University of Granada, Spain; Instituto de Investigación Biosanitaria de Granada, ibs.GRANADA, Spain (M.R., R.J., F.O., J.G., J.D.); CIBER Enfermedades Cardiovasculares, Granada, Spain (R.J., J.D.); Department of Pharmacology, School of Medicine, University Complutense of Madrid, Spain (F.P.-V.); CIBER Enfermedades Respiratorias, Madrid, Spain (F.P.-V.); and Instituto de Investigación Sanitaria Gregorio Marañón (IiSGM), Madrid, Spain (F.P.-V.).
Hypertension. 2017 Apr;69(4):641-650. doi: 10.1161/HYPERTENSIONAHA.116.08655. Epub 2017 Feb 27.
Women with systemic lupus erythematosus exhibit a high prevalence of hypertension, endothelial dysfunction, and renal injury. We tested whether GW0742, a peroxisome proliferator activator receptor β/δ (PPARβ/δ) agonist, ameliorates disease activity and cardiovascular complications in a female mouse model of lupus. Thirty-week-old NZBWF1 (lupus) and NZW/LacJ (control) mice were treated with GW0742 or with the PPARβ/δ antagonist GSK0660 plus GW0742 for 5 weeks. Blood pressure, plasma double-stranded DNA autoantibodies and cytokines, nephritis, hepatic opsonins, spleen lymphocyte populations, endothelial function, and vascular oxidative stress were compared in treated and untreated mice. GW0742 treatment reduced lupus disease activity, blood pressure, cardiac and renal hypertrophy, splenomegaly, albuminuria, and renal injury in lupus mice, but not in control. GW0742 increased hepatic opsonins mRNA levels in lupus mice and reduced the elevated T, B, Treg, and Th1 cells in spleens from lupus mice. GW0742 lowered the higher plasma concentration of proinflammatory cytokines observed in lupus mice. Aortae from lupus mice showed reduced endothelium-dependent vasodilator responses to acetylcholine and increased nicotinamide adenine dinucleotide phosphate oxidase-driven vascular reactive oxygen species production, which were normalized by GW0742 treatment. All these effects of GW0742 were inhibited by PPARβ/δ blockade with GSK0660. Pharmacological activation of PPARβ/δ reduced hypertension, endothelial dysfunction, and organ damage in severe lupus mice, which was associated with reduced plasma antidouble-stranded DNA autoantibodies and anti-inflammatory and antioxidant effects in target tissues. Our findings identify PPARβ/δ as a promising target for an alternative approach in the treatment of systemic lupus erythematosus and its associated vascular damage.
系统性红斑狼疮女性患者高血压、内皮功能障碍和肾损伤的患病率较高。我们测试了过氧化物酶体增殖物激活受体β/δ(PPARβ/δ)激动剂GW0742是否能改善狼疮雌性小鼠模型的疾病活动和心血管并发症。30周龄的NZBWF1(狼疮)和NZW/LacJ(对照)小鼠接受GW0742或PPARβ/δ拮抗剂GSK0660加GW0742治疗5周。比较治疗组和未治疗组小鼠的血压、血浆双链DNA自身抗体和细胞因子、肾炎、肝调理素、脾淋巴细胞群体、内皮功能和血管氧化应激。GW0742治疗降低了狼疮小鼠的狼疮疾病活动、血压、心脏和肾脏肥大、脾肿大、蛋白尿和肾损伤,但对对照组无效。GW0742增加了狼疮小鼠肝调理素mRNA水平,并减少了狼疮小鼠脾脏中升高的T、B、Treg和Th1细胞。GW0742降低了狼疮小鼠中观察到的较高血浆促炎细胞因子浓度。狼疮小鼠的主动脉对乙酰胆碱的内皮依赖性血管舒张反应降低,烟酰胺腺嘌呤二核苷酸磷酸氧化酶驱动的血管活性氧生成增加,而GW0742治疗使其恢复正常。GSK0660对PPARβ/δ的阻断抑制了GW0742的所有这些作用。PPARβ/δ的药理激活降低了重度狼疮小鼠的高血压、内皮功能障碍和器官损伤,这与血浆抗双链DNA自身抗体减少以及靶组织中的抗炎和抗氧化作用有关。我们的研究结果表明PPARβ/δ是治疗系统性红斑狼疮及其相关血管损伤的一种有前景的替代方法的靶点。
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