Trotta Maria Consiglia, Herman Hildegard, Ciceu Alina, Mladin Bianca, Rosu Marcel, Lepre Caterina Claudia, Russo Marina, Bácskay Ildikó, Fenyvesi Ferenc, Marfella Raffaele, Hermenean Anca, Balta Cornel, D'Amico Michele
Department of Experimental Medicine, University of Campania "Luigi Vanvitelli", Naples, Italy.
"Aurel Ardelean" Institute of Life Sciences, Vasile Goldis Western University of Arad, Arad, Romania.
Front Pharmacol. 2023 Dec 18;14:1332212. doi: 10.3389/fphar.2023.1332212. eCollection 2023.
Cardiac fibrosis is strongly induced by diabetic conditions. Both chrysin (CHR) and calixarene OTX008, a specific inhibitor of galectin 1 (Gal-1), seem able to reduce transforming growth factor beta (TGF-β)/SMAD pro-fibrotic pathways, but their use is limited to their low solubility. Therefore, we formulated a dual-action supramolecular system, combining CHR with sulfobutylated β-cyclodextrin (SBECD) and OTX008 (SBECD + OTX + CHR). Here we aimed to test the anti-fibrotic effects of SBECD + OTX + CHR in hyperglycemic H9c2 cardiomyocytes and in a mouse model of chronic diabetes. H9c2 cardiomyocytes were exposed to normal (NG, 5.5 mM) or high glucose (HG, 33 mM) for 48 h, then treated with SBECD + OTX + CHR (containing OTX008 0.75-1.25-2.5 µM) or the single compounds for 6 days. TGF-β/SMAD pathways, Mitogen-Activated Protein Kinases (MAPKs) and Gal-1 levels were assayed by Enzyme-Linked Immunosorbent Assays (ELISAs) or Real-Time Quantitative Reverse Transcription Polymerase chain reaction (qRT-PCR). Adult CD1 male mice received a single intraperitoneal (i.p.) administration of streptozotocin (STZ) at a dosage of 102 mg/kg body weight. From the second week of diabetes, mice received 2 times/week the following i.p. treatments: OTX (5 mg/kg)-SBECD; OTX (5 mg/kg)-SBECD-CHR, SBECD-CHR, SBECD. After a 22-week period of diabetes, mice were euthanized and cardiac tissue used for tissue staining, ELISA, qRT-PCR aimed to analyse TGF-β/SMAD, extracellular matrix (ECM) components and Gal-1. In H9c2 cells exposed to HG, SBECD + OTX + CHR significantly ameliorated the damaged morphology and reduced TGF-β1, its receptors (TGFβR1 and TGFβR2), SMAD2/4, MAPKs and Gal-1. Accordingly, these markers were reduced also in cardiac tissue from chronic diabetes, in which an amelioration of cardiac remodeling and ECM was evident. In both settings, SBECD + OTX + CHR was the most effective treatment compared to the other ones. The CHR-based supramolecular SBECD-calixarene drug delivery system, by enhancing the solubility and the bioavailability of both CHR and calixarene OTX008, and by combining their effects, showed a strong anti-fibrotic activity in rat cardiomyocytes and in cardiac tissue from mice with chronic diabetes. Also an improved cardiac tissue remodeling was evident. Therefore, new drug delivery system, which could be considered as a novel putative therapeutic strategy for the treatment of diabetes-induced cardiac fibrosis.
糖尿病状态可强烈诱导心脏纤维化。白杨素(CHR)和杯芳烃OTX008(一种半乳糖凝集素1(Gal-1)的特异性抑制剂)似乎都能够减少转化生长因子β(TGF-β)/SMAD促纤维化途径,但它们的应用因溶解度低而受到限制。因此,我们构建了一种双作用超分子体系,将CHR与磺丁基化β-环糊精(SBECD)和OTX008(SBECD + OTX + CHR)相结合。在此,我们旨在测试SBECD + OTX + CHR在高血糖H9c2心肌细胞和慢性糖尿病小鼠模型中的抗纤维化作用。将H9c2心肌细胞暴露于正常(NG,5.5 mM)或高糖(HG,33 mM)环境中48小时,然后用SBECD + OTX + CHR(含0.75 - 1.25 - 2.5 μM的OTX008)或单一化合物处理6天。通过酶联免疫吸附测定(ELISA)或实时定量逆转录聚合酶链反应(qRT-PCR)检测TGF-β/SMAD途径、丝裂原活化蛋白激酶(MAPKs)和Gal-1水平。成年CD1雄性小鼠腹腔注射一次链脲佐菌素(STZ),剂量为102 mg/kg体重。从糖尿病第二周起,小鼠每周接受2次以下腹腔注射治疗:OTX(5 mg/kg)-SBECD;OTX(5 mg/kg)-SBECD-CHR、SBECD-CHR、SBECD。糖尿病22周后,对小鼠实施安乐死,并将心脏组织用于组织染色、ELISA、qRT-PCR,旨在分析TGF-β/SMAD、细胞外基质(ECM)成分和Gal-1。在暴露于HG的H9c2细胞中,SBECD + OTX + CHR显著改善了受损的形态,并降低了TGF-β1、其受体(TGFβR1和TGFβR2)、SMAD2/4、MAPKs和Gal-1。相应地,在慢性糖尿病小鼠的心脏组织中,这些标志物也有所降低,其中心脏重塑和ECM得到明显改善。在这两种情况下,与其他治疗相比,SBECD + OTX + CHR是最有效的治疗方法。基于CHR的超分子SBECD-杯芳烃药物递送系统,通过提高CHR和杯芳烃OTX008的溶解度和生物利用度,并结合它们的作用,在大鼠心肌细胞和慢性糖尿病小鼠的心脏组织中显示出强大的抗纤维化活性。同时,心脏组织重塑也得到明显改善。因此,这种新的药物递送系统可被视为一种治疗糖尿病性心脏纤维化的新型潜在治疗策略。
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