首页> 外文期刊>JAMA otolaryngology-- head & neck surgery >Comparison of Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) and Ciliary Beat Frequency Activation by the CFTR Modulators Genistein, VRT-532, and UCCF-152 in Primary Sinonasal Epithelial Cultures.
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Comparison of Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) and Ciliary Beat Frequency Activation by the CFTR Modulators Genistein, VRT-532, and UCCF-152 in Primary Sinonasal Epithelial Cultures.

机译:比较囊性纤维化跨膜电导调节器(CFTR)和CFTR调节剂Genistein,VRT-532和UCCF-152在初级鼻窦上皮培养物中的纤毛搏动频率激活。

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IMPORTANCE Pharmacologic activation of mucociliary clearance (MCC) represents an emerging therapeutic strategy for patients with chronic rhinosinusitis, even in the absence of congenital mutations of the CFTR gene. Drug discovery efforts have identified small molecules that activate the cystic fibrosis transmembrane conductance regulator (CFTR), including potentiators under development for treatment of cystic fibrosis. OBJECTIVE To evaluate the properties of CFTR modulators and their effects on ciliary beat frequency (CBF) in human sinonasal epithelium (HSNE). DESIGN Primary HSNE cultures (wild type and F508del/F508del) were used to compare stimulation of CFTR-mediated Cl- conductance and CBF by the CFTR modulators genistein, VRT-532, and UCCF-152. MAIN OUTCOMES AND MEASURES Increase in CFTR-dependent anion transport and CBF. RESULTS HSNE cultures were analyzed using pharmacologic manipulation of ion transport (change in short-circuit current [?ISC]) and high-speed digital imaging (CBF). Activation of CFTR-dependent anion transport was significantly different among agonists (P??.001), with genistein exerting the greatest effect (mean [SD] ?ISC, genistein, 23.1 [1.8] μA/cm2??VRT-532, 8.1 [1.0] μA/cm2??UCCF-152, 3.4 [1.4] μA/cm2??control, 0.7 [0.2] μA/cm2; Tukey-Kramer P??.05) in the absence of forskolin. Genistein and UCCF-152 augmented CBF (under submerged conditions) significantly better (Tukey-Kramer P??.05) than cells treated with VRT-532 or dimethyl sulfoxide vehicle control (mean [SD] fold change over baseline, genistein, 1.63 [0.06]; UCCF-152, 1.56 [0.06]; VRT-532, 1.38 [0.08]; control, 1.27 [0.02]). Activation of CBF was blunted in F508del/F508del HSNE cultures. CONCLUSIONS AND RELEVANCE The degree of CBF stimulation was not dependent on the magnitude of Cl- secretion, suggesting that different mechanisms of action may underlie MCC activation by these small molecule potentiators. Agents that activate both CFTR-dependent ISC and CBF are particularly attractive as therapeutics because they may address 2 independent pathways that contribute to deficient MCC in chronic rhinosinusitis.
机译:重要信息即使在没有先天性CFTR基因突变的情况下,粘膜纤毛清除(MCC)的药理学活化仍是一种针对慢性鼻-鼻窦炎患者的新兴治疗策略。药物发现的努力已经确定了激活囊性纤维化跨膜电导调节剂(CFTR)的小分子,包括正在研发的用于治疗囊性纤维化的增效剂。目的评估CFTR调节剂的特性及其对人鼻窦上皮(HSNE)的纤毛搏动频率(CBF)的影响。设计使用主要的HSNE培养物(野生型和F508del / F508del)比较CFTR调节剂染料木黄酮,VRT-532和UCCF-152对CFTR介导的Cl电导和CBF的刺激。主要结果和措施增加依赖CFTR的阴离子转运和CBF。结果采用离子迁移的药理学方法(短路电流[ISC]的变化)和高速数字成像(CBF)对HSNE培养物进行了分析。激动剂之间CFTR依赖性阴离子转运的激活显着不同(P <0.001),金雀异黄素发挥最大的作用(平均[SD]ΔISC,染料木黄酮23.1 [1.8]μA/ cm2?>?VRT-532 ,在没有毛喉素存在的情况下,为8.1 [1.0]μA/ cm 2 ≥UCCF-152,3.4 [1.4]μA/ cm 2≥对照,0.7 [0.2]μA/ cm 2; Tukey-Kramer P≤0.05。 。 Genistein和UCCF-152增强的CBF(在淹没条件下)(Tukey-Kramer P 。05)比用VRT-532或二甲基亚砜载体对照处理的细胞(平均[SD]倍数变化基线,染料木黄酮1.63)好得多[0.06]; UCCF-152,1.56 [0.06]; VRT-532,1.38 [0.08];对照,1.27 [0.02])。在F508del / F508del HSNE培养物中,CBF的激活受到抑制。结论和相关性CBF刺激的程度不依赖于Cl分泌的大小,表明这些小分子增强剂激活MCC可能是不同的作用机制。激活同时依赖CFTR的ISC和CBF的药物作为治疗剂特别有吸引力,因为它们可以解决两条独立的途径,这些途径可导致慢性鼻-鼻窦炎的MCC缺乏。

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