Roberta Valeria Latorre , Martina Calicchia , Martina Bigliardi , Jessica Conti , Karina Kleinfelder , Paola Melotti , Claudio Sorio
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引用次数: 0
Abstract
Background
Many disease-causing variants in the Cystic Fibrosis Transmembrane conductance Regulator (CFTR) gene remain uncharacterized and untreated. Restoring the function of the impaired CFTR protein is the goal of personalized medicine, particularly in patients carrying rare CFTR variants. In this study, functional defects related to the rare R334W variant were evaluated after treatment with CFTR modulators or Roflumilast, a phosphodiesterase-4 inhibitor (PDE4i).
Methods
Rectal organoids from subjects with R334W/2184insA and R334W/2183AA > G genotypes were used to perform the Forskolin-induced swelling (FIS) assay. Organoids were left drug-untreated or treated with modulators VX-770 (I), VX-445 (E), and VX-661 (T) mixed, and their combination (ETI). Roflumilast (R) was used alone or as a combination of I + R.
Results
Our data show a significant increase in FIS rate following treatment with I alone. The combined use of modulators, such as ETI, did not increase further swelling than I alone, nor in protein maturation. Treatment with R shows an increase in FIS response similar to those of I, and the combination R + I significantly increases the rescue of CFTR activity.
Conclusions
Equivalent I and ETI treatment efficacy was observed for both genotypes. Furthermore, significant organoid swelling was observed with combined I + R used that supports the recently published data describing a potentiating effect of only I in patients carrying the variant R334W and, at the same time, corroborating the role of strategies that include PDE4 inhibitors further to potentiate the effect of I for this variant.
背景囊性纤维化跨膜传导调节器(CFTR)基因中的许多致病变体仍未定性和治疗。恢复受损的 CFTR 蛋白的功能是个性化医疗的目标,尤其是对于携带罕见 CFTR 变异基因的患者。在这项研究中,使用 CFTR 调节剂或磷酸二酯酶-4 抑制剂(PDE4i)罗氟司特治疗后,对与罕见 R334W 变异相关的功能缺陷进行了评估。有机体未经药物处理或用调节剂 VX-770 (I)、VX-445 (E) 和 VX-661 (T) 混合处理,以及它们的组合 (ETI) 处理。结果我们的数据显示,单独使用 I 治疗后,FIS 率显著增加。与单独使用 I 相比,联合使用 ETI 等调节剂不会进一步增加肿胀,也不会增加蛋白质成熟。R 的治疗显示 FIS 反应的增加与 I 相似,而 R + I 的组合则显著增加了对 CFTR 活性的挽救。此外,联合使用 I + R 还观察到明显的器官肿胀,这支持了最近发表的数据,该数据描述了仅 I 对携带 R334W 变体的患者的增效作用,同时也证实了包括 PDE4 抑制剂在内的策略在进一步增强 I 对该变体的作用方面所起的作用。