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囊性纤维化患者复杂等位基因 [E217G;G509D] 的临床和遗传特征及 CFTR 通道功能评估。

Clinical and Genetic Characteristics of a Patient with Cystic Fibrosis with a Complex Allele [E217G;G509D] and Functional Evaluation of the CFTR Channel.

机构信息

Research Centre for Medical Genetics, 115522 Moscow, Russia.

出版信息

Genes (Basel). 2023 Aug 28;14(9):1705. doi: 10.3390/genes14091705.

Abstract

The intricate nature of complex alleles presents challenges in the classification of gene mutations, encompassing potential disease-causing, neutral, or treatment-modulating effects. Notably, the complex allele [E217G;G509D] remains absent from international databases, with its pathogenicity yet to be established. Assessing the functionality of apical membrane ion channels in intestinal epithelium employed the intestinal current measurements (ICM) method, using rectal biopsy material. The effectivity of CFTR-targeted therapy was evaluated using a model of intestinal organoids of a patient harboring the genotype F508del/[E217G;G509D]. ICM analysis revealed diminished chloride channel function. Remarkably, [E217G;G509D] presence within intestinal organoids correlated with heightened residual CFTR function. Employing CFTR modulators facilitated the restoration of the functional CFTR protein. This multifaceted study intertwines genetic investigations, functional analyses, and therapeutic interventions, shedding light on the intricate interplay of complex alleles within CFTR mutations. The results highlight the potential of targeted CFTR modulators to restore functional integrity, offering promise for advancing precision treatments in cystic fibrosis management.

摘要

复杂等位基因的复杂性质给基因突变的分类带来了挑战,其中包括潜在的致病、中性或治疗调节作用。值得注意的是,国际数据库中尚未收录复杂等位基因 [E217G;G509D],其致病性尚未确定。采用直肠活检材料,通过肠电流测量 (ICM) 方法评估肠道上皮顶膜离子通道的功能。使用携带基因型 F508del/[E217G;G509D] 的患者肠类器官模型评估 CFTR 靶向治疗的效果。ICM 分析显示氯离子通道功能降低。值得注意的是,[E217G;G509D] 在肠类器官中的存在与 CFTR 残留功能的提高相关。使用 CFTR 调节剂有助于恢复功能性 CFTR 蛋白。这项多方面的研究将遗传研究、功能分析和治疗干预交织在一起,揭示了 CFTR 突变中复杂等位基因的复杂相互作用。研究结果强调了靶向 CFTR 调节剂恢复功能完整性的潜力,为推进囊性纤维化管理的精准治疗提供了希望。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a0c5/10530926/96bc9b29e5c2/genes-14-01705-g001.jpg

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