Investigation of CFTR Function in Human Nasal Epithelial Cells Informs Personalized Medicine.

IF 5.9 2区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Audrey Pion, Erin Kavanagh, Anya T Joynt, Karen S Raraigh, Lori Vanscoy, Elinor Langfelder-Schwind, John McNamara, Brooke Moore, Shivani Patel, Kate Merlo, Renee Temme, Valeria Capurro, Emanuela Pesce, Christian Merlo, Nicoletta Pedemonte, Garry R Cutting, Neeraj Sharma
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引用次数: 0

Abstract

We broaden the clinical versatility of human nasal epithelial (HNE) cells. HNEs were isolated from 10 participants harboring cystic fibrosis transmembrane conductance regulator (CFTR) variants: 9 with rare variants (Q359R [n =2], G480S, R334W [n =5], and R560T) and 1 harboring R117H;7T;TG10/5T;TG12. Cultures were differentiated at the air-liquid interface. CFTR function was measured in Ussing chambers at three conditions: baseline, ivacaftor, and elexacaftor + tezacaftor + ivacaftor (ETI). Four participants initiated modulators. Q359R HNEs had 5.4% (% wild-type) baseline CFTR function and 25.5% with ivacaftor. With therapy, sweat [Cl-] decreased and symptoms resolved. G480S HNEs had 4.1% baseline and 32.1% CFTR function with ETI. Clinically, forced expiratory volume in 1 second increased and sweat [Cl-] decreased (119 to 46 mmol/L) with ETI. In vitro cultures derived from 5 participants harboring R334W showed a moderate increase in CFTR function with exposure to modulators. For one of these participants, ETI was begun in vivo; symptoms and forced expiratory volume in 1 second improved. The c.1679G>C (R560T) HNEs had less than 4% baseline CFTR function and no modulator response. RNA analysis confirmed that c.1679G>C completely missplices. A symptomatic patient harboring R117H;7T;TG10/5T;TG12 exhibited reduced CFTR function (17.5%) in HNEs, facilitating a diagnosis of mild CF. HNEs responded to modulators (ivacaftor: 32.8%, ETI: 55.5%), and, since beginning therapy, lung function improved. We reaffirm HNE use for guiding therapeutic approaches, inform predictions on modulator response (e.g., R334W), and closely assess variants that affect splicing (e.g., c.1679G>C). Notably, functional studies in HNEs harboring R117H;7T;TG10/5T;TG12 facilitated a diagnosis of mild CF, suggesting the use for HNE functional studies as a clinical diagnostic test.

人类鼻腔上皮细胞 CFTR 功能研究为个性化医疗提供依据
我们拓宽了人鼻上皮细胞(HNE)的临床用途。我们从 10 名携带 CFTR 变体的参与者体内分离出 HNE:其中 9 人携带罕见变体(Q359R [n=2]、G480S、R334W [n=5] 和 R560T),1 人携带 R117H;7T;TG10/5T;TG12。培养物在空气-液体界面上分化。CFTR功能在Ussing室中以三种条件进行测量--基线、ivacaftor和lexacaftor+tezacaftor+ivacaftor(ESTI)。四名参与者开始使用调节剂。Q359R HNEs 的 CFTR 功能基线为 5.4%(%WT),使用 ivacaftor 时为 25.5%。接受治疗后,汗液[Cl-]减少,症状缓解。G480S HNEs 的 CFTR 功能基线为 4.1%,使用 ETI 后为 32.1%。临床上,使用 ETI 后,FEV1 增加,汗液[Cl-]减少(119 至 46mmol/L)。从五名携带 R334W 的患者身上提取的体外培养物显示,在接触调节剂后,CFTR 功能适度增加。c.1679G>C (R560T) HNEs 的 C 完全错接。一名携带 R117H;7T;TG10/5T;TG12的无症状患者的 HNEs 中 CFTR 功能降低(17.5%),有助于轻度 CF 诊断。HNE 对调节剂(依维卡夫托:32.8%;ETI:55.5%)有反应,自开始治疗以来,肺功能有所改善。在重申 HNE 用于指导治疗方法的同时,我们对调节剂反应(如 R334W)进行了预测,并密切评估了影响剪接的变异(如 c.1679G>C)。值得注意的是,对携带 R117H;7T;TG10/5T;TG12 的 HNE 进行功能研究有助于轻度 CF 诊断,这表明 HNE 功能研究可用作临床诊断测试。
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来源期刊
CiteScore
11.20
自引率
3.10%
发文量
370
审稿时长
3-8 weeks
期刊介绍: The American Journal of Respiratory Cell and Molecular Biology publishes papers that report significant and original observations in the area of pulmonary biology. The focus of the Journal includes, but is not limited to, cellular, biochemical, molecular, developmental, genetic, and immunologic studies of lung cells and molecules.
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