CFTR mutations and phenotypic correlations in people with cystic fibrosis: a retrospective study from a single centre in south India

IF 5 Q1 HEALTH CARE SCIENCES & SERVICES
Sneha D. Varkki , Rekha Aaron , Aaron Chapla , Sumita Danda , Priyanka Medhi , N. Jansi Rani , Grace R. Paul
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引用次数: 0

Abstract

Background

Emerging data reveal higher-than-expected prevalence of cystic fibrosis (CF) among non-European populations worldwide including in the Indian subcontinent. Systematic analyses of the CFTR mutation profile, and genotype-phenotype correlations among people with CF from south, east, or northeast India have not been reported before. We wanted to identify CFTR mutations in people with CF, and highlight novel variants, selective phenotypic correlations, and regional variances within India.

Methods

A retrospective study was conducted at Christian Medical College, Vellore, India (single tertiary referral hospital) from September 2010 to August 2022, involving 120 people with CF from (i) four south Indian states (Tamil Nadu, Andhra Pradesh, Kerala, Karnataka), (ii) in and nearby regions of West Bengal, India and (iii) Bangladesh. Comprehensive CFTR mutation analyses were done by Next-Generation Sequencing, and variants were categorized per American College of Medical Genetics guidelines and compared with validated Locus-specific databases. Demographic characteristics, mutation profile, novel mutations, selective phenotype correlations, and regional variances were assessed.

Findings

In 120 people with CF, 55 CFTR variants were identified, including six novel variants. F508del was the predominant mutation, yet with a lower allele frequency than reported among European populations (27% versus 70%). Phenotypic correlations suggested high mutational pathogenicity causing severe multi-organ morbidity, and death in 27%. Milder variants associated with pancreatic sufficiency were also evident in 23% of people with CF. Statistically significant regional variances were noted in genotype frequency, and clinical phenotype among people with CF from the two regions. Hotspot exons and introns that could potentially help create targeted mutation panels were identified.

Interpretation

The identification of 55 different CFTR variants among 120 people with CF describes the diversity of mutations noted in India, while also revealing the challenges that providers may encounter in timely diagnosis and treatment of CF. However, these single-centre data have specific limitations and cannot be generalised to all people with CF from India or to those of non-European origin. Our data on regional CFTR mutations contribute to the emerging national registry on CF epidemiology in India, help formulate diagnostic and newborn screening algorithms, help optimise clinical care, and highlight urgency to improve access to life-changing modulator therapy.

Funding

Cystic Fibrosis Foundation, USA (towards the CF-India Demonstration Project) and Christian Medical College, Vellore, India.

囊性纤维化患者的 CFTR 基因突变和表型相关性:印度南部一个中心的回顾性研究
背景最新数据显示,囊性纤维化(CF)在包括印度次大陆在内的全球非欧洲人群中的发病率高于预期。对印度南部、东部或东北部 CF 患者的 CFTR 基因突变情况以及基因型与表型之间的相关性进行系统分析的研究以前从未报道过。2010年9月至2022年8月,我们在印度韦洛尔基督教医学院(单一三级转诊医院)开展了一项回顾性研究,涉及120名CF患者,他们分别来自(i)印度南部四个邦(泰米尔纳德邦、安得拉邦、喀拉拉邦、卡纳塔克邦),(ii)印度西孟加拉邦及其附近地区,以及(iii)孟加拉国。通过新一代测序技术对 CFTR 基因突变进行了全面分析,并根据美国医学遗传学会的指导原则对变异进行了分类,同时与经过验证的特定病灶数据库进行了比较。对人口统计学特征、变异概况、新型变异、选择性表型相关性和地区差异进行了评估。研究结果在 120 名 CF 患者中发现了 55 个 CFTR 变异,其中包括 6 个新型变异。F508del是最主要的变异,但等位基因频率低于欧洲人群(27%对70%)。表型相关性表明变异的致病性很高,会导致严重的多器官发病,27%的患者会死亡。在23%的CF患者中,与胰腺功能不足有关的较轻变异也很明显。据统计,这两个地区的CF患者在基因型频率和临床表型方面存在明显的地区差异。在 120 名 CF 患者中鉴定出 55 种不同的 CFTR 变异描述了印度突变的多样性,同时也揭示了提供者在及时诊断和治疗 CF 方面可能遇到的挑战。然而,这些单中心数据有其特定的局限性,不能推广到所有印度或非欧洲血统的CF患者。我们关于地区性CFTR突变的数据有助于印度CF流行病学的国家登记,有助于制定诊断和新生儿筛查算法,有助于优化临床护理,并突出了改善获得改变生命的调节剂治疗的紧迫性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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