Mutation spectrum and enzyme profiling of G6PD deficiency in neonates of north India: a prospective study.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
ACS Applied Bio Materials Pub Date : 2023-01-01
Upasana Bhattacharyya, Preeti Deswal, Sunil Kumar Polipalli, Diksha Sharma, Manpreet Kaur, Seema Kapoor, B K Thelma
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Abstract

Glucose-6-phosphate dehydrogenase (G6PD) deficiency is a common X-linked disorder with well-established clinical and allelic heterogeneity and ethnic disparity. With ~390,000 annual births with G6PD deficiency in India, it emerges as the most predictable and preventable inbornmetabolic error. Disease prevalence and mutation spectrum have been reasonably reported fromcentral, western and southern parts of India and are mostly retrospective studies.Although prevalence data fromnorth India is available, there is paucity of data on the mutation spectrum and genotype-phenotype correlation (GxP). Thus, we aimed at establishing the clinical and mutation profiles for G6PD, as a part of a large prospective newborn screening study conducted between 2014 and 2016 across hospitals in Delhi, India. G6PD activity levels were measured at 24-48 h of life for ~200,000 neonates using Victor 2D and/or Genomic Screening Processor followed by confirmatory spectrophotometric analysis usingRBClysates of the respective neonates based on clinical symptoms.Asubset of 570 enzyme deficient neonates were screened formutations by polymerase chain reaction-restriction fragment length polymorphismand/or Sanger sequencing.Mediterraneanwas the most common mutation (n=318; 55.8%) with the lowest enzyme activity and most severe phenotype, followed by G6PD Orissa (n=187;32.8%); Kerala-Kalyan (n=25); Jammu (n=24);Mahidol (n=14); Chattam(n=1) andNilgiri/Coimbra (n=1).Of the 163 intramural neonates followed up, 68 developed clinical jaundice. However, no correlation was observed between jaundice and enzyme level. Notable outcome of this first ever prospective screening approach for G6PD deficiency in neonates may help in prediction of disease severity and appropriate timely management.

印度北部新生儿G6PD缺乏症的突变谱和酶谱:一项前瞻性研究。
葡萄糖-6-磷酸脱氢酶(G6PD)缺乏症是一种常见的x连锁疾病,具有明确的临床和等位基因异质性和种族差异。印度每年约有39万新生儿患有G6PD缺乏症,这是最可预测和可预防的先天性代谢错误。印度中部、西部和南部地区的疾病患病率和突变谱已经有了合理的报道,而且大多是回顾性研究。尽管有印度北部的患病率数据,但缺乏突变谱和基因型-表型相关性(GxP)的数据。因此,我们的目标是建立G6PD的临床和突变谱,作为2014年至2016年在印度德里各医院进行的大型前瞻性新生儿筛查研究的一部分。使用Victor 2D和/或基因组筛选处理器测量约200,000名新生儿24-48小时的G6PD活性水平,然后根据临床症状使用相应新生儿的grbcleysate进行验证性分光光度分析。通过聚合酶链反应-限制性片段长度多态性和/或Sanger测序筛选570例酶缺陷新生儿的配方。地中海型是最常见的突变(n=318;55.8%),酶活性最低,表型最严重,其次是G6PD Orissa (n=187, 32.8%);Kerala-Kalyan (n = 25);Jammu (n=24);Mahidol (n=14);Chattam(n=1)和nilgiri /Coimbra (n=1)。在随访的163名新生儿中,68名出现临床黄疸。然而,黄疸与酶水平没有相关性。值得注意的是,这是首次对新生儿G6PD缺乏症进行前瞻性筛查的方法,可能有助于预测疾病严重程度和适当的及时管理。
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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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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