Spectrum of Rare and Novel Indel Mutations Responsible for β Thalassemia in Eastern India

IF 1.5 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Indian Journal of Clinical Biochemistry Pub Date : 2023-01-03 DOI:10.1007/s12291-022-01098-w
Sajan Sinha, Atanu Kumar Dutta, Paramita Bhattacharya, Subham Bhattacharya, Mrinal Kanti Das
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引用次数: 1

Abstract

There is limited data available regarding the clinical utility of routine molecular diagnosis of β Thalassaemia in addition to HPLC-based screening in low resource settings. The current study highlights the caveats of an HPLC-based screening compared to the inclusion of genetic confirmation as a second-tier test and its implications in terms of genotype-phenotype correlation. A prospective, institution-based, observational study was conducted at the Department of Paediatric Medicine, including 103 children aged up to 12 years. Five common mutations for β Thalassemia and the HbE mutation in the HBB gene were tested by a two-tiered approach using multiplex ARMS PCR and PCR RFLP methods respectively. Sanger sequencing of all three exons of the HBB gene was performed in all negative cases. Sequencing revealed many rare pathogenic mutations like c.316-106 C > G (dbSNP: 34,690,599); Hb Kairouan (c.92G > C); c.33 C > A (dbSNP rs35799536); c.47G > A (dbSNP rs63750783); c.51delC (HbVar ID 799); c.[93-2 A > C] and c.118 C > T (HbVar ID 845). We detected a novel Pathogenic M_000518.5(HBB):c.164_168delinsGGCATCA (p.Val55fs) mutation in a heterozygous state which was reported in the ClinVar database with accession ID VCV000590977.2. We also encountered several cases of silent carrier on HPLC and de novo occurrence of mutation. We conclude that the multiplex touchdown ARMS PCR methodology employed in the present study provides a low-cost solution for molecular diagnostics of Β Thalassaemia. The problem of silent carriers in HPLC is significant enough to rethink if we need supplemental genetic testing in the couple when one of the partners is a carrier.
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印度东部导致β地中海贫血的罕见和新型Indel突变谱
在资源匮乏的地区,除了基于高效液相色谱的筛查外,关于β地中海贫血常规分子诊断的临床应用数据有限。目前的研究强调了以高效液相色谱为基础的筛查与将遗传确认作为第二级检测的注意事项及其在基因型-表型相关性方面的意义。在儿科医学系进行了一项前瞻性、基于机构的观察性研究,包括103名12岁以下的儿童。采用多重ARMS PCR和PCR RFLP两种方法分别检测β地中海贫血的5种常见突变和HBB基因中的HbE突变。在所有阴性病例中,对HBB基因的所有三个外显子进行Sanger测序。测序显示许多罕见的致病突变,如C .316-106 C > G (dbSNP: 34,690,599);Hb Kairouan (C . 92g > C);c.33C > A (dbSNP rs35799536);c.47G > A (dbSNP rs63750783);c.51delC (HbVar ID 799);c.[93-2 A > c]C > T (HbVar ID 845)。我们检测到一种新的致病因子M_000518.5(HBB):c。在ClinVar数据库中报道了一个杂合状态的164_168delinsGGCATCA (p.Val55fs)突变,登录ID为VCV000590977.2。我们还在HPLC上遇到了几例沉默携带者和重新发生突变的病例。我们得出结论,本研究中采用的多重触点ARMS PCR方法为Β地中海贫血的分子诊断提供了一种低成本的解决方案。HPLC中沉默携带者的问题非常重要,足以让我们重新思考,当其中一方是携带者时,我们是否需要对夫妇进行补充基因检测。
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来源期刊
Indian Journal of Clinical Biochemistry
Indian Journal of Clinical Biochemistry BIOCHEMISTRY & MOLECULAR BIOLOGY-
CiteScore
4.50
自引率
4.80%
发文量
74
期刊介绍: The primary mission of the journal is to promote improvement in the health and well-being of community through the development and practice of clinical biochemistry and dissemination of knowledge and recent advances in this discipline among professionals, diagnostics industry, government and non-government organizations. Indian Journal of Clinical Biochemistry (IJCB) publishes peer reviewed articles that contribute to the existing knowledge in all fields of Clinical biochemistry, either experimental or theoretical, particularly deal with the applications of biochemistry, molecular biology, genetics, biotechnology, and immunology to the diagnosis, treatment, monitoring and prevention of human diseases. The articles published also include those covering the analytical and molecular diagnostic techniques, instrumentation, data processing, quality assurance and accreditation aspects of the clinical investigations in which chemistry has played a major role, or laboratory animal studies with biochemical and clinical relevance.
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