Analysis of gene mutations among South Indian patients with maple syrup urine disease: identification of four novel mutations.

IF 1.5 4区生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY

Indian journal of biochemistry & biophysics Pub Date : 2013-10-01

M P Narayanan, Krishnakumar N Menon, D M Vasudevan

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引用次数: 0

Abstract

Maple syrup urine disease (MSUD) is predominantly caused by mutations in the BCKDHA, BCKDHB and DBT genes, which encode for the E1alpha, E1beta and E2 subunits of the branched-chain alpha-keto acid dehydrogenase complex, respectively. Because disease causing mutations play a major role in the development of the disease, prenatal diagnosis at gestational level may have significance in making decisions by parents. Thus, this study was aimed to screen South Indian MSUD patients for mutations and assess the genotype-phenotype correlation. Thirteen patients diagnosed with MSUD by conventional biochemical screening such as urine analysis by DNPH test, thin layer chromatography for amino acids and blood amino acid quantification by HPLC were selected for mutation analysis. The entire coding regions of the BCKDHA, BCKDHB and DBT genes were analyzed for mutations by PCR-based direct DNA sequencing. BCKDHA and BCKDHB mutations were seen in 43% of the total ten patients, while disease-causing DBT gene mutation was observed only in 14%. Three patients displayed no mutations. Novel mutations were c.130C>T in BCKDHA gene, c. 599C>T and c.121_122delAC in BCKDHB gene and c.190G>A in DBT gene. Notably, patients harbouring these mutations were non-responsive to thiamine supplementation and other treatment regimens and might have a worse prognosis as compared to the patients not having such mutations. Thus, identification of these mutations may have a crucial role in the treatment as well as understanding the molecular mechanisms in MSUD.

本刊更多论文

南印度枫糖浆尿病患者的基因突变分析:鉴定四种新突变

枫糖浆尿病(MSUD)主要由BCKDHA、BCKDHB和DBT基因突变引起，这三个基因分别编码支链α -酮酸脱氢酶复合物的e1α、e1β和E2亚基。由于引起疾病的突变在疾病的发展中起主要作用，因此妊娠期的产前诊断可能对父母的决策具有重要意义。因此，本研究旨在筛选南印度MSUD患者的突变并评估基因型-表型相关性。选择13例经常规生化筛查诊断为MSUD的患者进行突变分析，如尿液DNPH分析、氨基酸薄层色谱分析、血液氨基酸HPLC定量等。利用pcr技术对BCKDHA、BCKDHB和DBT基因的整个编码区进行突变分析。10例患者中有43%出现BCKDHA和BCKDHB突变，而引起疾病的DBT基因突变仅占14%。三名患者没有出现突变。新突变为BCKDHA基因c. 130c >T, BCKDHB基因c. 599C>T和c. 121_122delac, DBT基因c. 190g >A。值得注意的是，携带这些突变的患者对补充硫胺素和其他治疗方案没有反应，与没有这种突变的患者相比，可能有更差的预后。因此，鉴定这些突变可能在治疗和理解MSUD的分子机制中起着至关重要的作用。

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

Indian journal of biochemistry & biophysics 生物-生化与分子生物学

CiteScore

2.90

自引率

50.00%

发文量

审稿时长

3 months

期刊介绍： Started in 1964, this journal publishes original research articles in the following areas: structure-function relationships of biomolecules; biomolecular recognition, protein-protein and protein-DNA interactions; gene-cloning, genetic engineering, genome analysis, gene targeting, gene expression, vectors, gene therapy; drug targeting, drug design; molecular basis of genetic diseases; conformational studies, computer simulation, novel DNA structures and their biological implications, protein folding; enzymes structure, catalytic mechanisms, regulation; membrane biochemistry, transport, ion channels, signal transduction, cell-cell communication, glycobiology; receptors, antigen-antibody binding, neurochemistry, ageing, apoptosis, cell cycle control; hormones, growth factors; oncogenes, host-virus interactions, viral assembly and structure; intermediary metabolism, molecular basis of disease processes, vitamins, coenzymes, carrier proteins, toxicology; plant and microbial biochemistry; surface forces, micelles and microemulsions, colloids, electrical phenomena, etc. in biological systems. Solicited peer reviewed articles on contemporary Themes and Methods in Biochemistry and Biophysics form an important feature of IJBB. Review articles on a current topic in the above fields are also considered. They must dwell more on research work done during the last couple of years in the field and authors should integrate their own work with that of others with acumen and authenticity, mere compilation of references by a third party is discouraged. While IJBB strongly promotes innovative novel research works for publication as full length papers, it also considers research data emanating from limited objectives, and extension of ongoing experimental works as ‘Notes’. IJBB follows “Double Blind Review process” where author names, affiliations and other correspondence details are removed to ensure fare evaluation. At the same time, reviewer names are not disclosed to authors.