Your search keyword '"non-synonymous"' showing total 2 results

1. Analysis of variants in mitochondrial genome and their putative pathogenicity in tuberculosis patients from Mizoram, North east India.

Author

Vanlalhruaii Tonsing, Mary, Vanlalbiakdiki Sailo, Christine, Zothansanga, Chhakchhuak, Lily, Chhakchhuak, Zothankhuma, Pandit, Bhaswati, Kumar, Dhiraj, Pratim Mazumder, Partha, and Senthil Kumar, Nachimuthu

Subjects

*TUBERCULOSIS patients, *MYCOBACTERIUM tuberculosis, *MITOCHONDRIAL DNA, *GENOMES, *TUBERCULOSIS, *MICROBIAL virulence, *MITOCHONDRIAL DNA abnormalities

Abstract

• First report of mtDNA coding and non-coding variants among TB patients. • In coding region, a total of 94 variants were present in different genes. • Variants in ND2 and ND6 genes were deleterious in Polyphen-2 and Provean. • 83 variants were observed in non-coding region (D-loop, 16 s, 12 s, tRNA-Gln, Thr). Tuberculosis caused by Mycobacterium tuberculosis is one of the main global health concerns. In this study, the entire mitochondrial genome from blood samples of tuberculosis patients was analyzed to understand the possible mtDNA variants. The potential impact of non-synonymous substitutions on protein functions were determined using prediction tools. 28 non- synonymous variants were found of which 2 variants (MT-ND2 g. A > G4824 p.T119A and MT-ND6 g. T > C14180 p.Y165C) were found to be deleterious among the cases only. Majority of the variants lie in the D-loop of the non-protein coding region of the mitochondrial DNA. We propose that mutations in the mitochondrial genome need to be validated further to understand their association with tuberculosis. [ABSTRACT FROM AUTHOR]

Published

2020

2. Genomic profiling of mitochondrial DNA reveals novel complex gene mutations in familial type 2 diabetes mellitus individuals from Mizo ethnic population, Northeast India.

Author

Lalrohlui, Freda, Zohmingthanga, John, hruaii, Vanlal, and Kumar, Nachimuthu Senthil

Subjects

*MITOCHONDRIAL DNA, *TYPE 2 diabetes, *DNA fingerprinting

Abstract

• The current work is the first approach related to mtDNA sequencing from a high risk tribal population. • Mutations in the coding and noncoding regions of the mitochondria might have contribution towards the development of T2D. • This study can be used as a diagnostic marker towards T2D. The variants reported for mitochondrial DNA (mtDNA) and type 2 diabetes (T2D) may not be accountable for the disease in certain other populations and the risk depends upon numerous factors which may include genetics, environment as well as ethnicity. This leads to a challenge in identifying, exploring and comparing the variants between diabetic cases and healthy controls in a remote unexplored tribal population. To study the possible contribution of mtDNA variants, we sequenced the entire mitochondrial genomes and the frequencies of mtSNPs, their association with familial T2D and the potential impact of non-synonymous substitutions on protein functions were determined. The mtSNP 8584 G > A (ATP6: A20T) was detected in 14.28% of the diabetic patients and none in the control groups. The mitochondrial ND3 variant 10398A > G was found to be significantly associated with the risk of T2D (OR = 9.489, 95% CI = 1.161–77.54, P value = 0.036). A novel Frame-shift substitution ND5: 81_81ins A at position 12,417 was observed in 53.57% of diabetic individuals. Majority of the variants lie in tRNA-Phe in the non-protein coding region of mtDNA for both diabetic cases and common cases. We concluded that mutations in the coding (synonymous or non-synonymous) and noncoding regions of the mitochondria might have contribution towards the development of T2D. Our study is the first to report the distinct mitochondrial variants which may be attributed to the susceptibility as well as development of type 2 diabetes in an ethnic tribe from northeast India. [ABSTRACT FROM AUTHOR]

Published

2020