Mitochondrial DNA mutations in Malaysian female breast cancer patients.

Mitochondrial DNA mutations in Malaysian female breast cancer patients.

Cancer development has been ascribed with diverse genetic variations which are identified in both mitochondrial and nuclear genomes. Mitochondrial DNA (mtDNA) alterations have been detected in several tumours which include lung, colorectal, renal, pancreatic and breast cancer. Several studies have e...

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Main Authors: Raevathi Omasanggar, Choo Yee Yu, Geik Yong Ang, Nor Aina Emran, Normayah Kitan, Anita Baghawi, Atiki Falparado Ahmad, Maizaton Atmadini Abdullah, Lay Kek Teh, Sandra Maniam
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2020-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0233461
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spelling doaj-3577a13356314a4797b724ed20825ae92021-03-03T21:51:20ZengPublic Library of Science (PLoS)PLoS ONE1932-62032020-01-01155e023346110.1371/journal.pone.0233461Mitochondrial DNA mutations in Malaysian female breast cancer patients.Raevathi OmasanggarChoo Yee YuGeik Yong AngNor Aina EmranNormayah KitanAnita BaghawiAtiki Falparado AhmadMaizaton Atmadini AbdullahLay Kek TehSandra ManiamCancer development has been ascribed with diverse genetic variations which are identified in both mitochondrial and nuclear genomes. Mitochondrial DNA (mtDNA) alterations have been detected in several tumours which include lung, colorectal, renal, pancreatic and breast cancer. Several studies have explored the breast tumour-specific mtDNA alteration mainly in Western population. This study aims to identify mtDNA alterations of 20 breast cancer patients in Malaysia by next generation sequencing analysis. Twenty matched tumours with corresponding normal breast tissues were obtained from female breast cancer patients who underwent mastectomy. Total DNA was extracted from all samples and the entire mtDNA (16.6kb) was amplified using long range PCR amplification. The amplified PCR products were sequenced using mtDNA next-generation sequencing (NGS) on an Illumina Miseq platform. Sequencing involves the entire mtDNA (16.6kb) from all pairs of samples with high-coverage (~ 9,544 reads per base). MtDNA variants were called and annotated using mtDNA-Server, a web server. A total of 18 of 20 patients had at least one somatic mtDNA mutation in their tumour samples. Overall, 65 somatic mutations were identified, with 30 novel mutations. The majority (59%) of the somatic mutations were in the coding region, whereas only 11% of the mutations occurred in the D-loop. Notably, somatic mutations in protein-coding regions were non-synonymous (49%) in which 15.4% of them are potentially deleterious. A total of 753 germline mutations were identified and four of which were novel mutations. Compared to somatic alterations, less than 1% of germline missense mutations are harmful. The findings of this study may enhance the current knowledge of mtDNA alterations in breast cancer. To date, the catalogue of mutations identified in this study is the first evidence of mtDNA alterations in Malaysian female breast cancer patients.https://doi.org/10.1371/journal.pone.0233461
collection DOAJ
language English
format Article
sources DOAJ
author Raevathi Omasanggar
Choo Yee Yu
Geik Yong Ang
Nor Aina Emran
Normayah Kitan
Anita Baghawi
Atiki Falparado Ahmad
Maizaton Atmadini Abdullah
Lay Kek Teh
Sandra Maniam
spellingShingle Raevathi Omasanggar
Choo Yee Yu
Geik Yong Ang
Nor Aina Emran
Normayah Kitan
Anita Baghawi
Atiki Falparado Ahmad
Maizaton Atmadini Abdullah
Lay Kek Teh
Sandra Maniam
Mitochondrial DNA mutations in Malaysian female breast cancer patients.
PLoS ONE
author_facet Raevathi Omasanggar
Choo Yee Yu
Geik Yong Ang
Nor Aina Emran
Normayah Kitan
Anita Baghawi
Atiki Falparado Ahmad
Maizaton Atmadini Abdullah
Lay Kek Teh
Sandra Maniam
author_sort Raevathi Omasanggar
title Mitochondrial DNA mutations in Malaysian female breast cancer patients.
title_short Mitochondrial DNA mutations in Malaysian female breast cancer patients.
title_full Mitochondrial DNA mutations in Malaysian female breast cancer patients.
title_fullStr Mitochondrial DNA mutations in Malaysian female breast cancer patients.
title_full_unstemmed Mitochondrial DNA mutations in Malaysian female breast cancer patients.
title_sort mitochondrial dna mutations in malaysian female breast cancer patients.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2020-01-01
description Cancer development has been ascribed with diverse genetic variations which are identified in both mitochondrial and nuclear genomes. Mitochondrial DNA (mtDNA) alterations have been detected in several tumours which include lung, colorectal, renal, pancreatic and breast cancer. Several studies have explored the breast tumour-specific mtDNA alteration mainly in Western population. This study aims to identify mtDNA alterations of 20 breast cancer patients in Malaysia by next generation sequencing analysis. Twenty matched tumours with corresponding normal breast tissues were obtained from female breast cancer patients who underwent mastectomy. Total DNA was extracted from all samples and the entire mtDNA (16.6kb) was amplified using long range PCR amplification. The amplified PCR products were sequenced using mtDNA next-generation sequencing (NGS) on an Illumina Miseq platform. Sequencing involves the entire mtDNA (16.6kb) from all pairs of samples with high-coverage (~ 9,544 reads per base). MtDNA variants were called and annotated using mtDNA-Server, a web server. A total of 18 of 20 patients had at least one somatic mtDNA mutation in their tumour samples. Overall, 65 somatic mutations were identified, with 30 novel mutations. The majority (59%) of the somatic mutations were in the coding region, whereas only 11% of the mutations occurred in the D-loop. Notably, somatic mutations in protein-coding regions were non-synonymous (49%) in which 15.4% of them are potentially deleterious. A total of 753 germline mutations were identified and four of which were novel mutations. Compared to somatic alterations, less than 1% of germline missense mutations are harmful. The findings of this study may enhance the current knowledge of mtDNA alterations in breast cancer. To date, the catalogue of mutations identified in this study is the first evidence of mtDNA alterations in Malaysian female breast cancer patients.
url https://doi.org/10.1371/journal.pone.0233461
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