Facile whole mitochondrial genome resequencing from nipple aspirate fluid using MitoChip v2.0

BACKGROUND: Mutations in the mitochondrial genome (mtgenome) have been associated with many disorders, including breast cancer. Nipple aspirate fluid (NAF) from symptomatic women could potentially serve as a minimally invasive sample for breast cancer screening by detecting somatic mutations in this...

Descripción completa

Detalles Bibliográficos
Autores principales: Jakupciak, John P, Maggrah, Andrea, Maragh, Samantha, Maki, Jennifer, Reguly, Brian, Maki, Katrina, Wittock, Roy, Robinson, Kerry, Wagner, Paul D, Thayer, Robert E, Gehman, Ken, Gehman, Teresa, Srivastava, Sudhir, Ngom, Alioune, Dakubo, Gabriel D, Parr, Ryan L
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2375897/
https://www.ncbi.nlm.nih.gov/pubmed/18402686
http://dx.doi.org/10.1186/1471-2407-8-95
_version_ 1782154669904101376
author Jakupciak, John P
Maggrah, Andrea
Maragh, Samantha
Maki, Jennifer
Reguly, Brian
Maki, Katrina
Wittock, Roy
Robinson, Kerry
Wagner, Paul D
Thayer, Robert E
Gehman, Ken
Gehman, Teresa
Srivastava, Sudhir
Ngom, Alioune
Dakubo, Gabriel D
Parr, Ryan L
author_facet Jakupciak, John P
Maggrah, Andrea
Maragh, Samantha
Maki, Jennifer
Reguly, Brian
Maki, Katrina
Wittock, Roy
Robinson, Kerry
Wagner, Paul D
Thayer, Robert E
Gehman, Ken
Gehman, Teresa
Srivastava, Sudhir
Ngom, Alioune
Dakubo, Gabriel D
Parr, Ryan L
author_sort Jakupciak, John P
collection PubMed
description BACKGROUND: Mutations in the mitochondrial genome (mtgenome) have been associated with many disorders, including breast cancer. Nipple aspirate fluid (NAF) from symptomatic women could potentially serve as a minimally invasive sample for breast cancer screening by detecting somatic mutations in this biofluid. This study is aimed at 1) demonstrating the feasibility of NAF recovery from symptomatic women, 2) examining the feasibility of sequencing the entire mitochondrial genome from NAF samples, 3) cross validation of the Human mitochondrial resequencing array 2.0 (MCv2), and 4) assessing the somatic mtDNA mutation rate in benign breast diseases as a potential tool for monitoring early somatic mutations associated with breast cancer. METHODS: NAF and blood were obtained from women with symptomatic benign breast conditions, and we successfully assessed the mutation load in the entire mitochondrial genome of 19 of these women. DNA extracts from NAF were sequenced using the mitochondrial resequencing array MCv2 and by capillary electrophoresis (CE) methods as a quality comparison. Sequencing was performed independently at two institutions and the results compared. The germline mtDNA sequence determined using DNA isolated from the patient's blood (control) was compared to the mutations present in cellular mtDNA recovered from patient's NAF. RESULTS: From the cohort of 28 women recruited for this study, NAF was successfully recovered from 23 participants (82%). Twenty two (96%) of the women produced fluids from both breasts. Twenty NAF samples and corresponding blood were chosen for this study. Except for one NAF sample, the whole mtgenome was successfully amplified using a single primer pair, or three pairs of overlapping primers. Comparison of MCv2 data from the two institutions demonstrates 99.200% concordance. Moreover, MCv2 data was 99.999% identical to CE sequencing, indicating that MCv2 is a reliable method to rapidly sequence the entire mtgenome. Four NAF samples contained somatic mutations. CONCLUSION: We have demonstrated that NAF is a suitable material for mtDNA sequence analysis using the rapid and reliable MCv2. Somatic mtDNA mutations present in NAF of women with benign breast diseases could potentially be used as risk factors for progression to breast cancer, but this will require a much larger study with clinical follow up.
format Text
id pubmed-2375897
institution National Center for Biotechnology Information
language English
publishDate 2008
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-23758972008-05-10 Facile whole mitochondrial genome resequencing from nipple aspirate fluid using MitoChip v2.0 Jakupciak, John P Maggrah, Andrea Maragh, Samantha Maki, Jennifer Reguly, Brian Maki, Katrina Wittock, Roy Robinson, Kerry Wagner, Paul D Thayer, Robert E Gehman, Ken Gehman, Teresa Srivastava, Sudhir Ngom, Alioune Dakubo, Gabriel D Parr, Ryan L BMC Cancer Research Article BACKGROUND: Mutations in the mitochondrial genome (mtgenome) have been associated with many disorders, including breast cancer. Nipple aspirate fluid (NAF) from symptomatic women could potentially serve as a minimally invasive sample for breast cancer screening by detecting somatic mutations in this biofluid. This study is aimed at 1) demonstrating the feasibility of NAF recovery from symptomatic women, 2) examining the feasibility of sequencing the entire mitochondrial genome from NAF samples, 3) cross validation of the Human mitochondrial resequencing array 2.0 (MCv2), and 4) assessing the somatic mtDNA mutation rate in benign breast diseases as a potential tool for monitoring early somatic mutations associated with breast cancer. METHODS: NAF and blood were obtained from women with symptomatic benign breast conditions, and we successfully assessed the mutation load in the entire mitochondrial genome of 19 of these women. DNA extracts from NAF were sequenced using the mitochondrial resequencing array MCv2 and by capillary electrophoresis (CE) methods as a quality comparison. Sequencing was performed independently at two institutions and the results compared. The germline mtDNA sequence determined using DNA isolated from the patient's blood (control) was compared to the mutations present in cellular mtDNA recovered from patient's NAF. RESULTS: From the cohort of 28 women recruited for this study, NAF was successfully recovered from 23 participants (82%). Twenty two (96%) of the women produced fluids from both breasts. Twenty NAF samples and corresponding blood were chosen for this study. Except for one NAF sample, the whole mtgenome was successfully amplified using a single primer pair, or three pairs of overlapping primers. Comparison of MCv2 data from the two institutions demonstrates 99.200% concordance. Moreover, MCv2 data was 99.999% identical to CE sequencing, indicating that MCv2 is a reliable method to rapidly sequence the entire mtgenome. Four NAF samples contained somatic mutations. CONCLUSION: We have demonstrated that NAF is a suitable material for mtDNA sequence analysis using the rapid and reliable MCv2. Somatic mtDNA mutations present in NAF of women with benign breast diseases could potentially be used as risk factors for progression to breast cancer, but this will require a much larger study with clinical follow up. BioMed Central 2008-04-10 /pmc/articles/PMC2375897/ /pubmed/18402686 http://dx.doi.org/10.1186/1471-2407-8-95 Text en Copyright © 2008 Jakupciak et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Jakupciak, John P
Maggrah, Andrea
Maragh, Samantha
Maki, Jennifer
Reguly, Brian
Maki, Katrina
Wittock, Roy
Robinson, Kerry
Wagner, Paul D
Thayer, Robert E
Gehman, Ken
Gehman, Teresa
Srivastava, Sudhir
Ngom, Alioune
Dakubo, Gabriel D
Parr, Ryan L
Facile whole mitochondrial genome resequencing from nipple aspirate fluid using MitoChip v2.0
title Facile whole mitochondrial genome resequencing from nipple aspirate fluid using MitoChip v2.0
title_full Facile whole mitochondrial genome resequencing from nipple aspirate fluid using MitoChip v2.0
title_fullStr Facile whole mitochondrial genome resequencing from nipple aspirate fluid using MitoChip v2.0
title_full_unstemmed Facile whole mitochondrial genome resequencing from nipple aspirate fluid using MitoChip v2.0
title_short Facile whole mitochondrial genome resequencing from nipple aspirate fluid using MitoChip v2.0
title_sort facile whole mitochondrial genome resequencing from nipple aspirate fluid using mitochip v2.0
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2375897/
https://www.ncbi.nlm.nih.gov/pubmed/18402686
http://dx.doi.org/10.1186/1471-2407-8-95
work_keys_str_mv AT jakupciakjohnp facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT maggrahandrea facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT maraghsamantha facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT makijennifer facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT regulybrian facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT makikatrina facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT wittockroy facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT robinsonkerry facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT wagnerpauld facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT thayerroberte facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT gehmanken facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT gehmanteresa facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT srivastavasudhir facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT ngomalioune facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT dakubogabrield facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20
AT parrryanl facilewholemitochondrialgenomeresequencingfromnippleaspiratefluidusingmitochipv20

Ejemplares similares