Early embryonic chromosome instability results in stable mosaic pattern in human tissues.

Early embryonic chromosome instability results in stable mosaic pattern in human tissues.

The discovery of copy number variations (CNV) in the human genome opened new perspectives on the study of the genetic causes of inherited disorders and the aetiology of common diseases. Here, a single-cell-level investigation of CNV in different human tissues led us to uncover the phenomenon of mito...

Full description

Bibliographic Details
Main Authors: Hasmik Mkrtchyan, Madeleine Gross, Sophie Hinreiner, Anna Polytiko, Marina Manvelyan, Kristin Mrasek, Nadezda Kosyakova, Elisabeth Ewers, Heike Nelle, Thomas Liehr, Marianne Volleth, Anja Weise
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2010-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2834743?pdf=render
id doaj-0716b224f2244967a53e5195644499f0
record_format Article
spelling doaj-0716b224f2244967a53e5195644499f02020-11-25T00:55:40ZengPublic Library of Science (PLoS)PLoS ONE1932-62032010-01-0153e959110.1371/journal.pone.0009591Early embryonic chromosome instability results in stable mosaic pattern in human tissues.Hasmik MkrtchyanMadeleine GrossSophie HinreinerAnna PolytikoMarina ManvelyanKristin MrasekNadezda KosyakovaElisabeth EwersHeike NelleThomas LiehrMarianne VollethAnja WeiseThe discovery of copy number variations (CNV) in the human genome opened new perspectives on the study of the genetic causes of inherited disorders and the aetiology of common diseases. Here, a single-cell-level investigation of CNV in different human tissues led us to uncover the phenomenon of mitotically derived genomic mosaicism, which is stable in different cell types of one individual. The CNV mosaic ratios were different between the 10 individuals studied. However, they were stable in the T lymphocytes, immortalized B lymphoblastoid cells, and skin fibroblasts analyzed in each individual. Because these cell types have a common origin in the connective tissues, we suggest that mitotic changes in CNV regions may happen early during embryonic development and occur only once, after which the stable mosaic ratio is maintained throughout the differentiated tissues. This concept is further supported by a unique study of immortalized B lymphoblastoid cell lines obtained with 20 year difference from two subjects. We provide the first evidence of somatic mosaicism for CNV, with stable variation ratios in different cell types of one individual leading to the hypothesis of early embryonic chromosome instability resulting in stable mosaic pattern in human tissues. This concept has the potential to open new perspectives in personalized genetic diagnostics and can explain genetic phenomena like diminished penetrance in autosomal dominant diseases. We propose that further genomic studies should focus on the single-cell level, to better understand the aetiology of aging and diseases mediated by somatic mutations.http://europepmc.org/articles/PMC2834743?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Hasmik Mkrtchyan
Madeleine Gross
Sophie Hinreiner
Anna Polytiko
Marina Manvelyan
Kristin Mrasek
Nadezda Kosyakova
Elisabeth Ewers
Heike Nelle
Thomas Liehr
Marianne Volleth
Anja Weise
spellingShingle Hasmik Mkrtchyan
Madeleine Gross
Sophie Hinreiner
Anna Polytiko
Marina Manvelyan
Kristin Mrasek
Nadezda Kosyakova
Elisabeth Ewers
Heike Nelle
Thomas Liehr
Marianne Volleth
Anja Weise
Early embryonic chromosome instability results in stable mosaic pattern in human tissues.
PLoS ONE
author_facet Hasmik Mkrtchyan
Madeleine Gross
Sophie Hinreiner
Anna Polytiko
Marina Manvelyan
Kristin Mrasek
Nadezda Kosyakova
Elisabeth Ewers
Heike Nelle
Thomas Liehr
Marianne Volleth
Anja Weise
author_sort Hasmik Mkrtchyan
title Early embryonic chromosome instability results in stable mosaic pattern in human tissues.
title_short Early embryonic chromosome instability results in stable mosaic pattern in human tissues.
title_full Early embryonic chromosome instability results in stable mosaic pattern in human tissues.
title_fullStr Early embryonic chromosome instability results in stable mosaic pattern in human tissues.
title_full_unstemmed Early embryonic chromosome instability results in stable mosaic pattern in human tissues.
title_sort early embryonic chromosome instability results in stable mosaic pattern in human tissues.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2010-01-01
description The discovery of copy number variations (CNV) in the human genome opened new perspectives on the study of the genetic causes of inherited disorders and the aetiology of common diseases. Here, a single-cell-level investigation of CNV in different human tissues led us to uncover the phenomenon of mitotically derived genomic mosaicism, which is stable in different cell types of one individual. The CNV mosaic ratios were different between the 10 individuals studied. However, they were stable in the T lymphocytes, immortalized B lymphoblastoid cells, and skin fibroblasts analyzed in each individual. Because these cell types have a common origin in the connective tissues, we suggest that mitotic changes in CNV regions may happen early during embryonic development and occur only once, after which the stable mosaic ratio is maintained throughout the differentiated tissues. This concept is further supported by a unique study of immortalized B lymphoblastoid cell lines obtained with 20 year difference from two subjects. We provide the first evidence of somatic mosaicism for CNV, with stable variation ratios in different cell types of one individual leading to the hypothesis of early embryonic chromosome instability resulting in stable mosaic pattern in human tissues. This concept has the potential to open new perspectives in personalized genetic diagnostics and can explain genetic phenomena like diminished penetrance in autosomal dominant diseases. We propose that further genomic studies should focus on the single-cell level, to better understand the aetiology of aging and diseases mediated by somatic mutations.
url http://europepmc.org/articles/PMC2834743?pdf=render
work_keys_str_mv AT hasmikmkrtchyan earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT madeleinegross earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT sophiehinreiner earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT annapolytiko earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT marinamanvelyan earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT kristinmrasek earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT nadezdakosyakova earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT elisabethewers earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT heikenelle earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT thomasliehr earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT mariannevolleth earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
AT anjaweise earlyembryonicchromosomeinstabilityresultsinstablemosaicpatterninhumantissues
_version_ 1725229996336742400

Similar Items