Initiation of genome instability and preneoplastic processes through loss of Fhit expression.

Initiation of genome instability and preneoplastic processes through loss of Fhit expression.

Genomic instability drives tumorigenesis, but how it is initiated in sporadic neoplasias is unknown. In early preneoplasias, alterations at chromosome fragile sites arise due to DNA replication stress. A frequent, perhaps earliest, genetic alteration in preneoplasias is deletion within the fragile F...

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Main Authors: Joshua C Saldivar, Satoshi Miuma, Jessica Bene, Seyed Ali Hosseini, Hidetaka Shibata, Jin Sun, Linda J Wheeler, Christopher K Mathews, Kay Huebner
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC3510054?pdf=render
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spelling doaj-0438ea136d22470fb814e9264ecf03362020-11-24T22:04:57ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042012-01-01811e100307710.1371/journal.pgen.1003077Initiation of genome instability and preneoplastic processes through loss of Fhit expression.Joshua C SaldivarSatoshi MiumaJessica BeneSeyed Ali HosseiniHidetaka ShibataJin SunLinda J WheelerChristopher K MathewsKay HuebnerGenomic instability drives tumorigenesis, but how it is initiated in sporadic neoplasias is unknown. In early preneoplasias, alterations at chromosome fragile sites arise due to DNA replication stress. A frequent, perhaps earliest, genetic alteration in preneoplasias is deletion within the fragile FRA3B/FHIT locus, leading to loss of Fhit protein expression. Because common chromosome fragile sites are exquisitely sensitive to replication stress, it has been proposed that their clonal alterations in cancer cells are due to stress sensitivity rather than to a selective advantage imparted by loss of expression of fragile gene products. Here, we show in normal, transformed, and cancer-derived cell lines that Fhit-depletion causes replication stress-induced DNA double-strand breaks. Using DNA combing, we observed a defect in replication fork progression in Fhit-deficient cells that stemmed primarily from fork stalling and collapse. The likely mechanism for the role of Fhit in replication fork progression is through regulation of Thymidine kinase 1 expression and thymidine triphosphate pool levels; notably, restoration of nucleotide balance rescued DNA replication defects and suppressed DNA breakage in Fhit-deficient cells. Depletion of Fhit did not activate the DNA damage response nor cause cell cycle arrest, allowing continued cell proliferation and ongoing chromosomal instability. This finding was in accord with in vivo studies, as Fhit knockout mouse tissue showed no evidence of cell cycle arrest or senescence yet exhibited numerous somatic DNA copy number aberrations at replication stress-sensitive loci. Furthermore, cells established from Fhit knockout tissue showed rapid immortalization and selection of DNA deletions and amplifications, including amplification of the Mdm2 gene, suggesting that Fhit loss-induced genome instability facilitates transformation. We propose that loss of Fhit expression in precancerous lesions is the first step in the initiation of genomic instability, linking alterations at common fragile sites to the origin of genome instability.http://europepmc.org/articles/PMC3510054?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Joshua C Saldivar
Satoshi Miuma
Jessica Bene
Seyed Ali Hosseini
Hidetaka Shibata
Jin Sun
Linda J Wheeler
Christopher K Mathews
Kay Huebner
spellingShingle Joshua C Saldivar
Satoshi Miuma
Jessica Bene
Seyed Ali Hosseini
Hidetaka Shibata
Jin Sun
Linda J Wheeler
Christopher K Mathews
Kay Huebner
Initiation of genome instability and preneoplastic processes through loss of Fhit expression.
PLoS Genetics
author_facet Joshua C Saldivar
Satoshi Miuma
Jessica Bene
Seyed Ali Hosseini
Hidetaka Shibata
Jin Sun
Linda J Wheeler
Christopher K Mathews
Kay Huebner
author_sort Joshua C Saldivar
title Initiation of genome instability and preneoplastic processes through loss of Fhit expression.
title_short Initiation of genome instability and preneoplastic processes through loss of Fhit expression.
title_full Initiation of genome instability and preneoplastic processes through loss of Fhit expression.
title_fullStr Initiation of genome instability and preneoplastic processes through loss of Fhit expression.
title_full_unstemmed Initiation of genome instability and preneoplastic processes through loss of Fhit expression.
title_sort initiation of genome instability and preneoplastic processes through loss of fhit expression.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2012-01-01
description Genomic instability drives tumorigenesis, but how it is initiated in sporadic neoplasias is unknown. In early preneoplasias, alterations at chromosome fragile sites arise due to DNA replication stress. A frequent, perhaps earliest, genetic alteration in preneoplasias is deletion within the fragile FRA3B/FHIT locus, leading to loss of Fhit protein expression. Because common chromosome fragile sites are exquisitely sensitive to replication stress, it has been proposed that their clonal alterations in cancer cells are due to stress sensitivity rather than to a selective advantage imparted by loss of expression of fragile gene products. Here, we show in normal, transformed, and cancer-derived cell lines that Fhit-depletion causes replication stress-induced DNA double-strand breaks. Using DNA combing, we observed a defect in replication fork progression in Fhit-deficient cells that stemmed primarily from fork stalling and collapse. The likely mechanism for the role of Fhit in replication fork progression is through regulation of Thymidine kinase 1 expression and thymidine triphosphate pool levels; notably, restoration of nucleotide balance rescued DNA replication defects and suppressed DNA breakage in Fhit-deficient cells. Depletion of Fhit did not activate the DNA damage response nor cause cell cycle arrest, allowing continued cell proliferation and ongoing chromosomal instability. This finding was in accord with in vivo studies, as Fhit knockout mouse tissue showed no evidence of cell cycle arrest or senescence yet exhibited numerous somatic DNA copy number aberrations at replication stress-sensitive loci. Furthermore, cells established from Fhit knockout tissue showed rapid immortalization and selection of DNA deletions and amplifications, including amplification of the Mdm2 gene, suggesting that Fhit loss-induced genome instability facilitates transformation. We propose that loss of Fhit expression in precancerous lesions is the first step in the initiation of genomic instability, linking alterations at common fragile sites to the origin of genome instability.
url http://europepmc.org/articles/PMC3510054?pdf=render
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