Signatures of post-zygotic structural genetic aberrations in the cells of histologically normal breast tissue that can predispose to sporadic breast cancer

Forsberg, Lars A.; Rasi, Chiara; Pekár, Gyula; Davies, Hanna; Piotrowski, Arkadiusz; Absher, Devin; Razzaghian, Hamid Reza; Ambicka, Aleksandra; Halaszka, Krzysztof; Przewoźnik, Marcin; Kruczak, Anna; Mandava, Geeta; Pasupulati, Saichand; Hacker, Julia; Prakash, K. Reddy; Dasari, Ravi Chandra; Lau, Joey; Penagos-Tafurt, Nelly; Olofsson, Helena; Hallberg, Gunilla; Skotnicki, Piotr; Mituś, Jerzy; Skokowski, Jarosław; Jankowski, Michał; Śrutek, Ewa; Zegarski, Wojciech; Janson, Eva Tiensuu; Ryś, Janusz; Tot, Tibor; Dumanski, Jan P.

doi:10.1101/gr.187823.114

Cited by 28 publications

(32 citation statements)

References 47 publications

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“…Interestingly, the duplicated haploid copy of chr1q in BN-T was not identical to that observed in the breast cancer samples ( Figure 3B). Although another study observed that oncogene amplification was a major factor in clonal expansion of premalignant cells (23) in the breast, this seems not to be the trigger event of premalignant cells in our study, but suggests that point mutations might be drivers of clonal expansion of premalignant cells.…”

Section: Sequencing Of Single Cells and Cell Pools Identified The Evomentioning

confidence: 54%

Coexisting genomic aberrations associated with lymph node metastasis in breast cancer

Bao¹,

Qian²,

Lyng³

et al. 2018

Journal of Clinical Investigation

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Section: Sequencing Of Single Cells and Cell Pools Identified The Evomentioning

confidence: 54%

Coexisting genomic aberrations associated with lymph node metastasis in breast cancer

Bao¹,

Qian²,

Lyng³

et al. 2018

Journal of Clinical Investigation

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“…Recently, Forsberg et al used whole genome analysis of breast cancer and adjacent histologically normal tissues (uninvolved margins at varying distances) to demonstrate that the most common genomic abnormality in adjacent normal tissue was a gain in gene copy number of ERBB2. Following ERBB2 genomic amplification, amplification of other growth factor receptor genes (EGFR, FGFR1, IGF1R, LIFR, and NGFR) were the most frequent genetic aberrations [52]. The above studies provide compelling evidence that the presence of genomic instability and specific cancer-related chromosomal aberrations are often present in histologically normal tissue adjacent to breast tumors.…”

Section: Cancer-like Alterations In Tumor Adjacent Histologically Normentioning

confidence: 99%

Towards a personalized surgical margin for breast conserving surgery—Implications of field cancerization in local recurrence

Lebya

Garcia-Smith

Swaminathan³

et al. 2017

Journal of Surgical Oncology

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The amount of normal tissue that should be excised during breast conserving surgery is widely debated. Tissue adjacent to breast tumors, although histologically normal, possesses many of the molecular abnormalities found in tumor tissues. Here, we propose that the ideal physical distance for a surgical margin may not be universal. Rather, an adequate surgical margin likely varies from patient to patient, depending on the biology of the tissue that remains after surgery. J. Surg. Oncol. 2017;115:109-115. © 2017 Wiley Periodicals, Inc.

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“…For example, sequencing data from a large-scale case-control study suggests mosaic protein truncating mutations in PPM1D may be a risk factor for breast and ovarian cancer[58], although further prospective studies are needed to verify this relationship. Additionally, a recent investigation of uninvolved margin tissue from breast cancer cases suggests mosaic copy number aberrations are present in over a third of cases and often include mosaic gains of ERBB2 and growth factor receptor genes[59]. Better understanding which events are important for future disease risk and the penetrance of such events will be important as the field moves forward in assessing clonal mosaicism as markers of risk for common diseases.…”

Section: Detection Of Genetic Mosaicism As a Biomarkermentioning

confidence: 99%

The ageing genome, clonal mosaicism and chronic disease

Machiela

Chanock

2017

Current Opinion in Genetics & Development

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Clonal mosaicism arises when a post-zygotic mutational event is detectable in subpopulations of cells as an alternative genotype while not present in the germline genome. Although described in a subset of pediatric disorders, new genomic technologies have detected higher than anticipated frequencies of clonal mosaicism in adult population studies, stimulating investigation as to how clonal mosaicism could contribute to chronic human diseases, such as cancer, diabetes and neurodegenerative disorders. It has also been postulated to be an important mechanism for functional cellular diversity, including the brain. Early studies have characterized the spectrum of detectable mosaic alterations and have begun to investigate whether detectable mosaicism could be important as an overall biomarker for risk or in the case of hematologic cancers, identification of preleukemic clones.

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Signatures of post-zygotic structural genetic aberrations in the cells of histologically normal breast tissue that can predispose to sporadic breast cancer

Cited by 28 publications

References 47 publications

Coexisting genomic aberrations associated with lymph node metastasis in breast cancer

Coexisting genomic aberrations associated with lymph node metastasis in breast cancer

Towards a personalized surgical margin for breast conserving surgery—Implications of field cancerization in local recurrence

The ageing genome, clonal mosaicism and chronic disease

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