Genome evolution during progression to breast cancer

Newburger, Daniel E.; Kashef-Haghighi, Dorna; Weng, Ziming; Salari, Raheleh; Sweeney, Robert T.; Brunner, Alayne; Zhu, Shirley; Guo, Xiangqian; Varma, Sushama; Troxell, Megan L.; West, Robert B.; Batzoglou, Serafim; Sidow, Arend

doi:10.1101/gr.151670.112

Cited by 104 publications

(126 citation statements)

References 45 publications

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“…[14][15][16][17] Accumulating evidence suggests that PIK3CA point mutations may also be common in other proliferative breast lesions such as benign papillomas and columnar cell lesions. [18][19][20][21][22][23] Prior studies have failed to identify PIK3CA mutations in histologically normal breast tissue, even with the same sensitive methods employed here. 1,8,16,19 In this study, we demonstrated a 50% frequency of PIK3CA point mutations in usual ductal hyperplasia and columnar cell lesions across 62 lesions, representing the largest series to date.…”

Section: Discussionmentioning

confidence: 93%

“…(43) Li et al 16 studied PIK3CA mutations in usual ductal hyperplasia and found no mutations in 16 lesions, in contrast to our results; the differences may be due to sample size and methodologic sensitivity, as they used less-sensitive direct Sanger sequencing. 16 The activating PIK3CA hotspot mutations seen frequently in breast cancers and proliferative lesions, most notably H1047R, E542K and, E545K, have transforming potential when overexpressed in a variety of cell culture models, [8][9][10] which arise before the most common ancestor in the genomic history of several breast carcinomas 23,44 and have thus been logically viewed as drivers of carcinogenesis. Interestingly, expression of the PIK3CA H1047R mutation at physiologic or inducible supraphysiologic levels in the mouse mammary gland leads to increased branching, duct dilation, and luminal epithelial hyperplasia.…”

Section: Discussionmentioning

confidence: 99%

“…[14][15][16][17] However, several small studies suggest that pre-neoplastic or benign breast lesions, such as papillomas, radial scars, or columnar cell lesions, may also very frequently harbor PIK3CA mutations. [18][19][20][21][22][23] The goal of this study was to systematically screen a large number of hyperplastic and putative precursor breast lesions, along with accompanying carcinomas for known activating mutations in PIK3CA and other key signaling molecules.…”

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Frequent phosphatidylinositol-3-kinase mutations in proliferative breast lesions

et al. 2014

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The phosphatidylinositol-3-kinase pathway is one of the most commonly altered molecular pathways in invasive breast carcinoma, with phosphatidylinositol-3-kinase catalytic subunit (PIK3CA) mutations in 25% of invasive carcinomas. Ductal carcinoma in situ (DCIS), benign papillomas, and small numbers of columnar cell lesions harbor an analogous spectrum of PIK3CA and AKT1 mutations, yet there is little data on usual ductal hyperplasia and atypical ductal and lobular neoplasias. We screened 192 formalin-fixed paraffin-embedded breast lesions from 75 patients for point mutations using a multiplexed panel encompassing 643 point mutations across 53 genes, including 58 PIK3CA substitutions. PIK3CA point mutations were identified in 31/62 (50%) proliferative lesions (usual ductal hyperplasia and columnar cell change), 10/14 (71%) atypical hyperplasias (atypical ductal hyperplasia and flat epithelial atypia), 7/16 (44%) lobular neoplasias (atypical lobular hyperplasia and lobular carcinoma in situ), 10/21 (48%) DCIS, and 13/37 (35%) invasive carcinomas. In genotyping multiple lesions of different stage from the same patient/specimen, we found considerable heterogeneity; most notably, in 12 specimens the proliferative lesion was PIK3CA mutant but the concurrent carcinoma was wild type. In 11 additional specimens, proliferative epithelium and cancer contained different point mutations. The frequently discordant genotypes of usual ductal hyperplasia/columnar cell change and concurrent carcinoma support a role for PIK3CA-activating point mutations in breast epithelial proliferation, perhaps more so than transformation. Further, these data suggest that proliferative breast lesions are heterogeneous and may represent non-obligate precursors of invasive carcinoma. Keywords: atypical ductal hyperplasia; breast carcinoma; columnar cell change; PIK3CA; usual ductal hyperplasia The phosphatidylinositol-3-kinase pathway is one of the most commonly mutated pathways in invasive breast carcinoma. Activating mutations in the phosphatidylinositol-3-kinase catalytic subunit (PIK3CA) are present in B25% of invasive carcinomas and are present in an even higher percentage (on the order of 40%) of low-grade estrogen receptorpositive carcinomas (luminal A intrinsic subtype). 1-10 PIK3CA mutations cluster in 'hotspots' in exon 9 (helical domain, E542K and E545K) and exon 20 (kinase domain, H1047R/L). [1][2][3][4][5][6][7][8][9][10] In addition, this pathway is activated by mutations in the plekstrinhomology domain of AKT1 in B5% of breast carcinomas, by the loss of the phosphatase PTEN (phosphatase and tensin homolog on chromosome 10), or rarely by amplification or alterations in other regulatory subunits, and is a target of active drug development. [8][9][10][11] In recent large studies of estrogen receptor-positive tumors, the presence of activating PIK3CA hotspot point mutations has been paradoxically associated with more favorable outcome as compared with breast carcinomas with wild-type PIK3CA. 3,12,13 We and other groups have previously s...

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Section: Discussionmentioning

confidence: 93%

Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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Frequent phosphatidylinositol-3-kinase mutations in proliferative breast lesions

et al. 2014

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“…S14). Evolutionary phylogenies were constructed using the somatic mutation hierarchy algorithm (20,47) in 22 patients for whom multiple tumors were interrogated by exome sequencing, using all detected somatic mutations. Enrichment of mutations within EIPs was tested using a Fisher exact test with a Bonferroni correction for multiple hypothesis testing.…”

Section: Methodsmentioning

confidence: 99%

Mutations in early follicular lymphoma progenitors are associated with suppressed antigen presentation

Green

Kihira²,

Liu³

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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Follicular lymphoma (FL) is incurable with conventional therapies and has a clinical course typified by multiple relapses after therapy. These tumors are genetically characterized by B-cell leukemia/lymphoma 2 (BCL2) translocation and mutation of genes involved in chromatin modification. By analyzing purified tumor cells, we identified additional novel recurrently mutated genes and confirmed mutations of one or more chromatin modifier genes within 96% of FL tumors and two or more in 76% of tumors. We defined the hierarchy of somatic mutations arising during tumor evolution by analyzing the phylogenetic relationship of somatic mutations across the coding genomes of 59 sequentially acquired biopsies from 22 patients. Among all somatically mutated genes, CREBBP mutations were most significantly enriched within the earliest inferable progenitor. These mutations were associated with a signature of decreased antigen presentation characterized by reduced transcript and protein abundance of MHC class II on tumor B cells, in line with the role of CREBBP in promoting class II transactivator (CIITA)-dependent transcriptional activation of these genes. CREBBP mutant B cells stimulated less proliferation of T cells in vitro compared with wild-type B cells from the same tumor. Transcriptional signatures of tumor-infiltrating T cells were indicative of reduced proliferation, and this corresponded to decreased frequencies of tumor-infiltrating CD4 helper T cells and CD8 memory cytotoxic T cells. These observations therefore implicate CREBBP mutation as an early event in FL evolution that contributes to immune evasion via decreased antigen presentation. lymphoma | exome | hierarchy | antigen presentation | CREBBP

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“…With fractions of mutated alleles evolving over time, the study of the exact mutated allele fractions, of their subclonal distribution and possible role in clonal evolution gains more importance (7)(8)(9).…”

Section: Introductionmentioning

confidence: 99%

Deep Sequencing Reveals Occurrence of Subclonal ALK Mutations in Neuroblastoma at Diagnosis

Bellini

Bernard

Leroy

et al. 2015

Clinical Cancer Research

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Purpose: In neuroblastoma, activating ALK receptor tyrosine kinase point mutations play a major role in oncogenesis. We explored the potential occurrence of ALK mutations at a subclonal level using targeted deep sequencing.Experimental Design: In a clinically representative series of 276 diagnostic neuroblastoma samples, exons 23 and 25 of the ALK gene, containing the F1174 and R1275 mutation hotspots, respectively, were resequenced with an extremely high depth of coverage.Results: At the F1174 hotspot (exon 23), mutations were observed in 15 of 277 samples (range of fraction of mutated allele per sample: 0.562%-40.409%). At the R1275 hotspot (exon 25), ALK mutations were detected in 12 of 276 samples (range of fraction of mutated allele: 0.811%-73.001%). Altogether, subclonal events with a mutated allele fraction below 20% were observed in 15/27 ALK-mutated samples. The presence of an ALK mutation was associated with poorer 5-year overall survival (OS: 75% vs. 57%, P ¼ 0.0212 log-rank test), with a strong correlation between F1174 ALK mutations and MYCN amplification being observed.Conclusions: In this series, deep sequencing allows the detection of F1174 and R1275 ALK mutational events at diagnosis in 10% of cases, with subclonal events in more than half of these, which would have gone undetected by Sanger sequencing. These findings are of clinical importance given the potential role of ALK mutations in clonal evolution and relapse. These findings also demonstrate the importance of deep sequencing techniques for the identification of patients especially when considering targeted therapy.

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Genome evolution during progression to breast cancer

Cited by 104 publications

References 45 publications

Frequent phosphatidylinositol-3-kinase mutations in proliferative breast lesions

Frequent phosphatidylinositol-3-kinase mutations in proliferative breast lesions

Mutations in early follicular lymphoma progenitors are associated with suppressed antigen presentation

Deep Sequencing Reveals Occurrence of Subclonal ALK Mutations in Neuroblastoma at Diagnosis

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