Ductal invasive G2 and G3 carcinomas of the breast are the end stages of at least two different lines of genetic evolution

Buerger, Horst; Mommers, Ellen C.M.; Littmann, Ruth; Simon, Ronald; Diallo, Raihanatou; Poremba, Christopher; Dockhorn‐Dworniczak, Barbara; Diest, Paul J. van; Boecker, Werner

doi:10.1002/path.875

Cited by 146 publications

(134 citation statements)

References 21 publications

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“…58 In an analysis of all cancers as well as in the largest subgroup of carcinomas with NST, 8p deletions were strongly linked to features of unfavorable tumor phenotype, such as advanced tumor stage, high tumor grade, rapid high tumor cell proliferation rate and poor survival. These findings are in line with previous studies reporting associations between 8p loss/LOH with adverse tumor phenotype [25][26][27][28][29] and poor clinical outcome. 25,27,29,31 Studies that could find associations of 8p deletions with tumor progression had involved remarkably small cohorts of 40, 35 44, 36 46, 33 52,38 55, 39 60, 14 61, 32 76 34 and 105 37 patients.…”

Section: Discussionsupporting

confidence: 83%

“…8p deletion typically involves extended areas or even the entire 8p arm, with several putative tumor suppressor genes which are located in this region. [17][18][19][20][21][22][23][24] Some breast cancer studies found associations between 8p deletions and advanced tumor stage, [25][26][27] highgrade, 28 metastatic growth, 25,27,29 familial breast cancer risk, 30 and poor prognosis, 25,27,29,31 but these associations could not be confirmed by others. 14,[32][33][34][35][36][37][38][39] To better understand the clinical relevance of 8p deletions in breast cancer, including association to tumor grade, pathological tumor stage, patient survival, hormone receptor status, and amplifications of HER2, MYC and CCND1, we analyzed more than 2,100 breast cancers with clinical follow-up data.…”

Section: Introductionmentioning

confidence: 75%

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8p deletion is strongly linked to poor prognosis in breast cancer

Lebok

Mittenzwei

Kluth

et al. 2015

Cancer Biology & Therapy

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Deletions of chromosome 8p occur frequently in breast cancers, but analyses of its clinical relevance have been limited to small patient cohorts and provided controversial results. A tissue microarray with 2,197 breast cancers was thus analyzed by fluorescence in-situ hybridization using an 8p21 probe in combination with a centromere 8 reference probe. 8p deletions were found in 50% of carcinomas with no special type, 67% of papillary, 28% of tubular, 37% of lobular cancers and 56% of cancers with medullary features. Deletions were always heterozygous. 8p deletion was significantly linked to advanced tumor stage (P < 0.0001), high-grade (P < 0.0001), high tumor cell proliferation (Ki67 Labeling Index; P < 0.0001), and shortened overall survival (P < 0.0001). For example, 8p deletion was seen in 32% of 290 grade 1, 43% of 438 grade 2, and 65% of 427 grade 3 cancers. In addition, 8p deletions were strongly linked to amplification of MYC (P < 0.0001), HER2 (P < 0.0001), and CCND1 (p D 0.001), but inversely associated with ER receptor expression (p D 0.0001). Remarkably, 46.5% of 8p-deleted cancers harbored amplification of at least one of the analyzed genes as compared to 27.5% amplifications in 8p-non-deleted cancers (P < 0.0001). In conclusion, 8p deletion characterizes a subset of particularly aggressive breast cancers. As 8p deletions are easy to analyze, this feature appears to be highly suited for future DNA based prognostic breast cancer panels. The strong link of 8p deletion with various gene amplifications raises the possibility of a role for regulating genomic stability.

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Section: Discussionsupporting

confidence: 83%

Section: Introductionmentioning

confidence: 75%

8p deletion is strongly linked to poor prognosis in breast cancer

Lebok

Mittenzwei

Kluth

et al. 2015

Cancer Biology & Therapy

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“…However, 216q also correlated with lower grades of malignancy and lower proliferation rates. Similar observations were made by Buerger et al 26 who found 216q and a lower mitotic activity index to be more frequent in grade II than in grade III female breast cancers. These authors proposed a cytogenetic progression model in which tumors with 216q might define a cytogenetic pathway separating grade II from grade III tumors.…”

Section: Discussionsupporting

confidence: 76%

Comparative genomic hybridization analysis on male breast cancer

Rudlowski

Schulten

Golas

et al. 2006

Intl Journal of Cancer

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The spectrum of genetic alterations in primary male breast cancer is not well established. We analyzed chromosomal imbalances in 39 tumor samples from primary male breast cancer by comparative genomic hybridization (CGH) and correlated CGH findings with clinicopathological factors. Chromosomal gains were most frequent at 1q (46%), 8q (46%), 16p (36%), 17q (36%), Xq (28%), 20q (26%) and Xp (18%). Losses were most commonly observed at 8p (36%), 16q (28%), 13q (28%), 6q (18%), 11q (18%) and 22q (18%). Gains at 16p, 20q and Xq and losses at 13q correlated significantly with higher degree of cytogenetic complexity. Significant associations with clinicopathological factors were observed for 18q and 216q with larger tumor size and 216q with lower proliferative activity and lower grade of malignancy. A comparison with reported CGH data from female breast cancer showed a similar pattern of chromosomal imbalances, including 11q, 28p, 18q, 213q, 116p, 216q, 117q and 120q. Our results indicate that male breast cancer shares a common pattern of imbalances with female breast cancer, suggesting that similar genetic events may underlie the development and progression of male and female breast cancer. ' 2005 Wiley-Liss, Inc.Key words: male breast cancer; comparative genomic hybridization; genomic aberrations Male breast cancer is an uncommon disease, accounting for 1% of all breast cancer cases. 1 The phenotypic characteristics are not well studied, and are mainly inferred from female breast cancer. Although both diseases share similarities, there are notable differences in risk factors, prognosis and survival. 2 Most male breast cancers are estrogen receptor (ER) and progesterone receptor (PR) positive 1 and expression levels of the HER-2/neu receptor are typically low. 3 The vast majority are ductal tumors and lobular tumors are rare. 4 The comparably unfavorable outcome in male breast cancer has been attributed to more advanced local tumor stages and high incidence of lymph node invasion. It has been postulated that close proximity to skin and nipple facilitates early invasion of lymph vessels, leading to earlier regional and distant metastasis. 5 Germline BRCA2 mutations account for a significant part of male breast cancer, but the majority of patients lack a known inherited predisposition. 6 As in women, axillary lymph node status, tumor size, histological grade and hormone receptor status have been proposed to be the prognostic factors in men with breast cancer. 1 Data regarding more recent molecular markers and their prognostic significance in male breast cancer are limited. The identification of genetic changes and new molecular markers in male breast cancer may provide insights into the biologic differences between male and female breast cancer patients and could aid in clinical management. 7 So far, data on the presence of specific genetic alterations in male breast cancer are limited. Most of these studies are focused on the analysis of germline mutations.No comprehensive molecular cytogenetic study on male breast ca...

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“…21 Altogether, these data supported the hypothesis that low/intermediate-and high-grade breast carcinoma develop according to distinct pathways: chromosome 16q loss was proposed as a marker of a distinct genetic pathway in breast carcinoma development. 3,7 In the present study, all but one samples were classified as G2 or G3 and only three samples were invasive lobular carcinoma. The percentage of samples showing chromosome 1q gain/16q loss was lower in G3 with respect to G2 samples.…”

Section: Discussionmentioning

confidence: 45%

“…2,5 Chromosome 1q gains and 16q losses are considered as early changes since they have been detected as the sole chromosome abnormalities in near-diploid breast carcinoma 1,6 and in well-differentiated samples with a few alterations. 3,7 These genetic changes and the resulting chromosome imbalances have been thought to play a pathogenic role in breast carcinoma development. As simultaneous chromosome 1q gains and 16q losses have often been detected, we hypothesized that they might be related with particular biopathologic characteristics.…”

mentioning

confidence: 99%

Simultaneous chromosome 1q gain and 16q loss is associated with steroid receptor presence and low proliferation in breast carcinoma

et al. 2004

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We applied comparative genomic hybridization (CGH) to 46 breast carcinoma samples, collected from 1993 to 1995, in order to detect chromosome 1q gains and 16q losses and to define whether samples showing both these alterations had distinct biopathologic features and different clinical outcome. A total of 22 samples (48%) had simultaneous chromosome 1q gain and 16q loss, which was always associated with other genetic changes. In total, 23 samples had various chromosome imbalances (including chromosome 1q gain independent of chromosome 16q loss and vice versa) and one sample did not show detectable alterations. Samples having chromosome 1q gain/16q loss were compared to the other samples with regard to neoplasm size, lymph-node status, histologic and nuclear grade, estrogen and progesterone receptor presence, Ki-67, pRB, Cyclin D1, Cyclin A, p53, p21 and p27 expression as detected by immunohistochemistry. The samples showing chromosome 1q gain/16q loss had high steroid hormone receptor expression (P ¼ 0.02), low cell growth fraction (Ki-67, P ¼ 0.03) and high p27 expression (Po0.001). No statistical correlation with disease-free survival and overall survival or response to hormonal therapy was found. We conclude that simultaneous chromosome 1q gain/16q loss is a frequent event in invasive breast cancer, which occurs in a subset of both intermediateand high-grade breast carcinomas. Although the final chromosome 1q and 16q imbalances might have originated from different chromosome alterations in low-and high-grade samples, the gene-dosage effect might be important in conferring peculiar biopathologic characteristics to this subset of samples. The cytogenetic and molecular mechanisms underlying these chromosome changes deserve further investigations.

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Ductal invasive G2 and G3 carcinomas of the breast are the end stages of at least two different lines of genetic evolution

Cited by 146 publications

References 21 publications

8p deletion is strongly linked to poor prognosis in breast cancer

8p deletion is strongly linked to poor prognosis in breast cancer

Comparative genomic hybridization analysis on male breast cancer

Simultaneous chromosome 1q gain and 16q loss is associated with steroid receptor presence and low proliferation in breast carcinoma

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