Loss of Heterozygosity in Normal Tissue Adjacent to Breast Carcinomas

Deng, Guoren; Lu, Yuanzheng; Zlotnikov, Galina; Thor, Ann D.; Smith, Helene S.

doi:10.1126/science.274.5295.2057

Cited by 523 publications

(360 citation statements)

References 17 publications

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“…This study and (James et al, 1997) have confirmed that genetic changes found in DCIS lesions are similar to those found in invasive breast carcinoma. Furthermore, a recent paper has also described some changes in morphologically normal tissue adjacent to breast carcinomas (Deng et al, 1996). One significant conclusion to be drawn from this work is that, even at the preinvasive stage of DCIS, breast cancer is a heterogeneous disease in which the pathway of changes accompanying progression is far from clear.…”

Section: Discussionmentioning

confidence: 67%

Loss of heterozygosity at chromosome 9p in ductal carcinoma in situ and invasive carcinoma of the breast

Marsh

Varley²

1998

Br J Cancer

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Summary Twenty-three cases of ductal carcinoma in situ (DCIS), ten of which had an associated invasive component, were studied for loss of heterozygosity (LOH) of microsatellite markers on chromosome 9p and the results compared with a panel of 20 invasive breast carcinomas. In addition to the gene encoding p16, chromosome 9p is also thought to contain other putative tumour-suppressor genes. If the three panels of breast tumours showed LOH of markers in this region this would suggest that such putative genes were important in breast carcinogenesis. By studying both preinvasive and invasive breast tumours, it should also be possible to gain further information about the relationship between lesions of a different stage and to determine whether DCIS is indeed a precursor of invasive ductal carcinoma. Levels of LOH were low in the invasive-only set of tumours. Surprisingly, considerably higher levels of loss were observed in the tumours with an in situ component. Also, much heterogeneity was observed between different DCIS ducts or invasive tumour and DCIS from the same case.

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Section: Discussionmentioning

confidence: 67%

Loss of heterozygosity at chromosome 9p in ductal carcinoma in situ and invasive carcinoma of the breast

Marsh

Varley²

1998

Br J Cancer

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“…In surgically resected samples, extensive areas of normal epithelium were frequently present, and the relatively large microdissected foci may have contained more than one clonal or subclonal populations. Allelic losses have also been described in histologically normal epithelium adjacent to or near breast and gallbladder carcinomas (Deng et al, 1996;Wistuba et al, 1995).…”

Section: Discussionmentioning

confidence: 99%

“…Losses at other 3p regions (3p12, 3p14.2, 3p14 ± 21) and the TP53 gene were present mainly in histologically advanced lesions (dysplasia and CIS). Of interest, 3p deletions have been described as early events during the multistage pathogenesis of several other epithelial cancers including head and neck, cervix and breast (Deng et al, 1996;Wistuba et al, 1997b). In contrast, deletions at chromosome 5q and 13q (near the APC and at RB genes) were mainly associated with invasive carcinomas, and were relatively rare in precursor lesions.…”

Section: Discussionmentioning

confidence: 99%

Sequential molecular abnormalities are involved in the multistage development of squamous cell lung carcinoma

et al. 1999

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To understand the molecular pathways involved in the pathogenesis of squamous cell lung carcinoma, we obtained DNA from 94 microdissected foci from 12 archival surgically resected tumors including histologically normal epithelium (n=13), preneoplastic lesions (n=54), carcinoma is situ (CIS) (n=15) and invasive tumors (n=12). We determined loss of heterozygosity (LOH) at 10 chromosomal regions (3p12, 3p14.2, 3p14.1-21.3, 3p21, 3p22-24, 3p25, 5q22, 9p21, 13q14 RB, and 17p13 TP53) frequently deleted in lung cancer, using 31 polymorphic microsatellite markers, including 24 that spanned the entire 3p arm. Our major ®ndings are as follows: (1) Thirty one percent of histologically normal epithelium and 42% of mildly abnormal (hyperplasia/metaplasia) specimens had clones of cells with allelic loss at one or more regions; (2) There was a progressive increase of the overall LOH frequency within clones with increasing severity of histopathological changes; (3) The earliest and most frequent regions of allelic loss occurred at 3p21, 3p22-24, 3p25 and 9p21; (4) The size of the 3p deletions increased with progressive histologic changes; (5) TP53 allelic loss was present in many histologically advanced lesions (dysplasia and CIS); (6) Analyses of 58 normal and non-invasive foci having any molecular abnormality, indicated that 30 probably arose as independent clonal events, while 28 were potentially of the same clonal origin as the corresponding tumor; (7) Nevertheless, when the allelic losses in the 30 clonally independent lesions and their clonally unrelated tumors were compared the same parental allele was lost in 113 of 125 (90%) of comparisons. The mechanism by which this phenomenon (known as allele speci®c mutations) occurs is unknown; (8) Four patterns of allelic loss in clones were found. Histologically normal or mildly abnormal foci had a negative pattern (no allelic loss) or early pattern of loss while all foci of CIS and invasive tumor had an advanced pattern. However dysplasias demonstrated the entire spectrum of allelic loss patterns, and were the only histologic category having the intermediate pattern. Our ®ndings indicate that multiple, sequentially occurring allele speci®c molecular changes commence in widely dispersed, apparently clonally independent foci, early in the multistage pathogenesis of squamous cell carcinomas of the lung.

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“…In addition, recent evidence from the late Helene Smith and others have demonstrated that contiguous portions of the ductal systems in the human breast are clonally derived (Tsai et al, 1996). Further studies by this group and others have demonstrated that human mammary tumors in situ share with the surrounding normal parenchyma, common genetic mutations, suggesting that progressive malignant changes toward malignancy in the human breast, as in the mouse, occur as the result of acquired mutation in a multipotent cellular antecedent (Deng et al, 1996;Rosenberg et al, 1997). At the present time the question of whether the genetics of mouse mammary tumorigenesis is directly relevant to human breast cancer remains largely unanswered.…”

Section: The Mouse As a Model For Human Breast Cancermentioning

confidence: 99%

MMTV-induced mammary tumorigenesis: gene discovery, progression to malignancy and cellular pathways

2000

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The study of the mouse mammary tumor virus (MMTV) has provided important insights into the mechanisms of gene transcription regulation by steroid hormones, the mode of action of heritable super antigens and the progressive nature of neoplastic transformation in the mammary gland. Here we describe the current situation with respect to the latter aspect of MMTV biology and the prospects for further advance in our understanding of breast cancer in humans that may be expected from a continued study of MMTV-induced mammary neoplasia. MMTV is a heritable somatic mutagen whose target range is limited. Commonly, the tumorigenic capacity of MMTV is restricted to mammary gland, whereas infection is found in a variety of cell types. In order to replicate, proviral DNA must be inserted into the cell DNA and cell division is required to ®x the mutation. Yet only in the mammary epithelium does this lead to neoplastic transformation. This suggests a unique relationship between MMTV and mammary epithelium. In evaluating this relationship, we and others have discovered genes and potential gene pathways that are pertinent in mammary di erentiation and neoplasia. In addition, the clonal nature of these progressive events from normal to malignant phenotype has become increasingly clear. The weight of these observations compel us to conclude that mammary neoplasms arise from multipotent mammary epithelial cells through a process of acquired mutations that are re¯ected in the increasingly malignant nature of the population of progeny produced by these damaged stem cells.

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Loss of Heterozygosity in Normal Tissue Adjacent to Breast Carcinomas

Cited by 523 publications

References 17 publications

Loss of heterozygosity at chromosome 9p in ductal carcinoma in situ and invasive carcinoma of the breast

Loss of heterozygosity at chromosome 9p in ductal carcinoma in situ and invasive carcinoma of the breast

Sequential molecular abnormalities are involved in the multistage development of squamous cell lung carcinoma

MMTV-induced mammary tumorigenesis: gene discovery, progression to malignancy and cellular pathways

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