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非典型乳腺增生中单克隆微卫星改变的检测

Detection of monoclonal microsatellite alterations in atypical breast hyperplasia.

作者信息

Rosenberg C L, de las Morenas A, Huang K, Cupples L A, Faller D V, Larson P S

机构信息

Department of Pathology, Boston University School of Medicine, Massachusetts 02118, USA.

出版信息

J Clin Invest. 1996 Sep 1;98(5):1095-100. doi: 10.1172/JCI118890.

Abstract

Atypical hyperplastic (AH) breast lesions are currently classified and treated as benign proliferative disorders, but their presence is associated with a four- to fivefold increased risk of developing breast cancer. Currently, it is not known if an AH lesion is a marker of increased risk, or is itself a premalignant lesion. To investigate this question, we used a series of 15 microsatellite loci to analyze 15 separate AH lesions microdissected from the archived pathology specimens of subjects with no coincident or previous breast malignancy. We found that a significant subset (6/15, or 40%) of these AH lesions demonstrated evidence of monoclonal microsatellite alterations, both length variation and allele loss. These monoclonal alterations suggest that the AH lesion has already undergone genetic changes conferring a growth advantage. Thus, these AH lesions may actually be early neoplasms. We also noted that monoclonality characterized AH lesions in younger as compared with older women (44 vs. 59 yrs, P < 0.05) and that a subset of monoclonal lesions (4/6) demonstrated microsatellite alterations at more than one locus, suggesting that an undetermined type of genetic instability may play a role early in the development of abnormal breast proliferations. These findings contribute to our understanding of the pathogenesis of AH lesions and may have implications regarding their relationship to breast tumors.

摘要

非典型增生(AH)性乳腺病变目前被归类为良性增生性疾病并进行相应治疗,但其存在与患乳腺癌的风险增加四至五倍相关。目前尚不清楚AH病变是风险增加的标志物,还是其本身就是一种癌前病变。为了研究这个问题,我们使用了一系列15个微卫星位点,对从无同时发生或既往乳腺恶性肿瘤的受试者存档病理标本中显微切割得到的15个单独的AH病变进行分析。我们发现,这些AH病变中有相当一部分(6/15,即40%)显示出单克隆微卫星改变的证据,包括长度变异和等位基因缺失。这些单克隆改变表明AH病变已经经历了赋予生长优势的基因变化。因此,这些AH病变实际上可能是早期肿瘤。我们还注意到,与老年女性相比,单克隆性在年轻女性的AH病变中更为常见(44岁对59岁,P < 0.05),并且一部分单克隆病变(4/6)在不止一个位点显示出微卫星改变,这表明一种未确定类型的基因不稳定性可能在异常乳腺增生的早期发展中起作用。这些发现有助于我们理解AH病变的发病机制,并且可能对其与乳腺肿瘤的关系具有启示意义。

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