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子宫内膜癌女性的子宫包含一系列组织病理学上的单克隆假定癌前病变,其中一些存在微卫星不稳定性。

Uteri of women with endometrial carcinoma contain a histopathological spectrum of monoclonal putative precancers, some with microsatellite instability.

作者信息

Jovanovic A S, Boynton K A, Mutter G L

机构信息

Department of Pathology, Brigham and Women's Hospital, Boston, Massachusetts 02115, USA.

出版信息

Cancer Res. 1996 Apr 15;56(8):1917-21.

PMID:8620514
Abstract

We have tested the hypothesis that endometrial precancers persist in uteri of patients with endometrial carcinoma and are monoclonal. Twenty-two hysterectomies with both well-differentiated endometrial adenocarcinoma and adjacent (normal or abnormal) noncancerous endometrium underwent successful clonal analysis using a PCR assay for nonrandom X chromosome inactivation. Monoclonal lesions included endometrial carcinoma, endometrial polyps, and atypical endometrial hyperplasias, whereas normal and anovulatory endometrium were polyclonal. Comparison of the specific X chromosome copy preferentially inactivated by the matched monoclonal cancers and associated monoclonal lesions allowed us to exclude polyps, but not endometrial hyperplasias, as potential precancers. The repetitive genetic marker (HUMARA) for X inactivation was altered in some cancers, permitting identification of microsatellite instability (RER+). Two patients with RER+ cancers also had adjacent RER+ hyperplasias. The seven monoclonal and two RER+ hyperplasias had focal or diffuse cytological atypia, a feature previously associated with risk for endometrial cancer. We conclude that: (a) putative endometrial precancers and cancers share a monoclonal growth pattern; (b) cancers with microsatellite instability may acquire this feature as precancers; and (c) monoclonal endometrial precancers have the morphology of hyperplasias, which vary in the extent of cytological atypia and degree of architectural complexity.

摘要

我们验证了这样一个假说

子宫内膜癌前病变在子宫内膜癌患者的子宫中持续存在且为单克隆性。对22例患有高分化子宫内膜腺癌及相邻(正常或异常)非癌性子宫内膜的子宫切除标本,采用聚合酶链反应(PCR)检测非随机X染色体失活进行克隆分析。单克隆性病变包括子宫内膜癌、子宫内膜息肉和非典型子宫内膜增生,而正常子宫内膜和无排卵性子宫内膜为多克隆性。通过比较匹配的单克隆癌及相关单克隆病变优先失活的特定X染色体拷贝,我们排除了息肉作为潜在癌前病变的可能性,但未排除子宫内膜增生。在一些癌症中,X失活的重复性遗传标记(HUMARA)发生改变,从而得以识别微卫星不稳定性(RER+)。两名患有RER+癌症的患者其相邻的增生也为RER+。7例单克隆性增生和2例RER+增生具有局灶性或弥漫性细胞学异型性,这一特征先前被认为与子宫内膜癌风险相关。我们得出以下结论:(a)假定的子宫内膜癌前病变和癌症具有共同的单克隆生长模式;(b)具有微卫星不稳定性的癌症可能在癌前病变阶段即获得这一特征;(c)单克隆性子宫内膜癌前病变具有增生的形态,其细胞学异型程度和结构复杂程度各不相同。

相似文献

1
Uteri of women with endometrial carcinoma contain a histopathological spectrum of monoclonal putative precancers, some with microsatellite instability.子宫内膜癌女性的子宫包含一系列组织病理学上的单克隆假定癌前病变,其中一些存在微卫星不稳定性。
Cancer Res. 1996 Apr 15;56(8):1917-21.
2
Allelotype mapping of unstable microsatellites establishes direct lineage continuity between endometrial precancers and cancer.不稳定微卫星的等位基因分型确定了子宫内膜癌前病变与癌症之间的直接谱系连续性。
Cancer Res. 1996 Oct 1;56(19):4483-6.
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Molecular analysis of endometrial hyperplasia in HNPCC-suspicious patients may predict progression to endometrial carcinoma.对疑似遗传性非息肉病性结直肠癌(HNPCC)患者的子宫内膜增生进行分子分析,可能预测其进展为子宫内膜癌。
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Detection of clonality and genetic alterations in endometrial pipelle biopsy and its surgical specimen counterpart.子宫内膜吸取活检及其手术标本对应物中克隆性和基因改变的检测。
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Endometrial precancer diagnosis by histopathology, clonal analysis, and computerized morphometry.通过组织病理学、克隆分析和计算机形态测定法诊断子宫内膜癌前病变。
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A polymerase chain reaction assay for non-random X chromosome inactivation identifies monoclonal endometrial cancers and precancers.一种用于非随机X染色体失活的聚合酶链反应检测可识别单克隆子宫内膜癌和癌前病变。
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K-ras mutations appear in the premalignant phase of both microsatellite stable and unstable endometrial carcinogenesis.K-ras突变出现在微卫星稳定和不稳定的子宫内膜癌发生的癌前阶段。
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X chromosome inactivation in the normal female genital tract: implications for identification of neoplasia.正常女性生殖道中的X染色体失活:对肿瘤识别的意义。
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Sporadic microsatellite instability is specific to neoplastic and preneoplastic endometrial tissues.散发性微卫星不稳定性特定于肿瘤性和肿瘤前子宫内膜组织。
Am J Clin Pathol. 2000 Apr;113(4):576-82. doi: 10.1309/4mgm-fmrc-6awk-yqy2.

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