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巴雷特食管隐窝基底和表层区域的DNA倍体异常及相关肿瘤性病变。

DNA ploidy abnormalities in basal and superficial regions of the crypts in Barrett's esophagus and associated neoplastic lesions.

作者信息

Zhang Xiaoqi, Huang Qin, Goyal Raj K, Odze Robert D

机构信息

Departments of Medicine, Veterans Affairs Boston Healthcare System, Harvard Medical School, West Roxbury, MA 02132, USA.

出版信息

Am J Surg Pathol. 2008 Sep;32(9):1327-35. doi: 10.1097/PAS.0b013e31816b6459.

Abstract

The purpose of this study was to define the zonal DNA content distribution in the basal versus the superficial crypt cells in Barrett's esophagus (BE) and related neoplastic lesions. One hundred and five tissue sections of BE patients and 12 gastric tissue section as controls were stained with hematoxylin-eosin and Feulgen and high-fidelity DNA histograms were generated from whole crypts (n=117) and also separately from the basal and superficial portions of the crypts (n=71). Three parameters were analyzed: (1) peak DNA index (DI), classified into diploidy (DI=0.9-1.1) or aneuploidy (DI>1.1), the latter of which was further divided into 3 types: mild (DI=1.1-1.3), moderate (DI=1.3-1.8), and severe (DI>1.8). (2) Heterogeneity index (HI), representing groups of cells with different DNA content. (3) Percentage of cells with DI exceeding 5N rate (5N-ER). In full crypts, compared with gastric controls, the prevalence of DNA aneuploidy increased significantly (P<0.01) from nondysplastic BE to basal crypt dysplasia (BCD), low-grade dysplasia (LGD), high-grade dysplasia (HGD), and adenocarcinoma (AC). Nondysplastic BE, BCD, and LGD had mostly mild aneuploidy, and the majority of HGD and AC had either moderate or severe aneuploidy. In addition, both HI and 5N-ER increased progressively from BCD and LGD to HGD and AC (P<0.01). When analyzed separately, the superficial crypt cells were diploid in nondysplastic BE and BCD, but were aneuploid in 50% of LGD and 100% of HGD cases. In contrast, basal crypt cells were aneuploid in 37% of nondysplastic BE, 50% of BCD, 73% of LGD, and 100% of HGD cases. A similar progressive increase in the HI and 5N-ER values in basal crypt cells was observed with dysplastic progression. The changes in DNA ploidy profiles of basal crypt cells in BCD and LGD were remarkably similar. These results suggest that with neoplastic progression, dysplastic changes in BE begin in the basal crypt cells and then extend further up the crypts, and BCD represents a true early form of dysplasia limited to the crypt bases.

摘要

本研究的目的是确定巴雷特食管(BE)及相关肿瘤性病变中,隐窝基底细胞与表层细胞的区域DNA含量分布情况。对105例BE患者的组织切片和12例作为对照的胃组织切片进行苏木精-伊红染色和福尔根染色,并从完整隐窝(n = 117)以及隐窝的基底部分和表层部分分别生成高保真DNA直方图(n = 71)。分析了三个参数:(1)峰值DNA指数(DI),分为二倍体(DI = 0.9 - 1.1)或非整倍体(DI>1.1),后者进一步分为3种类型:轻度(DI = 1.1 - 1.3)、中度(DI = 1.3 - 1.8)和重度(DI>1.8)。(2)异质性指数(HI),代表具有不同DNA含量的细胞群。(3)DI超过5N率(5N - ER)的细胞百分比。在完整隐窝中,与胃对照组相比,从无异型增生的BE到基底隐窝异型增生(BCD)、低级别异型增生(LGD)、高级别异型增生(HGD)和腺癌(AC),DNA非整倍体的患病率显著增加(P<0.01)。无异型增生的BE、BCD和LGD大多为轻度非整倍体,而大多数HGD和AC为中度或重度非整倍体。此外,HI和5N - ER从BCD和LGD到HGD和AC均逐渐增加(P<0.01)。单独分析时,在无异型增生的BE和BCD中,表层隐窝细胞为二倍体,但在50%的LGD和100%的HGD病例中为非整倍体。相比之下,在37%的无异型增生的BE、50%的BCD、

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