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High-grade prostate intraepithelial neoplasia shares cytogenetic alterations with invasive prostate cancer.

机译:高度前列腺上皮内瘤变与浸润性前列​​腺癌共享细胞遗传学改变。

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BACKGROUND: High-grade prostate intraepithelial neoplasia (PIN) is the most likely precursor of prostate adenocarcinoma. However, the relationship between this lesion and prostate cancer has not yet been established. The detection of cytogenetic changes in the lesions prior to prostate adenocarcinoma would be useful in demonstrating such a pathogenic relationship. METHODS: Twenty eight high-grade PIN cases were found among 57 specimens of radical prostatectomy performed for clinically localized prostate cancer. Fluorescence in situ hybridization (FISH) analysis using centromeric probes to enumerate chromosomes 7, 8, 10, and 12 was performed to study the numerical chromosome alterations. FISH analysis was carried out over isolated nuclei obtained from high-grade PIN areas and prostate cancer foci in the same prostatectomy specimen. RESULTS: Of the 28 suitable cases it was possible to complete the study in 26 tumor and 20 PIN areas. The remaining cases were excluded because of insufficient tissue or poor preservation. Cytogenetic alterations (aneuploidy) were found in 16 of the 26 (62%) tumors studied. The most frequent chromosome alteration was trisomy 7, detected in 12 (75%) aneuploid tumors, followed by monosomy 8 present in 5 (31%) aneuploid tumors. Trisomy 7 was also the most frequent isolated chromosome alteration since it was detected in 7 (44%) tumors. Thirteen of 20 (65%) PIN cases were aneuploid when studied by FISH. Trisomy 7, trisomy 8, and monosomy 8 were the most common cytogenetic alterations in the 20 PIN areas studied, being observed in nine (45%), six (30%), and four (20%) cases, respectively. FISH analysis showed a high correlation (75% cases) in ploidy and pattern of cytogenetic alterations between high-grade PIN areas and the paired prostate cancer focus in the same specimen. CONCLUSIONS: The above results show a cytogenetic link between high-grade PIN and prostate cancer, suggesting that the former could be an early form of prostate cancer.
机译:背景:高度前列腺上皮内瘤变(PIN)是最可能的前列腺腺癌前体。然而,该病灶与前列腺癌之间的关系尚未建立。在前列腺腺癌之前的病变中检测细胞遗传学变化将有助于证明这种致病关系。方法:在57例行前列腺癌根治术的标本中,发现了28例高等级PIN病例。进行荧光原位杂交(FISH)分析,使用着丝粒探针枚举7、8、10和12号染色体,以研究染色体的数字变化。在同一前列腺切除术标本中,对从高级PIN区域和前列腺癌灶获得的孤立核进行了FISH分析。结果:在28个合适的病例中,有可能在26个肿瘤和20个PIN区域完成研究。由于组织不足或保存不良,将其余病例排除在外。在研究的26种肿瘤中的16种(62%)中发现了细胞遗传学改变(非整倍性)。最常见的染色体改变是在12个(75%)非整倍性肿瘤中检测到7三体性,然后在5个(31%)非整倍性肿瘤中出现8号三体性。三体性7也是最常见的分离染色体改变,因为它在7个(44%)肿瘤中被检测到。通过FISH研究时,在20例PIN病例中有13例(65%)为非整倍体。三体性7,三体性8和单体性8是研究的20个PIN区域中最常见的细胞遗传学改变,分别在9例(45%),6例(30%)和4例(20%)病例中观察到。 FISH分析显示,在同一标本中,高级PIN区域与配对的前列腺癌病灶之间的倍性和细胞遗传学改变模式具有高度相关性(75%病例)。结论:以上结果表明高级PIN与前列腺癌之间存在细胞遗传学联系,这表明前者可能是前列腺癌的早期形式。

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