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Characterization of a complex chromosome aberration in two cases of peritoneal mesothelioma arising primarily in the hernial sac.

机译:腹膜间皮瘤的两个病例中主要发生在疝囊中的复杂染色体畸变的特征。

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摘要

Malignant mesotheliomas of the hernial sac are uncommon and only a few cases have been diagnosed incidentally during herniorrhaphy procedures. The prognosis is poor and patient management is difficult because current treatment modalities do little to prolong survival. Molecular markers could be useful to identify potential therapeutic targets. Using microarray-comparative genomic hybridization (aCGH), two cases of peritoneal mesothelioma that were found incidentally at the time of hernia repair, were investigated. A high number of genetic aberrations was detected in both cases. The gains were prevalent. The tumors showed identical lost regions at 2q13, 6q25.3, 6q26, 6q26-->q27, 9q31.1-->9q31.3, 10p15.3, 11q13.2, 13q14.2, 19q13.42-->q43, and gains at 1p36.33, 3q29, 5p15.33, 7p22.3, 10p15.1-->10p14, 11q13.2, 12q24.23, 12q24.33, 16p13.3, 17p13.3, 18p11.31, 19q13.43, 21q21.1-->q21.2, 22q11.1-->q11.22, Xp21.2, Xq28. Survival was longer in the patient with a lower total number of genetic defects. aCGH provides a high-resolution map of copy number changes that may be critical to mesothelioma progression.
机译:疝囊恶性间皮瘤很少见,在疝气修补术过程中偶然发现了少数病例。由于目前的治疗方式对延长生存期几乎无济于事,因此预后不佳且患者管理困难。分子标记物可用于鉴定潜在的治疗靶标。使用微阵列比较基因组杂交(aCGH),对在疝修补时偶然发现的两例腹膜间皮瘤病例进行了调查。在两种情况下均检测到大量的遗传畸变。收益是普遍的。肿瘤在2q13、6q25.3、6q26、6q26-> q27、9q31.1-> 9q31.3、10p15.3、11q13.2、13q14.2、19q13.42-> q43处显示相同的丢失区域,并在1p36.33、3q29、5p15.33、7p22.3、10p15.1-> 10p14、11q13.2、12q24.23、12q24.33、16p13.3、17p13.3、18p11.31, 19q13.43、21q21.1-> q21.2、22q11.1-> q11.22,Xp21.2,Xq28。具有较低遗传缺陷总数的患者生存期更长。 aCGH提供了拷贝数变化的高分辨率图,这可能对间皮瘤的进展至关重要。

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