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PAX2-null secretory cell outgrowths in the oviduct and their relationship to pelvic serous cancer

机译:输卵管中PAX2无效的分泌细胞增生及其与盆腔浆液性癌的关系

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With the exception of germ-line mutations in ovarian cancer susceptibility genes, genetic predictors for women destined for ovarian serous cancer cannot be identified in advance of malignancy. We recently showed that benign secretory cell outgrowths (SCOUTs) in the oviduct are increased in frequency with concurrent serous cancer and typically lack PAX2 expression (PAX2-null). The present study examined the relationship of PAX2-null SCOUTs to high-grade serous cancers by comparing oviducts from women with benign gynecologic conditions and high-grade serous cancers. PAX2-null SCOUTs were identified by immunostaining and computed as a function of location, frequency (F) per number of cross-sections examined, and age. Six hundred thirty-nine cross-sections from 35 serous cancers (364) and 35 controls (275) were examined. PAX2-null SCOUTs consisted of discrete linear stretches of altered epithelium ranging from cuboidal/columnar, to pseudostratified, the latter including ciliated differentiation. They were evenly distributed among proximal and fimbrial tubal sections. One hundred fourteen (F=0.31) and 45 (F=0.16) PAX2-null SCOUTs were identified in cases and controls, respectively. Mean individual case-specific frequencies for cases and controls were 0.39 and 0.14, respectively. SCOUT frequency increased significantly with age in both groups (P=0.01). However, when adjusted for age and the number of sections examined, the differences in frequency between cases and controls remained significant at P=0.006. This study supports a relationship between discrete PAX2 gene dysregulation in the oviduct and both increasing age and, more significantly, the presence of co-existing serous cancer. We propose a unique co-variable in benign oviductal epithelium—the PAX2-null SCOUT—that reflects underlying dysregulation in genes linked to serous neoplasia.
机译:除了卵巢癌易感基因中的种系突变外,无法在恶性肿瘤之前确定针对卵巢浆液性癌女性的遗传预测因子。我们最近发现,输卵管中的良性分泌细胞生长(SCOUT)与并发性浆液性癌症的发生频率增加,并且通常缺乏PAX2表达(PAX2为空)。本研究通过比较良性妇科疾病和高级别浆液性癌妇女输卵管,检查了PAX2无效SCOUT与高级别浆液性癌的关系。通过免疫染色鉴定PAX2空的SCOUT,并根据位置,每检查的横截面数的频率(F)和年龄进行计算。检查了来自35个浆液性癌(364)和35个对照(275)的639个横截面。 PAX2为空的SCOUT包括上皮改变的离散线性延伸,范围从长方体/柱状到伪分层,后者包括纤毛分化。它们均匀分布在近端和纤维状输卵管段之间。在病例和对照组中分别鉴定出一百一十四(F = 0.31)和四十五(F = 0.16)的PAX2无效SCOUT。病例和对照的平均个体病例频率分别为0.39和0.14。两组的SCOUT频率均随着年龄的增长而显着增加(P = 0.01)。但是,当根据年龄和所检查的切片数进行调整后,病例与对照组之间的频率差异仍然很明显,P = 0.006。这项研究支持输卵管中不连续的PAX2基因失调与年龄的增加以及更严重的是共存浆液性癌症的存在之间的关系。我们提出了良性输卵管上皮细胞的独特协变量-PAX2-null SCOUT-反映与浆液性瘤形成相关的基因的潜在失调。

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