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E-cadherin to P-cadherin switching in lobular breast cancer with tubular elements

机译:e-cadherin与p-cadherin用管状元素切换小叶乳腺癌

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Loss of E-cadherin expression due to mutation of the CDH1 gene is a characteristic feature of invasive lobular breast cancer (ILBC). Beta-catenin, which binds to the cytoplasmic domain of E-cadherin, is simultaneously downregulated, reflecting disassembly of adherens junctions (AJs) and loss of cell adhesion. E-cadherin to P-cadherin expression switching can rescue AJs and cell adhesion. However, P-cadherin has not been implicated in ILBC, so far. We aimed to characterize 13 ILBCs with exceptional histomorphology, which we termed ILBCs with tubular elements. The CDH1 mutational status was determined by next generation sequencing and whole-genome copy number (CN) profiling. Expression of cadherins was assessed by immunohistochemistry. ILBCs with tubular elements were ER-positive (13/13) and HER2-negative (13/13) and harbored deleterious CDH1 mutations (11/13) accompanied by loss of heterozygosity due to deletion of chromosome 16q22.1 (9/11). E-cadherin expression was lost or reduced in noncohesive tumor cells and in admixed tubular elements (13/13). Beta-catenin expression was lost in noncohesive tumor cells, but was retained in tubular elements (11/13), indicating focal rescue of AJ formation. N-cadherin and R-cadherin were always negative (0/13). Strikingly, P-cadherin was commonly positive (12/13) and immunoreactivity was accentuated in tubular elements. Adjacent lobular carcinoma in situ (LCIS) was always P-cadherin-negative (0/7). In a reference cohort of LCIS specimens, P-cadherin was constantly not expressed (0/25). In a reference cohort of invasive mammary carcinomas, P-cadherin-positive cases (36/268, 13%) were associated with triple-negative nonlobular breast cancer (P < 0.001). Compared with ILBCs from the reference cohort, P-cadherin expression was more common in ILBCs with tubular elements (12/13 versus 7/84, P < 0.001). In summary, E-cadherin to P-cadherin switching occurs in a subset of ILBCs. P-cadherin is the molecular determinant of a mixed-appearing histomorphology in ILBCs with tubular elements.
机译:由于CDH1基因突变引起的E-Cadherin表达的丧失是侵入式小叶乳腺癌(ILBC)的特征。与E-Cadherin的细胞质结构域结合的β-连环蛋白同时下调,反射粘附结(AJS)的拆卸和细胞粘附的损失。 e-cadherin至p-cadherin表达切换可以拯救AJS和细胞粘附。然而,到目前为止,p-cadherin尚未在ILBC中涉及。我们的旨在表征13个ILBC,其具有特殊的组织组态,我们将ILBC与管状元素称为。 CDH1突变状态由下一代测序和全基因组拷贝数(CN)分析确定。通过免疫组织化学评估钙丝的表达。具有管状元素的ILBCS是ER-阳性(13/13)和HER2阴性(13/13)和题联伴有缺失染色体16Q22.1(9/11)的杂合子丧失的哈率丧失(11/13) 。在非粘性肿瘤细胞和混合的管状元素(13/13)中,e-cadherin表达丢失或减少。 β-连环蛋白表达在非粘性肿瘤细胞中丢失,但保留在管状元素(11/13)中,表明AJ形成的局灶性救助。 n-cadherin和R-cadherin总是阴性(0/13)。尖锐的是,p-cadherin通常是阳性(12/13),并且在管状元件中突出免疫反应性。原位(LCIS)相邻的小叶癌始终是p-cadherin-阴性(0/7)。在LCIS标本的参考队列中,P-Cadherin不断地表达(0/25)。在侵入性乳腺癌的参考队列中,p-cadherin-阳性病例(36/268,13%)与三负非平节乳腺癌有关(p <0.001)。与来自参考队列的ILBCS相比,P-Cadherin表达在ILBC中更常见,具有管状元件(12/13与7/84,P <0.001)。总之,在ILBCS的子集中发生E-Cadherin至p-cadherin切换。 p-cadherin是ILBCS中具有管状元件的混合出现组织形态学的分子定值。

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