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Comparison of lymphatic vessel density and expression of VEGF-C and VEGF-D lymphangiogenic factors in Warthin's tumours and oncocytic adenomas

机译:淋巴血管密度与VEGF-C和VEGF-D淋巴管生成因子在Warthin的肿瘤和鼻细胞腺瘤中的表达比较

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摘要

Objectives: To compare the density of lymphatic vessels and VEGF-C and VEGF-D expression in Warthin's tumours (WTs) and oncocytic adenomas (OCAs). Methods: Twenty three WTs and 13 OCAs of the parotid gland were analyzed. Lymphatic vessels were detected using the D2-40 antibody. For evaluation of the intratumour and peritumour lymphatic vessel density (iLVD and pLVD, respectively) the area of greatest vascularisation (hot spots) was chosen, using a ×40 field, and the number of vessels per square millimeter was counted in a ×200 field. The staining intensity for VEGF-C and VEGF-D immunoreaction in the tumour cells was graded from 0 to 3. Results: The mean iLVD and pLVD values in WTs was 4.7 (range 1-8) and 6.9 (range 3-10), those in the OCAs 1.0 (range 0-3) and 5.8 (range 2-8), respectively. The differences in the iLVD, but not pLVD between the two tumour groups were statistically significant. In both entities, the pLVD markedly outnumbered the iLVD. The intratumour vessels in the WTs were present exclusively in the lymphoid stroma. In the group of 23 WTs, 13 (56.6%), 17 (73.9%) and 10 (43.4%) samples revealed positive VEGF-C, VEGF-D and both immunoreactions, respectively. 10 of 13 (77%) cases revealed VEGF-D immunoreaction and in none of them was the VEGF-C reaction present. Conclusion: The tumours had a comparable high density of peritumorous lymphatic network. However, WTs markedly differed from OCAs in the number of the intratumorous vessels. These were abundant solely in the stroma of WT, while practically lacking in the neoplastic epithelium of the WT and relatively rare in OCAs. We suggest that homeostasis in both entities is mediated mainly by peritumorous lymphatics. The lymphatic drainage in WTs is also fostered exclusively by stromal lymphatics, whereas in stroma poor OCAs by the vessels present in their neoplastic epithelium. We also believe that WTs stimulate proliferation of pre-existing lymphatic capillaries by means of the paracrine secretion of VEGF-C and VEGF-D in the neoplastic as well as reactive stromal cells, while in the OCAs only the latter factor takes part in their lymphangiogenesis.
机译:目的:比较Warthin的肿瘤(WTS)和生用腺瘤(OCAS)中淋巴血管和VEGF-C和VEGF-D表达的密度。方法:分析了腮腺的二十三个WTS和13个OCA。使用D2-40抗体检测淋巴管血管。为了评估腹腔和腹部淋巴血管密度(分别是inlvd和plvd),选择最大的血管(热点)面积,使用×40个磁场,并且每平方毫米的血管数量计数在×200场中。肿瘤细胞VEGF-C和VEGF-D免疫反应的染色强度从0到3分梯度。结果:WTS中的平均ILVD和PLVD值为4.7(范围1-8)和6.9(范围3-10), ocas 1.0(范围0-3)和5.8(范围2-8)中的那些。两种肿瘤组之间的ILVD的差异,但不是PLVD在统计学上显着。在两个实体中,PLVD显着超过了ILVD。 WTS中的肿瘤内容血管仅在淋巴基状基质中存在。在23个WTS中,13个(56.6%),17(73.9%)和10(43.4%)样品分别显示出阳性VEGF-C,VEGF-D和两种免疫反应。 10个(77%)病例中的10例揭示了VEGF-D免疫反应,并且它们中的任何一个都是VEGF-C的反应。结论:肿瘤具有比较高密度的诱捕淋巴结网络。然而,WTS在腹部血管的数量中显着不同于OCA。这些完全在WT的基质中丰富,而实际上缺乏WT的肿瘤上皮,并且在ocas中相对罕见。我们建议两个实体的稳态主要由诱滞淋巴管介导。 WTS中的淋巴引流还由基质淋巴管促进,而在其肿瘤上皮中存在的血管基质可怜的OCAS。我们还认为WTS通过在肿瘤族和VEGF-D的旁碱基和VEGF-D在肿瘤和活性基质细胞中刺激预先存在的淋巴细胞毛细血管的增殖,而在OCAS中只有后一种因素占淋巴管发生。

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