首页> 外文期刊>Journal of experimental & clinical cancer research : >Expressions of Lewis antigens in human non-small cell pulmonary cancer and primary liver cancer with different pathological conditions.
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Expressions of Lewis antigens in human non-small cell pulmonary cancer and primary liver cancer with different pathological conditions.

机译:Lewis抗原在不同病理条件下的人非小细胞肺癌和原发性肝癌中的表达。

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摘要

The expressions of three X series Lewis antigens, including Lewis X (Le(x)), sialyl Lewis X (SLe(x)) and sialyl dimeric Lewis X (SDLe(x)) were studied with immuno-histochemical methods in human non-small cell pulmonary cancer (NSCPC) and primary liver cancer (PLC) with different pathological conditions. The Lewis antigens are mainly expressed on the cell surfaces, medially or slightly in the cytoplasm, but not in the cell nuclei of the cancer tissues. The regions adjacent to the cancer tissues do not express any Lewis antigens. The positive rates of these antigens in NSCPC were within the range of 75% to approximately 86%. There was no apparent difference in positive rates between the cases with different differentiation and the presence or absence of metastasis in peripheral lymph nodes, nor among the three antigens, except that the positive rate of SDLe(x) was lower (about 56%) in the cases with well/medium differentiation and without metastasis. However, the expression-intensities (SI indexes) of all three antigens were significantly higher in the samples of poor differentiation and with metastasis as compared to those with well/medium differentiation and without metastasis. The two sialyl Lewis antigens increased more significantly than non-sialylated Le(x). The expressions of these antigens were also observed in the peripheral lymph nodes with metastasis, but not in those without metastasis. The positive rates of Le(x), SLe(x) and SDLe(x) in human primary liver cancer were 83.3%, 88.9% and 77.8%, respectively. In the cases with cancer cell thrombosis (CCT) in portal vein (an index of metastasis), the expressions of all these three antigens were stronger than those in the cases without CCT. SLe(x) was the most abundant and most highly increased Lewis antigen on the surface of NSCPC and PLC, especially in the cases with poor differentiation and metastasis. In the study of the enzymatic basis of the increased Lewis antigens in PLC by using Northern blot, it was found that the level of alpha1,3 FucT-III/VI mRNA in PLC tissues was much higher than that in the adjacent regions, and more significantly higher in the cancer tissues from patients with CCT in portal vein. In contrast, the expression of alpha1,3 FucT-VII was rather low in cancer tissues and not different from the adjacent regions in spite of the presence or absence of CCT. These results reveal that the SLe(x) in PLC is mainly synthesized by alpha1,3 FucT-III/VI (especially VI) and is the most important Lewis antigen involved in the metastasis of PLC.
机译:用免疫组织化学方法研究了三种X系列Lewis抗原的表达,包括Lewis X(Le(x)),唾液酸化Lewis X(SLe(x))和唾液酸二聚体Lewis X(SDLe(x))。小细胞肺癌(NSCPC)和原发性肝癌(PLC)具有不同的病理状况。 Lewis抗原主要在细胞表面表达,在细胞质中或略微表达,而不在癌症组织的细胞核中表达。与癌组织相邻的区域不表达任何路易斯抗原。这些抗原在NSCPC中的阳性率在75%至约86%的范围内。在差异分化和周围淋巴结是否存在转移的病例之间,以及在三种抗原之间,阳性率没有明显差异,只是SDLe(x)的阳性率较低(约56%)。具有良好/中等分化且无转移的病例。然而,与具有良好/中等分化且无转移的那些相比,在分化较差和具有转移的样品中所有三种抗原的表达强度(SI指数)显着更高。两种唾液酸化的Lewis抗原比未唾液酸化的Le(x)显着增加。在有转移的外周淋巴结中也观察到了这些抗原的表达,而在没有转移的外周淋巴结中没有观察到。人原发性肝癌中Le(x),SLe(x)和SDLe(x)的阳性率分别为83.3%,88.9%和77.8%。在门静脉有癌细胞血栓形成(CCT)的情况下(转移指数),这三种抗原的表达均强于没有CCT的情况。 SLe(x)是NSCPC和PLC表面上最丰富和增加最多的Lewis抗原,尤其是在分化和转移不良的情况下。利用Northern blot研究PLC中Lewis抗原增加的酶学基础,发现PLC组织中α1,3FucT-III / VI mRNA的水平远高于邻近区域,并且更多来自门静脉CCT患者的癌症组织中的癌旁组织明显更高。相反,尽管存在CCT或不存在CCT,但是α1,3 FucT-VII在癌症组织中的表达相当低,与相邻区域没有区别。这些结果表明,PLC中的SLe(x)主要由alpha1,3 FucT-III / VI(特别是VI)合成,并且是参与PLC转移的最重要的Lewis抗原。

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