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首页> 外文期刊>World Journal of Gastroenterology >Use of lectin microarray to differentiate gastric cancer from gastric ulcer
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Use of lectin microarray to differentiate gastric cancer from gastric ulcer

机译:凝集素微阵列在区分胃癌和胃溃疡中的应用

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AIM: To investigate the feasibility of lectin microarray for differentiating gastric cancer from gastric ulcer. METHODS: Twenty cases of human gastric cancer tissue and 20 cases of human gastric ulcer tissue were collected and processed. Protein was extracted from the frozen tissues and stored. The lectins were dissolved in buffer, and the sugar-binding specificities of lectins and the layout of the lectin microarray were summarized. The median of the effective data points for each lectin was globally normalized to the sum of medians of all effective data points for each lectin in one block. Formalin-fixed paraffin-embedded gastric cancer tissues and their corresponding gastric ulcer tissues were subjected to Ag retrieval. Biotinylated lectin was used as the primary antibody and HRP-streptavidin as the secondary antibody. The glycopatterns of glycoprotein in gastric cancer and gastric ulcer specimens were determined by lectin microarray, and then validated by lectin histochemistry. Data are presented as mean ± SD for the indicated number of independent experiments. RESULTS: The glycosylation level of gastric cancer was significantly higher than that in ulcer. In gastric cancer, most of the lectin binders showed positive signals and the intensity of the signals was stronger, whereas the opposite was the case for ulcers. Significant differences in the pathological score of the two lectins were apparent between ulcer and gastric cancer tissues using the same lectin. For MPL and VVA, all types of gastric cancer detected showed stronger staining and a higher positive rate in comparison with ulcer, especially in the case of signet ring cell carcinoma and intra-mucosal carcinoma. GalNAc bound to MPL showed a significant increase. A statistically significant association between MPL and gastric cancer was observed. As with MPL, there were significant differences in VVA staining between gastric cancer and ulcer. CONCLUSION: Lectin microarray can differentiate the different glycopatterns in gastric cancer and gastric ulcer, and the lectins MPL and VVA can be used as biomarkers.
机译:目的:探讨凝集素微阵列鉴别胃癌与胃溃疡的可行性。方法:收集并处理20例人胃癌组织和20例人胃溃疡组织。从冷冻组织中提取蛋白质并储存。将凝集素溶解在缓冲液中,总结了凝集素的糖结合特异性和凝集素微阵列的布局。将每种凝集素的有效数据点的中位数全局标准化为一个块中每种凝集素的所有有效数据点的中值之和。将福尔马林固定石蜡包埋的胃癌组织及其相应的胃溃疡组织进行Ag取出。使用生物素化的凝集素作为一抗,使用HRP-链霉亲和素作为二抗。用凝集素微阵列测定胃癌和胃溃疡标本中糖蛋白的糖模式,然后用凝集素组织化学方法进行验证。数据表示为指定数量的独立实验的平均值±SD。结果:胃癌的糖基化水平明显高于溃疡患者。在胃癌中,大多数凝集素结合剂均显示阳性信号,且信号强度更强,而溃疡则相反。使用相同的凝集素,在溃疡组织和胃癌组织之间,两种凝集素的病理评分存在明显差异。对于MPL和VVA,与溃疡相比,检测到的所有类型的胃癌均表现出更强的染色和更高的阳性率,特别是在印戒细胞癌和粘膜内癌的情况下。与MPL结合的GalNAc显着增加。观察到MPL与胃癌之间的统计学显着相关性。与MPL一样,胃癌和溃疡之间VVA染色也有显着差异。结论:凝集素微阵列可以区分胃癌和胃溃疡中的不同糖模式,凝集素MPL和VVA可作为生物标志物。

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