Fecal expression of Escherichia coli lysine decarboxylase (LdcC) is downregulated in E-cadherin negative lobular breast carcinoma.

IF 2.2 4区 医学 Q3 PHYSIOLOGY Physiology international Pub Date : 2020-07-17 DOI:10.1556/2060.2020.00016
Zs Sári, T Kovács, T Csonka, M Török, É Sebő, J Toth, D Tóth, E Mikó, B Kiss, D Szeőcs, K Uray, Zs Karányi, I Kovács, G Méhes, P Árkosy, P Bai
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引用次数: 10

Abstract

Breast cancer is characterized by oncobiosis, the abnormal composition of the microbiome in neoplastic diseases. The biosynthetic capacity of the oncobiotic flora in breast cancer is suppressed, as suggested by metagenomic studies. The microbiome synthesizes a set of cytostatic and antimetastatic metabolites that are downregulated in breast cancer, including cadaverine, a microbiome metabolite with cytostatic properties. We set out to assess how the protein expression of constitutive lysine decarboxylase (LdcC), a key enzyme for cadaverine production, changes in the feces of human breast cancer patients (n = 35). We found that the fecal expression of Escherichia coli LdcC is downregulated in lobular cases as compared to invasive carcinoma of no special type (NST) cases. Lobular breast carcinoma is characterized by low or absent expression of E-cadherin. Fecal E. coli LdcC protein expression is downregulated in E-cadherin negative breast cancer cases as compared to positive ones. Receiver operating characteristic (ROC) analysis of LdcC expression in lobular and NST cases revealed that fecal E. coli LdcC protein expression might have predictive values. These data suggest that the oncobiotic transformation of the microbiome indeed leads to the downregulation of the production of cytostatic and antimetastatic metabolites. In E-cadherin negative lobular carcinoma that has a higher potential for metastasis formation, the protein levels of enzymes producing antimetastatic metabolites are downregulated. This finding represents a new route that renders lobular cases permissive for metastasis formation. Furthermore, our findings underline the role of oncobiosis in regulating metastasis formation in breast cancer.

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大肠杆菌赖氨酸脱羧酶(LdcC)在e -钙粘蛋白阴性的小叶乳腺癌中表达下调。
乳腺癌的特征是肿瘤菌群,肿瘤疾病中微生物组的异常组成。宏基因组学研究表明,乳腺癌中肿瘤菌群的生物合成能力受到抑制。该微生物组合成了一组在乳腺癌中下调的细胞抑制和抗转移代谢物,包括尸胺,一种具有细胞抑制特性的微生物组代谢物。我们开始评估人类乳腺癌患者粪便中组成型赖氨酸脱羧酶(LdcC)蛋白表达的变化,LdcC是产生尸胺的关键酶(n = 35)。我们发现,与无特殊类型的浸润性癌(NST)病例相比,小叶病例的粪便中大肠杆菌LdcC的表达下调。小叶型乳腺癌以e -钙粘蛋白低表达或不表达为特征。与E-cadherin阳性乳腺癌患者相比,E-cadherin阴性乳腺癌患者的粪便大肠杆菌LdcC蛋白表达下调。小叶和NST患者LdcC表达的受试者工作特征(ROC)分析显示,粪便大肠杆菌LdcC蛋白表达可能具有预测价值。这些数据表明,微生物组的共生转化确实会导致细胞抑制剂和抗转移代谢物产生的下调。在E-cadherin阴性的小叶癌中,产生抗转移代谢物的酶的蛋白质水平下调,转移形成的可能性更高。这一发现代表了一种新的途径,使得小叶病例允许转移形成。此外,我们的研究结果强调了肿瘤共生在调节乳腺癌转移形成中的作用。
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来源期刊
Physiology international
Physiology international Medicine-Physiology (medical)
CiteScore
3.40
自引率
0.00%
发文量
37
期刊介绍: The journal provides a forum for important new research papers written by eminent scientists on experimental medical sciences. Papers reporting on both original work and review articles in the fields of basic and clinical physiology, pathophysiology (from the subcellular organization level up to the oranizmic one), as well as related disciplines, including history of physiological sciences, are accepted.
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