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胆汁酸在癌变中的作用。

The role of bile acids in carcinogenesis.

机构信息

Centre for Functional Genomics and Bio-Chips, Institute of Biochemistry and Molecular Genetics, Faculty of Medicine, University of Ljubljana, Ljubljana, Slovenia.

Department of Medical Chemistry, University of Debrecen, Egyetem tér 1., Debrecen, 4032, Hungary.

出版信息

Cell Mol Life Sci. 2022 Apr 16;79(5):243. doi: 10.1007/s00018-022-04278-2.

Abstract

Bile acids are soluble derivatives of cholesterol produced in the liver that subsequently undergo bacterial transformation yielding a diverse array of metabolites. The bulk of bile acid synthesis takes place in the liver yielding primary bile acids; however, other tissues have also the capacity to generate bile acids (e.g. ovaries). Hepatic bile acids are then transported to bile and are subsequently released into the intestines. In the large intestine, a fraction of primary bile acids is converted to secondary bile acids by gut bacteria. The majority of the intestinal bile acids undergo reuptake and return to the liver. A small fraction of secondary and primary bile acids remains in the circulation and exert receptor-mediated and pure chemical effects (e.g. acidic bile in oesophageal cancer) on cancer cells. In this review, we assess how changes to bile acid biosynthesis, bile acid flux and local bile acid concentration modulate the behavior of different cancers. Here, we present in-depth the involvement of bile acids in oesophageal, gastric, hepatocellular, pancreatic, colorectal, breast, prostate, ovarian cancer. Previous studies often used bile acids in supraphysiological concentration, sometimes in concentrations 1000 times higher than the highest reported tissue or serum concentrations likely eliciting unspecific effects, a practice that we advocate against in this review. Furthermore, we show that, although bile acids were classically considered as pro-carcinogenic agents (e.g. oesophageal cancer), the dogma that switch, as lower concentrations of bile acids that correspond to their serum or tissue reference concentration possess anticancer activity in a subset of cancers. Differences in the response of cancers to bile acids lie in the differential expression of bile acid receptors between cancers (e.g. FXR vs. TGR5). UDCA, a bile acid that is sold as a generic medication against cholestasis or biliary surge, and its conjugates were identified with almost purely anticancer features suggesting a possibility for drug repurposing. Taken together, bile acids were considered as tumor inducers or tumor promoter molecules; nevertheless, in certain cancers, like breast cancer, bile acids in their reference concentrations may act as tumor suppressors suggesting a Janus-faced nature of bile acids in carcinogenesis.

摘要

胆汁酸是肝脏中产生的胆固醇可溶性衍生物,随后经历细菌转化生成多种代谢物。大部分胆汁酸合成发生在肝脏中,产生初级胆汁酸;然而,其他组织也有生成胆汁酸的能力(例如卵巢)。然后,肝脏中的胆汁酸被转运到胆汁中,并随后释放到肠道中。在大肠中,一部分初级胆汁酸被肠道细菌转化为次级胆汁酸。大部分肠道胆汁酸被重吸收并返回肝脏。一小部分次级和初级胆汁酸仍在循环中,并对癌细胞发挥受体介导和纯化学作用(例如食管癌中的酸性胆汁)。在这篇综述中,我们评估了胆汁酸生物合成、胆汁酸流量和局部胆汁酸浓度的变化如何调节不同癌症的行为。在这里,我们深入探讨了胆汁酸在食管癌、胃癌、肝细胞癌、胰腺癌、结直肠癌、乳腺癌、前列腺癌、卵巢癌中的作用。以前的研究经常使用高于生理浓度的胆汁酸,有时甚至使用比最高报道的组织或血清浓度高 1000 倍的浓度,可能会引起非特异性作用,我们在本综述中反对这种做法。此外,我们表明,尽管胆汁酸通常被认为是致癌物质(例如食管癌),但低浓度的胆汁酸具有抗癌活性,这一观点在某些癌症中已经得到了验证。这种观点的转变是由于不同癌症之间胆汁酸受体的表达不同(例如 FXR 与 TGR5)。UDCA 是一种作为治疗胆汁淤积或胆管炎的通用药物出售的胆汁酸及其结合物,具有几乎完全的抗癌特性,这表明药物再利用的可能性。综上所述,胆汁酸被认为是肿瘤诱导或肿瘤促进分子;然而,在某些癌症中,如乳腺癌,参考浓度的胆汁酸可能作为肿瘤抑制物发挥作用,这表明胆汁酸在致癌作用中具有两面性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d564/11072446/c1369cbc6a1a/18_2022_4278_Fig1_HTML.jpg

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