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Basonuclin-2 调节细胞外基质的产生和降解。

Basonuclin-2 regulates extracellular matrix production and degradation.

机构信息

Centre for Cancer Biology, An Alliance of SA Pathology and University of South Australia, Adelaide, Australia.

Division of Bioinformatics, Walter and Eliza Hall Institute of Medical Research, Parkville, Australia.

出版信息

Life Sci Alliance. 2023 Aug 3;6(10). doi: 10.26508/lsa.202301984. Print 2023 Oct.

Abstract

Epithelial-mesenchymal transition is essential for tissue patterning and organization. It involves both regulation of cell motility and alterations in the composition and organization of the ECM-a complex environment of proteoglycans and fibrous proteins essential for tissue homeostasis, signaling in response to chemical and biomechanical stimuli, and is often dysregulated under conditions such as cancer, fibrosis, and chronic wounds. Here, we demonstrate that basonuclin-2 (BNC2), a mesenchymal-expressed gene, that is, strongly associated with cancer and developmental defects across genome-wide association studies, is a novel regulator of ECM composition and degradation. We find that at endogenous levels, BNC2 controls the expression of specific collagens, matrix metalloproteases, and other matrisomal components in breast cancer cells, and in fibroblasts that are primarily responsible for the production and processing of the ECM within the tumour microenvironment. In so doing, BNC2 modulates the motile and invasive properties of cancers, which likely explains the association of high BNC2 expression with increasing cancer grade and poor patient prognosis.

摘要

上皮-间充质转化对于组织形态发生和组织构成至关重要。它既涉及细胞运动的调节,也涉及细胞外基质(ECM)成分和组织构成的改变——细胞外基质是一种富含蛋白聚糖和纤维蛋白的复杂环境,对于组织稳态、对化学和生物力学刺激的信号反应至关重要,并且在癌症、纤维化和慢性伤口等情况下经常失调。在这里,我们证明了 basonuclin-2(BNC2),一种间充质表达的基因,与全基因组关联研究中的癌症和发育缺陷密切相关,是 ECM 组成和降解的新型调节因子。我们发现,在内源性水平上,BNC2 控制着乳腺癌细胞中特定胶原蛋白、基质金属蛋白酶和其他基质成分的表达,以及在肿瘤微环境中主要负责 ECM 产生和加工的成纤维细胞中特定胶原蛋白、基质金属蛋白酶和其他基质成分的表达。这样,BNC2 调节了癌症的运动和侵袭特性,这可能解释了高 BNC2 表达与癌症分级增加和患者预后不良的关联。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4dbe/10400885/5902f032292e/LSA-2023-01984_Fig1.jpg

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