人类人工基质-上皮组织替代物细胞外基质成熟的时空特征。

IF 4.4 1区 生物学 Q1 BIOLOGY BMC Biology Pub Date : 2024-11-18 DOI:10.1186/s12915-024-02065-y
Paula Ávila-Fernández, Miguel Etayo-Escanilla, David Sánchez-Porras, Ricardo Fernández-Valadés, Fernando Campos, Ingrid Garzón, Víctor Carriel, Miguel Alaminos, Óscar Darío García-García, Jesús Chato-Astrain
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引用次数: 0

摘要

背景:组织工程技术为在可控、可重现的系统中了解复杂过程提供了新策略。在这项研究中,我们生成了双层人体组织替代物,包括带有上皮的细胞结缔组织(全厚基质-上皮替代物或 SESS)和在无细胞生物材料上生成带有上皮层的人体组织替代物(上皮替代物或 ESS)。对这两种人造组织进行了连续时间段的研究,以分析细胞外基质的成熟过程:在上皮层方面,ESS细胞增殖活跃,细胞角蛋白5呈阳性表达,分化标志物表达量较低,而SESS上皮细胞分化水平较高,细胞角蛋白10和Claudin呈逐渐阳性表达。SESS 中的基质细胞倾向于在与上皮直接接触的基质区(1 区)聚集并积极合成细胞外基质成分,如胶原和蛋白多糖,而 ESS 中这些成分非常稀少。在基底膜方面,ESS 显示出部分分化的结构,其中含有纤连蛋白-1 和珠蛋白。然而,SESS 的基底膜分化程度较高,纤维连接蛋白 1、perlecan、nidogen 1、软骨素-6-硫酸酯蛋白多糖、agrin 以及胶原 IV 型和 VII 型均呈阳性表达,但该结构中的 lumican 呈阴性。最后,ESS 和 SESS 被证明是研究代谢途径调控的有用工具,揭示了ESS 和 SESS 中转化生长因子-β 途径的不同激活和上调:这些结果证实了上皮-基质相互作用与细胞外基质发育和分化的相关性,尤其是在基底膜成分方面,并建议使用双层人工组织替代物在体内重现人体组织的细胞外基质成熟和发育过程。
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Spatiotemporal characterization of extracellular matrix maturation in human artificial stromal-epithelial tissue substitutes.

Background: Tissue engineering techniques offer new strategies to understand complex processes in a controlled and reproducible system. In this study, we generated bilayered human tissue substitutes consisting of a cellular connective tissue with a suprajacent epithelium (full-thickness stromal-epithelial substitutes or SESS) and human tissue substitutes with an epithelial layer generated on top of an acellular biomaterial (epithelial substitutes or ESS). Both types of artificial tissues were studied at sequential time periods to analyze the maturation process of the extracellular matrix.

Results: Regarding epithelial layer, ESS cells showed active proliferation, positive expression of cytokeratin 5, and low expression of differentiation markers, whereas SESS epithelium showed higher differentiation levels, with a progressive positive expression of cytokeratin 10 and claudin. Stromal cells in SESS tended to accumulate and actively synthetize extracellular matrix components such as collagens and proteoglycans in the stromal area in direct contact with the epithelium (zone 1), whereas these components were very scarce in ESS. Regarding the basement membrane, ESS showed a partially differentiated structure containing fibronectin-1 and perlecan. However, SESS showed higher basement membrane differentiation, with positive expression of fibronectin 1, perlecan, nidogen 1, chondroitin-6-sulfate proteoglycans, agrin, and collagens types IV and VII, although this structure was negative for lumican. Finally, both ESS and SESS proved to be useful tools for studying metabolic pathway regulation, revealing differential activation and upregulation of the transforming growth factor-β pathway in ESS and SESS.

Conclusions: These results confirm the relevance of epithelial-stromal interaction for extracellular matrix development and differentiation, especially regarding basement membrane components, and suggest the usefulness of bilayered artificial tissue substitutes to reproduce ex vivo the extracellular matrix maturation and development process of human tissues.

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来源期刊
BMC Biology
BMC Biology 生物-生物学
CiteScore
7.80
自引率
1.90%
发文量
260
审稿时长
3 months
期刊介绍: BMC Biology is a broad scope journal covering all areas of biology. Our content includes research articles, new methods and tools. BMC Biology also publishes reviews, Q&A, and commentaries.
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