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将原发性唾液腺细胞封装在可酶解的聚乙二醇水凝胶中可促进腺泡细胞特性。

Encapsulation of primary salivary gland cells in enzymatically degradable poly(ethylene glycol) hydrogels promotes acinar cell characteristics.

作者信息

Shubin Andrew D, Felong Timothy J, Schutrum Brittany E, Joe Debria S L, Ovitt Catherine E, Benoit Danielle S W

机构信息

Department of Biomedical Engineering, University of Rochester, Rochester, NY, United States.

Department of Biology, Xavier University of Louisiana, New Orleans, LA, United States.

出版信息

Acta Biomater. 2017 Mar 1;50:437-449. doi: 10.1016/j.actbio.2016.12.049. Epub 2016 Dec 27.

Abstract

UNLABELLED

Radiation therapy for head and neck cancers leads to permanent xerostomia due to the loss of secretory acinar cells in the salivary glands. Regenerative treatments utilizing primary submandibular gland (SMG) cells show modest improvements in salivary secretory function, but there is limited evidence of salivary gland regeneration. We have recently shown that poly(ethylene glycol) (PEG) hydrogels can support the survival and proliferation of SMG cells as multicellular spheres in vitro. To further develop this approach for cell-based salivary gland regeneration, we have investigated how different modes of PEG hydrogel degradation affect the proliferation, cell-specific gene expression, and epithelial morphology within encapsulated salivary gland spheres. Comparison of non-degradable, hydrolytically-degradable, matrix metalloproteinase (MMP)-degradable, and mixed mode-degradable hydrogels showed that hydrogel degradation by any mechanism is required for significant proliferation of encapsulated cells. The expression of acinar phenotypic markers Aqp5 and Nkcc1 was increased in hydrogels that are MMP-degradable compared with other hydrogel compositions. However, expression of secretory acinar proteins Mist1 and Pip was not maintained to the same extent as phenotypic markers, suggesting changes in cell function upon encapsulation. Nevertheless, MMP- and mixed mode-degradability promoted organization of polarized cell types forming tight junctions and expression of the basement membrane proteins laminin and collagen IV within encapsulated SMG spheres. This work demonstrates that cellularly remodeled hydrogels can promote proliferation and gland-like organization by encapsulated salivary gland cells as well as maintenance of acinar cell characteristics required for regenerative approaches. Investigation is required to identify approaches to further enhance acinar secretory properties.

STATEMENT OF SIGNIFICANCE

Regenerative strategies to replace damaged salivary glands require the function and organization of acinar cells. Hydrogel-based approaches have shown promise to control cell function and phenotype. However, little is known about how specific parameters, such as the mechanism of hydrogel degradation (e.g., hydrolytic or enzymatic), influence the viability, proliferation, organization, and phenotype of salivary gland cells. In this work, it is shown that hydrogel-encapsulated primary salivary gland cell proliferation is dependent upon hydrogel degradation. Hydrogels crosslinked with enzymatically degradable peptides promoted the expression of critical acinar cell markers, which are typically downregulated in primary cultures. Furthermore, salivary gland cells encapsulated in enzymatically- but not hydrolytically-degradable hydrogels displayed highly organized and polarized salivary gland cell markers, which mimics characteristics found in native gland tissue. In sum, results indicate that salivary gland cells respond to cellularly remodeled hydrogels, resulting in self-assembly and organization akin to acini substructures of the salivary gland.

摘要

未标注

头颈部癌症的放射治疗会导致唾液腺分泌腺泡细胞丧失,从而引起永久性口干。利用原代下颌下腺(SMG)细胞的再生治疗在唾液分泌功能方面有一定改善,但唾液腺再生的证据有限。我们最近发现,聚乙二醇(PEG)水凝胶可在体外支持SMG细胞作为多细胞球的存活和增殖。为了进一步开发这种基于细胞的唾液腺再生方法,我们研究了PEG水凝胶不同的降解模式如何影响包封的唾液腺球体内细胞的增殖、细胞特异性基因表达和上皮形态。对不可降解、水解可降解、基质金属蛋白酶(MMP)可降解和混合模式可降解水凝胶的比较表明,任何机制引起的水凝胶降解都是包封细胞显著增殖所必需的。与其他水凝胶组合物相比,MMP可降解水凝胶中腺泡表型标志物Aqp5和Nkcc1的表达增加。然而,分泌性腺泡蛋白Mist1和Pip的表达没有维持到与表型标志物相同的程度,这表明包封后细胞功能发生了变化。尽管如此,MMP和混合模式可降解性促进了极化细胞类型的组织形成紧密连接,并促进了包封的SMG球体内基底膜蛋白层粘连蛋白和胶原蛋白IV的表达。这项工作表明,细胞重塑的水凝胶可以促进包封的唾液腺细胞的增殖和腺体样组织形成,以及维持再生方法所需的腺泡细胞特征。需要进行研究以确定进一步增强腺泡分泌特性的方法。

意义声明

替代受损唾液腺的再生策略需要腺泡细胞的功能和组织。基于水凝胶的方法已显示出控制细胞功能和表型的前景。然而,关于特定参数,如水凝胶降解机制(例如水解或酶解)如何影响唾液腺细胞的活力、增殖、组织和表型,人们知之甚少。在这项工作中,表明水凝胶包封的原代唾液腺细胞增殖依赖于水凝胶降解。与酶可降解肽交联的水凝胶促进了关键腺泡细胞标志物的表达,这些标志物在原代培养中通常会下调。此外,包封在酶解而非水解可降解水凝胶中的唾液腺细胞显示出高度组织化和极化的唾液腺细胞标志物,这模仿了天然腺体组织中的特征。总之,结果表明唾液腺细胞对细胞重塑的水凝胶有反应,导致类似于唾液腺腺泡亚结构的自组装和组织形成。

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