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Hyaluronan (HA) Interacting Proteins RHAMM and Hyaluronidase Impact Prostate Cancer Cell Behavior and Invadopodia Formation in 3D HA-Based Hydrogels

机译:透明质酸(Ha)相互作用蛋白RHamm和透明质酸酶的影响前列腺癌细胞行为与树突状伪足形成在三维Ha-基水凝胶

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摘要

To study the individual functions of hyaluronan interacting proteins in prostate cancer (PCa) motility through connective tissues, we developed a novel three-dimensional (3D) hyaluronic acid (HA) hydrogel assay that provides a flexible, quantifiable, and physiologically relevant alternative to current methods. Invasion in this system reflects the prevalence of HA in connective tissues and its role in the promotion of cancer cell motility and tissue invasion, making the system ideal to study invasion through bone marrow or other HA-rich connective tissues. The bio-compatible cross-linking process we used allows for direct encapsulation of cancer cells within the gel where they adopt a distinct, cluster-like morphology. Metastatic PCa cells in these hydrogels develop fingerlike structures, “invadopodia”, consistent with their invasive properties. The number of invadopodia, as well as cluster size, shape, and convergence, can provide a quantifiable measure of invasive potential. Among candidate hyaluronan interacting proteins that could be responsible for the behavior we observed, we found that culture in the HA hydrogel triggers invasive PCa cells to differentially express and localize receptor for hyaluronan mediated motility (RHAMM)/CD168 which, in the absence of CD44, appears to contribute to PCa motility and invasion by interacting with the HA hydrogel components. PCa cell invasion through the HA hydrogel also was found to depend on the activity of hyaluronidases. Studies shown here reveal that while hyaluronidase activity is necessary for invadopodia and inter-connecting cluster formation, activity alone is not sufficient for acquisition of invasiveness to occur. We therefore suggest that development of invasive behavior in 3D HA-based systems requires development of additional cellular features, such as activation of motility associated pathways that regulate formation of invadopodia. Thus, we report development of a 3D system amenable to dissection of biological processes associated with cancer cell motility through HA-rich connective tissues.
机译:为了研究透明质酸相互作用蛋白通过结缔组织在前列腺癌(PCa)运动中的个别功能,我们开发了一种新颖的三维(3D)透明质酸(HA)水凝胶测定法,提供了一种灵活,可量化且在生理上相关的替代方法方法。该系统中的侵袭反映了HA在结缔组织中的流行及其在促进癌细胞运动和组织侵袭中的作用,使该系统成为研究通过骨髓或其他富含HA的结缔组织侵袭的理想系统。我们使用的生物相容性交联过程可将癌细胞直接包封在凝胶中,从而使它们采用独特的簇状形态。这些水凝胶中的转移性PCa细胞会形成指状结构,称为“侵袭足”,与其侵入特性一致。侵袭足的数量以及簇的大小,形状和会聚程度可以提供对浸润潜能的定量测量。在可能与我们观察到的行为有关的候选透明质酸相互作用蛋白中,我们发现在HA水凝胶中进行培养会触发侵入性PCa细胞差异表达和定位透明质酸介导的运动(RHAMM)/ CD168受体,而在缺乏CD44的情况下,通过与HA水凝胶组分相互作用,似乎有助于PCa的运动和侵袭。还发现PCa细胞通过HA水凝胶的入侵取决于透明质酸酶的活性。此处显示的研究表明,透明质酸酶活性对于侵袭伪足和相互联系的簇形成是必需的,但仅活性不足以发生侵袭。因此,我们建议在基于3D HA的系统中开发侵袭行为需要开发其他细胞功能,例如激活与运动相关的途径,从而调节侵袭足的形成。因此,我们报告了一种3D系统的开发,该系统适合于通过富含HA的结缔组织解剖与癌细胞运动相关的生物过程。

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