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Engineering a Tumor Microenvironment‐Mimetic Niche for Tissue Regeneration with Xenogeneic Cancer Cells

机译:工程学肿瘤微环境模拟利基以异种癌细胞的组织再生。

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摘要

The insufficient number of cells suitable for transplantation is a long‐standing problem to cell‐based therapies aimed at tissue regeneration. Xenogeneic cancer cells (XCC) may be an alternative source of therapeutic cells, but their transplantation risks both immune rejection and unwanted spreading. In this study, a strategy to facilitate XCC transplantation is reported and their spreading in vivo is confined by constructing an engineering matrix that mimics the characteristics of tumor microenvironment. The data show that this matrix, a tumor homogenate‐containing hydrogel (THAG), successfully creates an immunosuppressive enclave after transplantation into immunocompetent mice. XCC of different species and tissue origins seeded into THAG survive well, integrated with the host and developed the intrinsic morphology of the native tissue, without being eliminated or spreading out of the enclave. Most strikingly, immortalized human hepatocyte cells and rat β‐cells loaded into THAG exert the physiological functions of the human liver and rat pancreas islets, respectively, in the mouse body. This study demonstrates a novel and feasible approach to harness the unique features of tumor development for tissue transplantation and regenerative medicine.
机译:适于移植的细胞数量不足是针对组织再生的基于细胞的疗法的长期存在的问题。异种癌细胞(XCC)可能是治疗细胞的替代来源,但是它们的移植同时具有免疫排斥和有害扩散的风险。在这项研究中,报道了促进XCC移植的策略,并且通过构建模仿肿瘤微环境特征的工程基质来限制它们在体内的传播。数据显示,这种基质是一种含有肿瘤匀浆的水凝胶(THAG),在移植到具有免疫能力的小鼠体内后成功创建了一个免疫抑制区。植入THAG的不同物种和组织起源的XCC可以很好地存活,可以与宿主整合并形成天然组织的固有形态,而不会被消除或散布在飞地之外。最为显着的是,装入THAG的永生化人肝细胞和大鼠β细胞分别在小鼠体内发挥人肝和大鼠胰岛的生理功能。这项研究表明了一种新颖可行的方法,可以利用肿瘤发展的独特特征进行组织移植和再生医学。

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