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用于故意转基因表达的促血管生成近红外响应水凝胶。

Pro-angiogenic near infrared-responsive hydrogels for deliberate transgene expression.

机构信息

University Hospital La Paz-IdiPAZ, Paseo de la Castellana 261, Madrid 28046, Spain; CIBER de Bioingeniería, Biomateriales y Nanomedicina, CIBER-BBN, Spain.

University Hospital La Paz-IdiPAZ, Paseo de la Castellana 261, Madrid 28046, Spain; CIBER de Bioingeniería, Biomateriales y Nanomedicina, CIBER-BBN, Spain.

出版信息

Acta Biomater. 2018 Sep 15;78:123-136. doi: 10.1016/j.actbio.2018.08.006. Epub 2018 Aug 9.

Abstract

UNLABELLED

CuS nanoparticles (CuSNP) are degradable, readily prepared, inexpensive to produce and efficiently cleared from the body. In this work, we explored the feasibility of CuSNP to function as degradable near infrared (NIR) nanotransducers within fibrin-based cellular scaffolds. To prepare NIR-responsive CuSNP hydrogels, fibrinogen was dissolved in cell culture medium and supplemented with aqueous dispersions of CuSNP. Fibrinogen polymerization was catalyzed by the addition of thrombin. In some experiments, HUVEC, C3H/10T1/2 or C3H/10T1/2-fLuc cells, that harbor a heat-activated and rapamycin-dependent gene switch for regulating the expression of firefly luciferase transgene, were incorporated to the sol phase of the hydrogel. For in vivo experiments, hydrogels were injected subcutaneously in the back of adult C3H/HeN mice. Upon NIR irradiation, CuSNP hydrogels allowed heat-inducible and rapamycin-dependent transgene expression in cells contained therein, in vitro and in vivo. C3H/10T1/2 cells cultured in CuSNP hydrogels increased metabolic activity, survival rate and fibrinolytic activity, which correlated with changes at the transcriptome level. Media conditioned by CuSNP hydrogels increased viability of HUVEC which formed pseudocapillary structures and remodeled protein matrix when entrapped within these hydrogels. After long-term implantation, the skin patches that covered the CuSNP hydrogels showed increased capillary density which was not detected in mice implanted with matrices lacking CuSNP. In summary, NIR-responsive scaffolds harboring CuSNP offer compelling features in the tissue engineering field, as degradable implants with enhanced integration capacity in host tissues that can provide remote controlled deployment of therapeutic gene products.

STATEMENT OF SIGNIFICANCE

Hydrogels composed of fibrin embedding copper sulfide nanoparticles (CuSNP) efficiently convert incident near infrared (NIR) energy into heat and can function as cellular scaffolding. NIR laser irradiation of CuSNP hydrogels can be employed to remotely induce spatiotemporal patterns of transgene expression in genetically engineered multipotent stem cells. CuSNP incorporation in hydrogel architecture accelerates the cell-mediated degradation of the fibrin matrix and induces pro-angiogenic responses that may facilitate the integration of these NIR-responsive scaffolds in host tissues. CuSNP hydrogels that harbor cells capable of controlled expression of therapeutic gene products may be well suited for tissue engineering as they are biodegradable, enhance implant vascularization and can be used to deploy growth factors in a desired spatiotemporal fashion.

摘要

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CuS 纳米粒子(CuSNP)可降解、易于制备、生产成本低廉且可高效从体内清除。在这项工作中,我们探索了 CuSNP 作为纤维蛋白基细胞支架内可降解近红外(NIR)纳米转导体的可行性。为了制备对近红外有响应的 CuSNP 水凝胶,纤维蛋白原溶解在细胞培养基中,并加入 CuSNP 的水性分散体。纤维蛋白原的聚合通过添加凝血酶来催化。在一些实验中,将携带热激活和雷帕霉素依赖性基因开关的 HUVEC、C3H/10T1/2 或 C3H/10T1/2-fLuc 细胞加入到水凝胶的溶胶相中,该基因开关用于调节萤火虫荧光素酶转基因的表达。对于体内实验,将水凝胶皮下注射到成年 C3H/HeN 小鼠的背部。近红外照射后,CuSNP 水凝胶可在体外和体内诱导其中所含细胞的热诱导和雷帕霉素依赖性转基因表达。在 CuSNP 水凝胶中培养的 C3H/10T1/2 细胞增加了代谢活性、存活率和纤维蛋白溶解活性,这与转录组水平的变化相关。CuSNP 水凝胶条件培养基增加了 HUVEC 的活力,使其形成拟血管结构,并在这些水凝胶中重塑蛋白质基质。长期植入后,覆盖 CuSNP 水凝胶的皮肤贴片显示出增加的毛细血管密度,而在没有 CuSNP 的基质中植入的小鼠则没有检测到这种密度。总之,含有 CuSNP 的近红外响应支架在组织工程领域具有引人注目的特性,因为它们是可降解的植入物,具有增强宿主组织整合能力,可以远程控制治疗性基因产物的释放。CuSNP 水凝胶的近红外激光照射可用于远程诱导基因工程多能干细胞中时空模式的转基因表达。CuSNP 掺入水凝胶结构可加速纤维蛋白基质的细胞介导降解,并诱导促血管生成反应,这可能有助于这些近红外响应支架在宿主组织中的整合。含有可控制表达治疗性基因产物的细胞的 CuSNP 水凝胶可能非常适合组织工程,因为它们是可生物降解的,可增强植入物的血管化,并可用于以所需的时空方式释放生长因子。

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