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同轴牺牲书写嵌入仿生血管网络到功能组织中。

Embedding Biomimetic Vascular Networks via Coaxial Sacrificial Writing into Functional Tissue.

机构信息

John A. Paulson School of Engineering and Applied Sciences, Harvard University, Cambridge, MA, USA.

Wyss Institute for Biologically Inspired Engineering, Harvard University, Boston, MA, USA.

出版信息

Adv Mater. 2024 Sep;36(36):e2401528. doi: 10.1002/adma.202401528. Epub 2024 Aug 2.

Abstract

Printing human tissues and organs replete with biomimetic vascular networks is of growing interest. While it is possible to embed perfusable channels within acellular and densely cellular matrices, they do not currently possess the biomimetic architectures found in native vessels. Here, coaxial sacrificial writing into functional tissues (co-SWIFT) is developed, an embedded bioprinting method capable of generating hierarchically branching, multilayered vascular networks within both granular hydrogel and densely cellular matrices. Coaxial printheads are designed with an extended core-shell configuration to facilitate robust core-core and shell-shell interconnections between printed branching vessels during embedded bioprinting. Using optimized core-shell ink combinations, biomimetic vessels composed of a smooth muscle cell-laden shell that surrounds perfusable lumens are coaxially printed into granular matrices composed of: 1) transparent alginate microparticles, 2) sacrificial microparticle-laden collagen, or 3) cardiac spheroids derived from human induced pluripotent stem cells. Biomimetic blood vessels that exhibit good barrier function are produced by seeding these interconnected lumens with a confluent layer of endothelial cells. Importantly, it is found that co-SWIFT cardiac tissues mature under perfusion, beat synchronously, and exhibit a cardio-effective drug response in vitro. This advance opens new avenues for the scalable biomanufacturing of vascularized organ-specific tissues for drug testing, disease modeling, and therapeutic use.

摘要

打印充满仿生血管网络的人体组织和器官越来越受到关注。虽然可以在无细胞和密集细胞基质中嵌入可灌注的通道,但它们目前不具备天然血管中存在的仿生结构。在这里,开发了同轴牺牲写入功能组织(co-SWIFT),这是一种嵌入式生物打印方法,能够在颗粒状水凝胶和密集细胞基质内生成分层分支的血管网络。同轴打印头采用扩展的核壳结构设计,以促进在嵌入式生物打印过程中打印出的分支血管之间的牢固的核-核和壳-壳连接。使用优化的核壳墨水组合,可以将包含平滑肌细胞的壳同轴打印到由以下成分组成的颗粒状基质中:1)透明质酸微球,2)牺牲微球负载的胶原,或 3)源自人诱导多能干细胞的心脏球体。通过用内皮细胞的汇合层对这些相互连接的腔进行接种,可以生成具有良好屏障功能的仿生血管。重要的是,发现 co-SWIFT 心脏组织在灌注下成熟,同步跳动,并在体外表现出心脏效应药物反应。这一进展为用于药物测试、疾病建模和治疗用途的血管化器官特异性组织的可扩展生物制造开辟了新途径。

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