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通过多孔硅介导的光穿孔实现空间分辨的类器官转染

Spatially-Resolved Organoid Transfection by Porous Silicon-Mediated Optoporation.

作者信息

Spiteri Chantelle, Caprettini Valeria, Wang Yikai, Dominguez-Gil Sofia, Kaasalainen Martti, Wang Cong, Martella Davide Alessandro, McLennan Samuel, Vashisth Priya, Gary-Bobo Magali, Nguyen Christophe, Bergholt Mads, Durand Jean-Olivier, Cunin Frédérique, Chiappini Ciro

机构信息

Centre for Craniofacial and Regenerative Biology, King's College London, London, SE1 9RT, United Kingdom.

London Centre for Nanotechnology, King's College London, London, WC2R 2LS, United Kingdom.

出版信息

Adv Mater. 2024 Dec;36(49):e2407650. doi: 10.1002/adma.202407650. Epub 2024 Oct 17.

Abstract

Engineering the spatial organisation of organotypic cultures is pivotal for refining tissue models that are useful for gaining deeper insights into complex, non-cell autonomous processes. These advanced models are key to improving the understanding of fundamental biological mechanisms and therapeutic strategies. Controlling gene regulation through spatially-resolved delivery of nucleic acids provides an attractive approach to produce such tissue models. An emerging strategy for spatially-resolved transfection uses photosensitizing nanoparticles coupled with laser pulses to optoporate cells in culture and locally mediate gene delivery. However, localized optoporation in 3D systems remains challenging. Here we propose a solution to this longstanding hurdle, demonstrating that porous silicon nanoparticles are a safe and bioresorbable photosensitising nanomaterial capable of spatially-resolved transfection of mRNA in MCF-7 organoids by near-infrared two-photon optoporation. Functionalization with an azobenzene-lysine photo-switchable moiety enhances the transfection efficiency of the nanoparticles up to 84% in a 2D cell system. Moreover, the nanoparticles enable spatially selective mRNA transfection to MCF-7 spheroids, demonstrating targeted  gene delivery in complex 3D cellular environments. The approach for spatially-resolved 3D optoporation offers a way forward for the design of tailored spheroids and organoids by spatially selective nucleic acids delivery.

摘要

构建类器官培养物的空间组织对于优化组织模型至关重要,这些模型有助于更深入地了解复杂的非细胞自主过程。这些先进模型是增进对基本生物学机制和治疗策略理解的关键。通过核酸的空间分辨递送控制基因调控为生产此类组织模型提供了一种有吸引力的方法。一种新兴的空间分辨转染策略是使用与激光脉冲耦合的光敏纳米颗粒对培养中的细胞进行光穿孔,并在局部介导基因递送。然而,在三维系统中进行局部光穿孔仍然具有挑战性。在这里,我们提出了一个解决这一长期障碍的方案,证明多孔硅纳米颗粒是一种安全且可生物降解的光敏纳米材料,能够通过近红外双光子光穿孔在MCF-7类器官中对mRNA进行空间分辨转染。用偶氮苯-赖氨酸光开关部分进行功能化可将纳米颗粒在二维细胞系统中的转染效率提高至84%。此外,这些纳米颗粒能够对MCF-7球体进行空间选择性mRNA转染,证明了在复杂的三维细胞环境中的靶向基因递送。这种空间分辨三维光穿孔方法为通过空间选择性核酸递送设计定制的球体和类器官提供了一条前进的道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/274c/11619231/59ee372d0b69/ADMA-36-2407650-g002.jpg

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