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通过 3D 胶原凝胶生成趋触性梯度的微流控技术,以增强神经突生长。

Microfluidic generation of haptotactic gradients through 3D collagen gels for enhanced neurite growth.

机构信息

Department of Biomedical Engineering, Rutgers, The State University of New Jersey, Piscataway, New Jersey 08854, USA.

出版信息

J Neurotrauma. 2011 Nov;28(11):2377-87. doi: 10.1089/neu.2010.1606. Epub 2011 Aug 5.

Abstract

We adapted a microfluidic system used previously to generate durotactic gradients of stiffness in a 3D collagen gel, to produce haptotactic gradients of adhesive ligands through the collagen gel. Oligopeptide sequences that included bioactive peptide sequences from laminin, YIGSR, or IKVAV, were grafted separately onto type I collagen using 1-ethyl-3-(3-dimethylaminopropyl) carbodiimide (EDC). Solutions of peptide-grafted collagen and untreated collagen were then used as source and sink input solutions, respectively, in an H-shaped microfluidic network fabricated using traditional soft lithography. One-dimensional gradients of the peptide-grafted collagen solution were generated in the channel that connected the source and sink channels, and these gradients became immobilized upon self-assembly of the collagen into a 3D fibrillar gel. The slope and average concentration of the gradients were adjusted by changing the concentration of the source solutions and by changing the length of the cross-channel. A separate, underlying channel in the microfluidic construct allowed the introduction of a chick embryo dorsal root ganglion into the network. Neurites from these explants grew significantly longer up steep gradients of YIGSR, but shallow gradients of IKVAV in comparison to untreated collagen controls. When these two gradients were presented in combination, the bias in growth acceleration was the largest and most consistent. No differences were observed in the number of neurites choosing to grow up or down the gradients in any condition. These results suggest that the incorporation of distinct gradients of multiple bioactive ligands can improve directional acceleration of regenerating axons.

摘要

我们采用了先前用于在 3D 胶原凝胶中产生硬度趋化性梯度的微流控系统,通过胶原凝胶产生黏附配体的趋化性梯度。将包含层粘连蛋白、YIGSR 或 IKVAV 生物活性肽序列的寡肽序列分别通过 1-乙基-3-(3-二甲基氨基丙基)碳二亚胺 (EDC) 接枝到 I 型胶原上。然后,将肽接枝胶原和未经处理的胶原溶液分别用作 H 形微流控网络中源和汇输入溶液,该网络使用传统的软光刻技术制造。在连接源和汇通道的通道中产生肽接枝胶原溶液的一维梯度,并且这些梯度在胶原自组装成 3D 纤维状凝胶时固定。通过改变源溶液的浓度和改变交叉通道的长度来调整梯度的斜率和平均浓度。微流控结构中的单独的下部通道允许将鸡胚背根神经节引入网络中。这些外植体的神经突在 YIGSR 的陡峭梯度上显著生长得更长,但与未经处理的胶原对照相比,在 IKVAV 的浅梯度上生长得更短。当这两个梯度组合呈现时,生长加速的偏差最大且最一致。在任何条件下,都没有观察到选择沿着梯度向上或向下生长的神经突数量的差异。这些结果表明,掺入多个生物活性配体的不同梯度可以改善再生轴的定向加速。

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