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Feasibility of spatially-offset Raman spectroscopy for in-vitro and in-vivo monitoring mineralisation of bone tissue-engineering scaffolds

机译:空间偏移拉曼光谱法在体外和体内监测骨组织工程支架矿化的可行性

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摘要

We investigated the feasibility of using spatially-offset Raman spectroscopy (SORS) for non-destructive characterisation of bone tissue engineering scaffolds. The deep regions of these scaffolds, or scaffolds implanted subcutaneously in live animals, are typically difficult to measure by confocal Raman spectroscopy techniques because of the limited depth penetration of light caused by the high level of light scattering. Layered samples consisting of bioactive glass foams (IEIC16), 3D-printed biodegradable poly-(lactic-co-glycolic acid) scaffolds (PLGA) and hydroxyapatite powder (HA) were used to mimic non-destructive detection of bio-mineralisation for intact real-size 3D tissue engineering constructs. SORS spectra were measured with a new SORS instrument using a digital micro-mirror device (DMD) to allow software selection of the spatial offsets. The results show that HA can be reliably detected at depths of 0-2.3 mm, which corresponds to the maximum accessible spatial offset of the current instrument. The intensity ratio of Raman bands associated to the scaffolds and HA with the spatial offset depended on the depth at which HA was located. Furthermore, we show the feasibility for in-vivo monitoring mineralisation of scaffold implanted subcutaneously by demonstrating the ability to measure transcutaneously Raman signals of the scaffolds and HA (fresh chicken skin used as a top layer). The ability to measure spectral depth profiles at high speed (5 s acquisition time), and the ease of implementation, make SORS a promising approach for non-invasive characterisation of cell/tissue development in-vitro, and for long-term in-vivo monitoring the mineralisation in 3D scaffolds subcutaneously implanted in small animals.
机译:我们调查了使用空间偏移拉曼光谱(SORS)进行骨组织工程支架非破坏性表征的可行性。由于由高水平的光散射引起的有限的光深度穿透,通常难以通过共聚焦拉曼光谱技术来测量这些支架或皮下植入活体动物中的支架的深区域。使用由生物活性玻璃泡沫(IEIC16),3D打印的可生物降解的聚乳酸-乙醇酸乙醇支架(PLGA)和羟基磷灰石粉末(HA)组成的分层样品来模拟生物矿化的无损检测,从而完整尺寸的3D组织工程构造。使用新的SORS仪器,使用数字微镜设备(DMD)测量SORS光谱,以允许软件选择空间偏移。结果表明,可以在0-2.3 mm的深度处可靠地检测到HA,这对应于当前仪器的最大可访问空间偏移。与支架和具有空间偏移的HA相关的拉曼谱带的强度比取决于HA所位于的深度。此外,我们通过展示测量支架和HA(新鲜鸡皮作为顶层)的经皮拉曼信号的能力,展示了体内监测皮下植入支架的矿化的可行性。能够以高速(5 s的采集时间)测量光谱深度剖面的能力以及易于实施的特性,使SORS成为了体外和长期体内非侵入性表征细胞/组织发育的有前途的方法监测皮下植入小型动物的3D支架的矿化情况。

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