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Prediction and validation of cell alignment along microvessels as order principle to restore tissue architecture in liver regeneration

机译:预测和验证沿微血管排列的细胞排列顺序以恢复肝脏再生中的组织结构

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摘要

Only little is known about how cells coordinately behave to establish functional tissue structure and restore microarchitecture during regeneration. Research in this field is hampered by a lack of techniques that allow quantification of tissue architecture and its development. To bridge this gap, we have established a procedure based on confocal laser scans, image processing, and three-dimensional tissue reconstruction, as well as quantitative mathematical modeling. As a proof of principle, we reconstructed and modeled liver regeneration in mice after damage by CCl4, a prototypical inducer of pericentral liver damage. We have chosen the regenerating liver as an example because of the tight link between liver architecture and function: the complex microarchitecture formed by hepatocytes and microvessels, i.e. sinusoids, ensures optimal exchange of metabolites between blood and hepatocytes. Our model captures all hepatocytes and sinusoids of a liver lobule during a 16 days regeneration process. The model unambiguously predicted a so-far unrecognized mechanism as essential for liver regeneration, whereby daughter hepatocytes align along the orientation of the closest sinusoid, a process which we named “hepatocyte-sinusoid alignment” (HSA). The simulated tissue architecture was only in agreement with the experimentally obtained data when HSA was included into the model and, moreover, no other likely mechanism could replace it. In order to experimentally validate the model of prediction of HSA, we analyzed the three-dimensional orientation of daughter hepatocytes in relation to the sinusoids. The results of this analysis clearly confirmed the model prediction. We believe our procedure is widely applicable in the systems biology of tissues.
机译:关于细胞如何协调行为以建立功能性组织结构并在再生过程中恢复微结构的了解甚少。由于缺乏能够量化组织结构及其发展的技术,该领域的研究受到了阻碍。为了弥合这一差距,我们建立了基于共聚焦激光扫描,图像处理和三维组织重建以及定量数学建模的程序。作为原理的证明,我们在小鼠中枢周围肝损伤的典型诱导物CCl4损伤后重建并建模了小鼠的肝再生。由于肝脏结构和功能之间的紧密联系,我们选择再生肝脏为例:由肝细胞和微血管(即正弦曲线)形成的复杂微体系结构可确保血液和肝细胞之间代谢物的最佳交换。我们的模型在16天的再生过程中捕获了肝小叶的所有肝细胞和正弦曲线。该模型明确地预测了迄今为止尚不清楚的机制对于肝脏再生至关重要,因此子代肝细胞沿着最接近的正弦曲线的方向排列,我们将这一过程称为“肝细胞-正弦曲线排列”(HSA)。仅当将HSA包含在模型中时,模拟的组织结构才与实验获得的数据一致,而且,没有其他可能的机制可以替代它。为了通过实验验证HSA的预测模型,我们分析了子肝细胞相对于正弦波的三维定向。分析结果清楚地证实了模型预测。我们相信我们的程序可广泛应用于组织的系统生物学。

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