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Two-Photon Imaging of Collagen Remodeling in RAFT Tissue Cultures

机译:RAFT组织培养物中胶原重塑的双光子成像

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摘要

Tissue remodeling is associated with both normal and abnormal processes including wound healing, fibrosis and cancer. In skin, abnormal remodeling causes permanent structural changes that can lead to hypertropic scarring and keloid formation. Normal remodeling, although fast and efficient in skin, is still imperfect, and a connective tissue scar remains at the wound site. As a result, methods are needed to optimize tissue remodeling in vivo in all cases of wound repair. Since fibroblast-mediated contraction of engineered 3-D collagen based tissues (RAFTs) represents an in vitro model of the tissue contraction and collagen remodeling that occurs in vivo, RAFT tissue contraction studies combined with two-photon microscopy (TPM) studies are used to provide information on ways to improve tissue remodeling in vivo. In the RAFT models discussed here, tissue contraction is modulated either by application of exogenous growth factors or photodynamic therapy. During tissue contraction, TPM is used to image changes in Collagen Type I fibers in the RAFT skin models. Tissues are imaged at depth at day 15 after modulation. TPM signal analysis shows that RAFT tissues having the highest collagen density have the fastest rate of decay of fluorescent signal with depth.
机译:组织重塑与正常和异常过程有关,包括伤口愈合,纤维化和癌症。在皮肤中,异常重塑会导致永久性结构变化,从而导致过度增生性瘢痕形成和瘢痕loid形成。正常的重塑,尽管在皮肤中快速有效,但仍不完善,结缔组织疤痕仍留在伤口处。结果,需要在所有伤口修复情况下优化体内组织重塑的方法。由于成纤维细胞介导的工程化3D胶原基组织收缩(RAFT)代表了体内发生的组织收缩和胶原重塑的体外模型,因此将RAFT组织收缩研究与两光子显微镜(TPM)研究结合起来用于提供有关改善体内组织重塑的方法的信息。在本文讨论的RAFT模型中,通过应用外源性生长因子或光动力疗法来调节组织收缩。在组织收缩过程中,TPM用于对RAFT皮肤模型中I型胶原纤维的变化进行成像。调制后第15天将组织成像。 TPM信号分析表明,胶原蛋白密度最高的RAFT组织具有随深度衰减的荧光信号的最快速率。

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