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在啮齿动物模型中对膀胱伤口愈合的分子和组织学研究。

Molecular and histological studies of bladder wound healing in a rodent model.

机构信息

Department of Women's and Children's Health, Center of Molecular Medicine, Karolinska Institutet, Stockholm, Sweden.

Department of Pediatric Surgery, Surgical Clinic C, Copenhagen University Hospital Rigshospitalet, Denmark.

出版信息

Wound Repair Regen. 2020 May;28(3):293-306. doi: 10.1111/wrr.12797. Epub 2020 Feb 12.

Abstract

The field of regenerative medicine encounters different challenges. The success of tissue-engineered implants is dependent on proper wound healing. Today, the process of normal urinary bladder wound healing is poorly characterized. We aspired to explore and elucidate the natural response to injury in an in vivo model in order to further optimize tissue regeneration in future studies. In this study, we aimed to characterize histological and molecular changes during normal healing in a rat model by performing a standardized incisional wound followed by surgical closure. We used a rodent model (n = 40) to follow the healing process in the urinary bladder for 28 days. Surgical exposure of the bladder without incision (n = 40) was performed in controls. Histological characterization and western blot analyses of proteins was carried out using specific staining and markers for inflammation, proliferation, angiogenesis, and tissue maturation. For the molecular characterization of gene expression total RNA was collected for RT -PCR in wound healing pathway arrays. Analysis of histology revealed distinct, but overlapping, phases of healing with a local inflammatory response (days 1-8) simultaneous with a rapid formation of granulation tissue and proliferation (days 2-8). We also identified significant changes in gene expression related to inflammation, proliferation, and extracellular matrix formation. Healing of an incisional wound in a rodent urinary bladder demonstrated that all the classical phases of wound healing: hemostasis, inflammation, proliferation followed by tissue maturation were present. Our data suggest that the bladder and the skin share similar molecular signaling during wound healing, although we noted differences in the duration of each phase compared to previous studies in rat skin. Further studies will address whether our findings can be extrapolated to the human bladder.

摘要

再生医学领域面临着不同的挑战。组织工程植入物的成功取决于适当的伤口愈合。如今,正常膀胱伤口愈合的过程还没有被很好地描述。我们渴望在体内模型中探索和阐明对损伤的自然反应,以便在未来的研究中进一步优化组织再生。在这项研究中,我们旨在通过标准化的切口伤口和手术闭合来研究和阐明在大鼠模型中正常愈合过程中的组织学和分子变化。我们使用了一种啮齿动物模型(n = 40)来观察膀胱在 28 天内的愈合过程。对照组中对膀胱进行了不切口的手术暴露(n = 40)。使用特定的染色和炎症、增殖、血管生成和组织成熟的标志物进行组织学特征和蛋白质的 Western blot 分析。为了对基因表达进行分子特征分析,我们收集了伤口愈合途径微阵列中的总 RNA 进行 RT-PCR。组织学分析显示,具有局部炎症反应(第 1-8 天)的愈合过程具有独特但重叠的阶段,同时快速形成肉芽组织和增殖(第 2-8 天)。我们还发现了与炎症、增殖和细胞外基质形成相关的基因表达的显著变化。在大鼠膀胱的切口伤口愈合中,我们发现了所有经典的伤口愈合阶段:止血、炎症、增殖,随后是组织成熟。我们的数据表明,膀胱和皮肤在伤口愈合过程中共享相似的分子信号,尽管与之前在大鼠皮肤中的研究相比,我们注意到每个阶段的持续时间存在差异。进一步的研究将探讨我们的发现是否可以推广到人类膀胱。

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