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Intratracheal Bleomycin Aerosolization: The Best Route of Administration for a Scalable and Homogeneous Pulmonary Fibrosis Rat Model?

机译:气管内博莱霉素雾化:可扩展且均质的肺纤维化大鼠模型的最佳给药途径?

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摘要

Idiopathic pulmonary fibrosis (IPF) is a chronic disease with a poor prognosis and is characterized by the accumulation of fibrotic tissue in lungs resulting from a dysfunction in the healing process. In humans, the pathological process is patchy and temporally heterogeneous and the exact mechanisms remain poorly understood. Different animal models were thus developed. Among these, intratracheal administration of bleomycin (BML) is one of the most frequently used methods to induce lung fibrosis in rodents. In the present study, we first characterized histologically the time-course of lung alteration in rats submitted to BLM instillation. Heterogeneous damages were observed among lungs, consisting in an inflammatory phase at early time-points. It was followed by a transition to a fibrotic state characterized by an increased myofibroblast number and collagen accumulation. We then compared instillation and aerosolization routes of BLM administration. The fibrotic process was studied in each pulmonary lobe using a modified Ashcroft scale. The two quantification methods were confronted and the interobserver variability evaluated. Both methods induced fibrosis development as demonstrated by a similar progression of the highest modified Ashcroft score. However, we highlighted that aerosolization allows a more homogeneous distribution of lesions among lungs, with a persistence of higher grade damages upon time.
机译:特发性肺纤维化(IPF)是一种预后较差的慢性疾病,其特征是愈合过程中功能障碍导致肺中纤维化组织的积累。在人类中,病理过程是零散的和时间上异质的,确切的机制仍然知之甚少。因此开发了不同的动物模型。其中,气管内施用博来霉素(BML)是诱导啮齿动物肺纤维化的最常用方法之一。在本研究中,我们首先在组织学上表征了接受BLM滴注的大鼠肺部改变的时程。在肺部观察到异质性损伤,在早期时间点为炎症期。随后转变为纤维化状态,其特征在于成肌纤维细胞数目增加和胶原蛋白积累。然后,我们比较了BLM管理的滴注和雾化途径。使用改良的Ashcroft量表研究了每个肺叶的纤维化过程。面对两种量化方法,并评估了观察者间的变异性。两种方法均能诱导纤维化的发展,如最高改良Ashcroft评分的相似进展所证明。但是,我们强调指出,雾化可以使病变在肺之间的分布更加均匀,并且随着时间的推移会持续遭受更高级别的损害。

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