<i>Ex vivo</i>micro-computed tomography analysis of bleomycin-induced lung fibrosis for preclinical drug evaluation

Scotton, Chris J.; Hayes, Brian; Alexander, Randell; Datta, Arnab; Forty, Ellen; Mercer, Paul F.; Blanchard, Andy; Chambers, Rachel C.

doi:10.1183/09031936.00182412

Cited by 62 publications

(60 citation statements)

References 31 publications

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“…Hence, in vivo micro-CT resolutions are much lower compared to the high resolution (3.5 μm/pixel) used in the automated histological analysis. An improved micro-CT analysis using higher sensitivity involving high resolution scanning [13,34,38,39] might also be used to enhance accurate quantification of low level of fibrotic alterations. High resolutions (1–2 μm/pixel) have also been achieved with micro-CT analysis on ex vivo fixed lungs [34].…”

Section: Discussionmentioning

confidence: 99%

“…In contrast, the automated analysis is applied to the entire lung section. It should be noted that micro-CT high resolutions are associated with sometimes prohibitively long scan/reconstruction times of several hours per sample precluding high throughput [13,34]. In contrast the automated analysis acquisition/analysis time is much shorter in the range of 1 hour for 100 entire lung sections.…”

Section: Discussionmentioning

confidence: 99%

“…In contrast the automated analysis acquisition/analysis time is much shorter in the range of 1 hour for 100 entire lung sections. Ex vivo micro-CT may also be used for a 3D evaluation of severity of lung fibrosis providing a more sensitive and quantitative measure as well as a marked reduction of scanning time [13]. …”

Section: Discussionmentioning

confidence: 99%

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Quantification of Pulmonary Fibrosis in a Bleomycin Mouse Model Using Automated Histological Image Analysis

Gilhodes¹,

Julé²,

Kreuz

et al. 2017

PLoS ONE

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Current literature on pulmonary fibrosis induced in animal models highlights the need of an accurate, reliable and reproducible histological quantitative analysis. One of the major limits of histological scoring concerns the fact that it is observer-dependent and consequently subject to variability, which may preclude comparative studies between different laboratories. To achieve a reliable and observer-independent quantification of lung fibrosis we developed an automated software histological image analysis performed from digital image of entire lung sections. This automated analysis was compared to standard evaluation methods with regard to its validation as an end-point measure of fibrosis. Lung fibrosis was induced in mice by intratracheal administration of bleomycin (BLM) at 0.25, 0.5, 0.75 and 1 mg/kg. A detailed characterization of BLM-induced fibrosis was performed 14 days after BLM administration using lung function testing, micro-computed tomography and Ashcroft scoring analysis. Quantification of fibrosis by automated analysis was assessed based on pulmonary tissue density measured from thousands of micro-tiles processed from digital images of entire lung sections. Prior to analysis, large bronchi and vessels were manually excluded from the original images. Measurement of fibrosis has been expressed by two indexes: the mean pulmonary tissue density and the high pulmonary tissue density frequency. We showed that tissue density indexes gave access to a very accurate and reliable quantification of morphological changes induced by BLM even for the lowest concentration used (0.25 mg/kg). A reconstructed 2D-image of the entire lung section at high resolution (3.6 μm/pixel) has been performed from tissue density values allowing the visualization of their distribution throughout fibrotic and non-fibrotic regions. A significant correlation (p<0.0001) was found between automated analysis and the above standard evaluation methods. This correlation establishes automated analysis as a novel end-point measure of BLM-induced lung fibrosis in mice, which will be very valuable for future preclinical drug explorations.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Quantification of Pulmonary Fibrosis in a Bleomycin Mouse Model Using Automated Histological Image Analysis

Gilhodes¹,

Julé²,

Kreuz

et al. 2017

PLoS ONE

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“…Lungs were fixed and inflated with 4% paraformaldehyde (PFA) at 20 cmH 2 O pressure overnight and then incubated through a serial ethanol gradient (50%, 70%, 80%, 90%, and 100%) followed by incubation with 100% hexamethyldisilazane overnight before air drying (80). Lung specimens were scanned at an isotropic resolution of 10 microns at 45 kVp, 200 mAs (81).…”

Section: Cldn18mentioning

confidence: 99%

Claudin-18–mediated YAP activity regulates lung stem and progenitor cell homeostasis and tumorigenesis

Zhou¹,

Flodby²,

Luo³

et al. 2018

Journal of Clinical Investigation

125

116

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Claudins, the integral tight junction (TJ) proteins that regulate paracellular permeability and cell polarity, are frequently dysregulated in cancer; however, their role in neoplastic progression is unclear. Here, we demonstrated that knockout of Cldn18, a claudin family member highly expressed in lung alveolar epithelium, leads to lung enlargement, parenchymal expansion, increased abundance and proliferation of known distal lung progenitors, the alveolar epithelial type II (AT2) cells, activation of Yes-associated protein (YAP), increased organ size, and tumorigenesis in mice. Inhibition of YAP decreased proliferation and colony-forming efficiency (CFE) of Cldn18 -/-AT2 cells and prevented increased lung size, while CLDN18 overexpression decreased YAP nuclear localization, cell proliferation, CFE, and YAP transcriptional activity. CLDN18 and YAP interacted and colocalized at cell-cell contacts, while loss of CLDN18 decreased YAP interaction with Hippo kinases p-LATS1/2. Additionally, Cldn18 -/-mice had increased propensity to develop lung adenocarcinomas (LuAd) with age, and human LuAd showed stage-dependent reduction of CLDN18.1. These results establish CLDN18 as a regulator of YAP activity that serves to restrict organ size, progenitor cell proliferation, and tumorigenesis, and suggest a mechanism whereby TJ disruption may promote progenitor proliferation to enhance repair following injury.

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“…In the first session, Professor Clive Page (London) described the usefulness of in vivo models to identify new drugs for respiratory disease, while Dr Chris Scotton (Exeter) spoke about novel ways of using in vivo imaging in murine models of lung disease,9 and Professor Stephen Renshaw (Sheffield) described how the zebrafish, which does not have lungs, is a useful model for studying pulmonary inflammation 10. In the second session, Professor Eric White (Michigan, USA) discussed novel 3D cell culture models for studying fibrotic lung disease, Professor Donna Davies (Southampton) described how novel tissue-engineered constructs with microfluidics platforms to deliver inflammatory cells will be used to develop novel therapeutic treatments for asthma, and Dr Carmel Nanthakumar (London) discussed how novel in vitro platforms are being used in industry to develop new anti-fibrotic drugs.…”

Section: Bts/british Association For Lung Researchmentioning

confidence: 99%

Review of the British Thoracic Society Winter Meeting 2014, 3-5 December, London, UK

Greening

José

Chalmers

et al. 2015

Thorax

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The British Thoracic Society Winter Meeting 2014 is reviewed in this article. This annual scientific meeting attracted its largest number of delegates ever and over 3 days in December up-to-date respiratory research was presented and current thinking in respiratory science and clinical academia was discussed. This article reviews a number of symposia and selected abstract presentations from the meeting.

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Ex vivomicro-computed tomography analysis of bleomycin-induced lung fibrosis for preclinical drug evaluation

Cited by 62 publications

References 31 publications

Quantification of Pulmonary Fibrosis in a Bleomycin Mouse Model Using Automated Histological Image Analysis

Quantification of Pulmonary Fibrosis in a Bleomycin Mouse Model Using Automated Histological Image Analysis

Claudin-18–mediated YAP activity regulates lung stem and progenitor cell homeostasis and tumorigenesis

Review of the British Thoracic Society Winter Meeting 2014, 3-5 December, London, UK

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