. 2006 Jun 30;7(1):95.

doi: 10.1186/1465-9921-7-95.

Migratory marker expression in fibroblast foci of idiopathic pulmonary fibrosis

Marco Chilosi¹, Alberto Zamò, Claudio Doglioni, Daniela Reghellin, Maurizio Lestani, Licia Montagna, Serena Pedron, Maria Grazia Ennas, Alessandra Cancellieri, Bruno Murer, Venerino Poletti

Affiliations

PMID: 16813649
PMCID: PMC1538593
DOI: 10.1186/1465-9921-7-95

Migratory marker expression in fibroblast foci of idiopathic pulmonary fibrosis

Marco Chilosi et al. Respir Res. 2006.

. 2006 Jun 30;7(1):95.

doi: 10.1186/1465-9921-7-95.

Authors

Marco Chilosi¹, Alberto Zamò, Claudio Doglioni, Daniela Reghellin, Maurizio Lestani, Licia Montagna, Serena Pedron, Maria Grazia Ennas, Alessandra Cancellieri, Bruno Murer, Venerino Poletti

Affiliation

¹ Department of Pathology, University of Verona, Strada Le Grazie 8, 37134 Verona, Italy. marco.chilosi@univr.it

PMID: 16813649
PMCID: PMC1538593
DOI: 10.1186/1465-9921-7-95

Abstract

Background: Fibroblast foci (FF) are considered a relevant morphologic marker of idiopathic pulmonary fibrosis/usual interstitial pneumonia (IPF/UIP), and are recognised as sites where fibrotic responses are initiated and/or perpetuated in this severe disease. Despite their relevance, the cellular and molecular mechanisms responsible for the formation of FF and their role in tissue remodelling are poorly defined. In previous studies we have provided evidence of abnormal activation of the wnt-signaling-pathway in IPF/UIP that is centred on FF and the overlying epithelium. This important morphogenetic pathway is able to trigger epithelial-mesenchymal-transition (EMT), a mechanism involved in developmental and metastatic processes, which is also potentially involved in pulmonary fibrosis.

Methods: Since EMT is characterised by enhancement of migratory potential of cells, we investigated the molecular profile of FF in 30 biopsies of IPF/UIP and a variety of control samples, focussing on the immunohistochemical expression of three molecules involved in cell motility and invasiveness, namely laminin-5-gamma2-chain, fascin, and heat-shock-protein-27.

Results: We provide evidence that in UIP these three molecules are abnormally expressed in discrete clusters of bronchiolar basal cells precisely localised in FF. These cellular clusters expressed laminin-5-gamma2-chain and heat-shock-protein-27 at very high levels, forming characteristic three-layered lesions defined as "sandwich-foci" (SW-FF). Upon quantitative analysis SW-FF were present in 28/30 UIP samples, representing more than 50% of recognisable FF in 21/30, but were exceedingly rare in a wide variety of lung pathologies examined as controls. In UIP, SW-FF were often observed in areas of microscopic honeycombing, and were also found at the interface between normal lung tissue and areas of dense scarring.

Conclusion: These molecular abnormalities strongly suggest that SW-FF represent the leading edge of pulmonary remodelling, where abnormal migration and re-epithelialisation take place, and that abnormal proliferation and migration of bronchiolar basal cells have a major role in the remodelling process characterising IPF/UIP. Further investigations will assess their possible use as reliable markers for better defining the UIP-pattern in difficult cases.

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Figures

**Figure 1**
**LAM5γ2 and HSP27 expression in FF of UIP biopsies**. Expression of LAM5γ2 (a, b, and c) and HSP27 (d, and e) in different cases of IPF/UIP. The immunoreactivity is similar for the two molecules, mainly restricted to basal cell sheets located between luminal bronchiolar cells and myofibroblast clusters of fibroblast foci (*sandwich*-FF).

**Figure 2**
**Characterisation on serial sections of the cells expressing LAM5γ2, fascin and HSP27 in "*sandwich*-FF" of UIP biopsies**. (a) A fibroblast focus is shown by tenascin immunostaining in a UIP biopsy at the edge between dense scarring and scarcely involved lung (square frame). In (b) The same FF is analysed for HSP27 (brown) and tenascin (red) by double-marker immunostaining. The same lesion was studied using serial sections, showing that surfactant SPA is not expressed by overlying epithelial cells (c), but a cluster of basal cells expresses high level of fascin (d) and MMP7/matrylisin (e). In dmyofibroblasts show discrete immunoreactivity for fascin. In the **f-g-h**sequence a "*sandwich-*FF" is shown, immunostained on serial sections for fascin (f), LAM5γ2 (g), and keratin-5, a marker of bronchiolar basal cells (h).

**Figure 3**
**Characterisation of "*sandwich*-FF" by double-marker immunostaining in UIP biopsies**. In (a) nuclear immunoreactivity of ΔN-p63 (brown-black), a well established marker of bronchiolar basal cells, clearly defines the nature of the cells expressing LAM5γ2 (cytoplasmic red immunoreactivity). In (b), another sandwich lesion immunostained by the double marker technique and showing strong expression of tenascin in the cluster of myofibroblasts is seen (red). The cluster of basal cells located between tenascin+ myofibroblasts and negative luminal bronchiolar cells strongly expresses LAM5γ2 (arrow).

**Figure 4**
**LAM5γ2 expression in control samples**. LAM5γ2 expression is observed in a subset of regenerating epithelial cells in cryptogenic organising pneumonia (COP, a), and diffuse alveolar damage/acute interstitial pneumonia (AIP/DAD, b), but is completely absent in allergic extrinsic alveolitis (AEA, c) and desquamative interstitial pneumonia (DIP, d), used as controls. In this UIP-like case (systemic sclerosis LAM5γ2 immunoreactivity was restricted to pneumocytes overlying FF (e, arrow), but the "sandwich" pattern was not observed despite the high number of fibroblast foci, as shown by tenascin immunostaining on serial sections (f, arrows).

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Migratory marker expression in fibroblast foci of idiopathic pulmonary fibrosis

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