A semi-automatic pipeline integrating histological and µCT data in a mouse model of lung fibrosis

Elena Vincenzi; Martina Buccardi; Erica Ferrini; Alice Fantazzini; Eugenia Polverini; Gino Villetti; Nicola Sverzellati; Andrea Aliverti; Curzio Basso; Francesca Pennati; Franco Fabio Stellari

doi:10.1186/s12967-024-05819-y

Journal of Translational Medicine (Nov 2024)

A semi-automatic pipeline integrating histological and µCT data in a mouse model of lung fibrosis

Elena Vincenzi,
Martina Buccardi,
Erica Ferrini,
Alice Fantazzini,
Eugenia Polverini,
Gino Villetti,
Nicola Sverzellati,
Andrea Aliverti,
Curzio Basso,
Francesca Pennati,
Franco Fabio Stellari

Affiliations

Elena Vincenzi: Camelot Biomedical Systems S.R.L
Martina Buccardi: Department of Mathematical, Physical and Computer Sciences, University of Parma
Erica Ferrini: Molecular Imaging Facility, Experimental Pharmacology & Translational Science Department, Chiesi Farmaceutici S.P.A
Alice Fantazzini: Camelot Biomedical Systems S.R.L
Eugenia Polverini: Department of Mathematical, Physical and Computer Sciences, University of Parma
Gino Villetti: Molecular Imaging Facility, Experimental Pharmacology & Translational Science Department, Chiesi Farmaceutici S.P.A
Nicola Sverzellati: Department of Medicine and Surgery, University of Parma
Andrea Aliverti: Dipartimento di Elettronica, Informazione e Bioingegneria, Politecnico di Milano
Curzio Basso: Camelot Biomedical Systems S.R.L
Francesca Pennati: Dipartimento di Elettronica, Informazione e Bioingegneria, Politecnico di Milano
Franco Fabio Stellari: Molecular Imaging Facility, Experimental Pharmacology & Translational Science Department, Chiesi Farmaceutici S.P.A

DOI: https://doi.org/10.1186/s12967-024-05819-y
Journal volume & issue: Vol. 22, no. 1
pp. 1 – 15

Abstract

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Abstract Background Drug discovery strongly relies on the thorough evaluation of preclinical experimental studies. In the context of pulmonary fibrosis, micro-computed tomography (µCT) and histology are well-established and complementary tools for assessing, in animal models, disease progression and response to treatment. µCT offers dynamic, real-time insights into disease evolution and the effects of therapies, while histology provides a detailed microscopic examination of lung tissue. Here, we present a semi-automatic pipeline that integrates these readouts by matching individual µCT volume slices with the corresponding histological sections, effectively linking densitometric data with Ashcroft score measurements. Methods The tool first geometrically aligns the vertical axis of the µCT volume with the cutting plane used to prepare the histological sample. Then, focusing on the left lung, it computes the affine registration that identifies the µCT coronal slice that best matches the histological section. Finally, quantitative µCT imaging parameters are extracted from the selected slice. In a proof-of-concept test, the tool was applied to a bleomycin-induced mouse model of lung fibrosis. Results The proposed approach demonstrated high accuracy and time effectiveness in matching µCT and histological sections minimizing manual intervention, with an overall success rate of 95%, and reduced time required to align µCT and histological data from 40 to 5 min. Significant correlations were found between quantitative data derived from µCT and histology data. Conclusions The precise combination of microscopic ex-vivo information with 3D in-vivo data enhances the accuracy and representativeness of tissue analysis and provides a structural context for omic studies, serving as the foundation for a multi-layer platform. By facilitating a detailed and objective view of disease progression and treatment response, this approach has the potential to accelerate the development of effective therapies for lung fibrosis.

Published in Journal of Translational Medicine

ISSN: 1479-5876 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://translational-medicine.biomedcentral.com/

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Abstract

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