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  5. An Agent-Based Model of Radiation-Induced Lung Fibrosis
 
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2022
Zweitveröffentlichung
Artikel
Verlagsversion

An Agent-Based Model of Radiation-Induced Lung Fibrosis

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TUDa URI
tuda/9823
URN
urn:nbn:de:tuda-tuprints-229737
DOI
10.26083/tuprints-00022973
Autor:innen
Cogno, Nicolò ORCID 0000-0003-4205-4640
Bauer, Roman
Durante, Marco ORCID 0000-0002-4615-553X
Kurzbeschreibung (Abstract)

Early- and late-phase radiation-induced lung injuries, namely pneumonitis and lung fibrosis (RILF), severely constrain the maximum dose and irradiated volume in thoracic radiotherapy. As the most radiosensitive targets, epithelial cells respond to radiation either by undergoing apoptosis or switching to a senescent phenotype that triggers the immune system and damages surrounding healthy cells. Unresolved inflammation stimulates mesenchymal cells’ proliferation and extracellular matrix (ECM) secretion, which irreversibly stiffens the alveolar walls and leads to respiratory failure. Although a thorough understanding is lacking, RILF and idiopathic pulmonary fibrosis share multiple pathways and would mutually benefit from further insights into disease progression. Furthermore, current normal tissue complication probability (NTCP) models rely on clinical experience to set tolerance doses for organs at risk and leave aside mechanistic interpretations of the undergoing processes. To these aims, we implemented a 3D agent-based model (ABM) of an alveolar duct that simulates cell dynamics and substance diffusion following radiation injury. Emphasis was placed on cell repopulation, senescent clearance, and intra/inter-alveolar bystander senescence while tracking ECM deposition. Our ABM successfully replicates early and late fibrotic response patterns reported in the literature along with the ECM sigmoidal dose-response curve. Moreover, surrogate measures of RILF severity via a custom indicator show qualitative agreement with published fibrosis indices. Finally, our ABM provides a fully mechanistic alveolar survival curve highlighting the need to include bystander damage in lung NTCP models.

Freie Schlagworte

agent-based modelling...

RILF

IPF

senescence

bystander

3D modelling

NTCP

Sprache
Englisch
Fachbereich/-gebiet
05 Fachbereich Physik > Institut für Physik Kondensierter Materie (IPKM)
DDC
500 Naturwissenschaften und Mathematik > 530 Physik
Institution
Universitäts- und Landesbibliothek Darmstadt
Ort
Darmstadt
Titel der Zeitschrift / Schriftenreihe
International Journal of Molecular Sciences
Jahrgang der Zeitschrift
23
Heftnummer der Zeitschrift
22
ISSN
1422-0067
Verlag
MDPI
Publikationsjahr der Erstveröffentlichung
2022
Verlags-DOI
10.3390/ijms232213920
PPN
50324192X
Zusätzliche Infomationen
This article belongs to the Special Issue Molecular and Cellular Mechanisms of Idiopathic Pulmonary Fibrosis and Interstitial Lung Diseases

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