3 research outputs found

    Data from: Mechanical factors direct mouse aortic remodeling during early maturation

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    Numerous diseases have been linked to genetic mutations that lead to reduced amounts or disorganization of arterial elastic fibres. Previous work has shown that mice with reduced amounts of elastin (Eln+/βˆ’) are able to live a normal lifespan through cardiovascular adaptations, including changes in haemodynamic stresses, arterial geometry and arterial wall mechanics. It is not known if the timeline and presence of these adaptations are consistent in other mouse models of elastic fibre disease, such as those caused by the absence of fibulin-5 expression (Fbln5βˆ’/βˆ’). Adult Fbln5βˆ’/βˆ’ mice have disorganized elastic fibres, decreased arterial compliance and high blood pressure. We examined mechanical behaviour of the aorta in Fbln5βˆ’/βˆ’ mice through early maturation when the elastic fibres are being assembled. We found that the physiologic circumferential stretch, stress and modulus of Fbln5βˆ’/βˆ’ aorta are maintained near wild-type levels. Constitutive modelling suggests that elastin contributions to the total stress are decreased, whereas collagen contributions are increased. Understanding how collagen fibre structure and mechanics compensate for defective elastic fibres to meet the mechanical requirements of the maturing aorta may help to better understand arterial remodelling in human elastinopathies

    Data for fitting constitutive model

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    Pressure, diameter, force, and axial stretch data combined for six loading protocols and used to fit the constitutive model in the manuscript. Unloaded dimensions for each aorta are also included
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