Development and maintenance of force and stiffness in airway smooth muscle

Airway smooth muscle (ASM) plays a central role in the excessive narrowing of the airway that characterizes the primary functional impairment in asthma. This phenomenon is known as airway hyper-responsiveness (AHR). Emerging evidence suggests that the development and maintenance of ASM force involves dynamic reorganization of the subcellular filament network in both the cytoskeleton and the contractile apparatus. In this review, evidence is presented to support the view that regulation of ASM contraction extends beyond the classical actomyosin interaction and involves processes within the cytoskeleton and at the interfaces between the cytoskeleton, the contractile apparatus, and the extracellular matrix. These processes are initiated when the muscle is activated, and collectively they cause the cytoskeleton and the contractile apparatus to undergo structural transformation, resulting in a more connected and solid state that allows force generated by the contractile apparatus to be transmitted to the extracellular domain. Solidification of the cytoskeleton also serves to stiffen the muscle and hence the airway. Oscillatory strain from tidal breathing and deep inspiration is believed to be the counter balance that prevents hypercontraction and stiffening of ASM in vivo. Dysregulation of this balance could lead to AHR seen in asthma.

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The Strain on Airway Smooth Muscle During a Deep Inspiration to Total Lung Capacity

Journal of Engineering and Science in Medical Diagnostics and Therapy ◽

10.1115/1.4042309 ◽

2019 ◽

Vol 2 (1) ◽

Cited By ~ 1

Author(s):

Ynuk Bossé

Keyword(s):

Smooth Muscle ◽

Airway Smooth Muscle ◽

Total Lung Capacity ◽

In Vitro Studies ◽

Deep Inspiration ◽

Bronchodilator Effect ◽

Lung Capacity ◽

Residual Capacity

The deep inspiration (DI) maneuver entices a great deal of interest because of its ability to temporarily ease the flow of air into the lungs. This salutary effect of a DI is proposed to be mediated, at least partially, by momentarily increasing the operating length of airway smooth muscle (ASM). Concerningly, this premise is largely derived from a growing body of in vitro studies investigating the effect of stretching ASM by different magnitudes on its contractility. The relevance of these in vitro findings remains uncertain, as the real range of strains ASM undergoes in vivo during a DI is somewhat elusive. In order to understand the regulation of ASM contractility by a DI and to infer on its putative contribution to the bronchodilator effect of a DI, it is imperative that in vitro studies incorporate levels of strains that are physiologically relevant. This review summarizes the methods that may be used in vivo in humans to estimate the strain experienced by ASM during a DI from functional residual capacity (FRC) to total lung capacity (TLC). The strengths and limitations of each method, as well as the potential confounders, are also discussed. A rough estimated range of ASM strains is provided for the purpose of guiding future in vitro studies that aim at quantifying the regulatory effect of DI on ASM contractility. However, it is emphasized that, owing to the many limitations and confounders, more studies will be needed to reach conclusive statements.

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Molecular Mechanisms for the Mechanical Modulation of Airway Responsiveness

Journal of Engineering and Science in Medical Diagnostics and Therapy ◽

10.1115/1.4042775 ◽

2019 ◽

Vol 2 (1) ◽

Cited By ~ 2

Author(s):

Wenwu Zhang ◽

Susan J. Gunst

Keyword(s):

Extracellular Matrix ◽

Smooth Muscle ◽

Airway Smooth Muscle ◽

Actin Polymerization ◽

Molecular Mechanisms ◽

Airway Responsiveness ◽

Small Gtpase ◽

Cortical Actin

The smooth muscle of the airways is exposed to continuously changing mechanical forces during normal breathing. The mechanical oscillations that occur during breathing have profound effects on airway tone and airway responsiveness both in experimental animals and humans in vivo and in isolated airway tissues in vitro. Experimental evidence suggests that alterations in the contractile and mechanical properties of airway smooth muscle tissues caused by mechanical perturbations result from adaptive changes in the organization of the cytoskeletal architecture of the smooth muscle cell. The cytoskeleton is a dynamic structure that undergoes rapid reorganization in response to external mechanical and pharmacologic stimuli. Contractile stimulation initiates the assembly of cytoskeletal/extracellular matrix adhesion complex proteins into large macromolecular signaling complexes (adhesomes) that undergo activation to mediate the polymerization and reorganization of a submembranous network of actin filaments at the cortex of the cell. Cortical actin polymerization is catalyzed by Neuronal-Wiskott–Aldrich syndrome protein (N-WASP) and the Arp2/3 complex, which are activated by pathways regulated by paxillin and the small GTPase, cdc42. These processes create a strong and rigid cytoskeletal framework that may serve to strengthen the membrane for the transmission of force generated by the contractile apparatus to the extracellular matrix, and to enable the adaptation of smooth muscle cells to mechanical stresses. This model for the regulation of airway smooth muscle function can provide novel perspectives to explain the normal physiologic behavior of the airways and pathophysiologic properties of the airways in asthma.

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An Evolving Network Model of Airway Smooth Muscle Crossbridge Dynamics and Length Adaptation

Volume 2: Biomedical and Biotechnology Engineering ◽

10.1115/imece2008-66826 ◽

2008 ◽

Author(s):

G. Ijpma ◽

A. M. Al-Jumaily ◽

S. P. Cairns

Keyword(s):

Smooth Muscle ◽

Airway Smooth Muscle ◽

Driving Mechanism ◽

Deep Inspiration ◽

Glassy Material ◽

Physiological Loading ◽

Normal Breathing ◽

Contractile Forces ◽

Filament Network

The main driving mechanism in asthmatic attacks is the contraction of airway smooth muscle (ASM). Physiological loading of ASM by normal breathing and deep inspiration has been shown to reduce ASM contractile force. Our research involves the development of a mathematical model to describe the dynamic behavior of ASM. In this model length adaptation is described by an evolving filament network of passive and active elements in parallel with a soft glassy material. Contractile forces are described by the evolving force length characteristics of some of the network links. It is envisaged that the model will bridge the gap between passive ASM dynamics and contractile dynamics. The model will be validated using experimental data from testing of ASM tissues in vitro.

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Invited Review: Do inflammatory mediators influence the contribution of airway smooth muscle contraction to airway hyperresponsiveness in asthma?

Journal of Applied Physiology ◽

10.1152/japplphysiol.00192.2003 ◽

2003 ◽

Vol 95 (2) ◽

pp. 844-853 ◽

Cited By ~ 56

Author(s):

Darren J. Fernandes ◽

Richard W. Mitchell ◽

Oren Lakser ◽

Maria Dowell ◽

Alastair G. Stewart ◽

...

Keyword(s):

Smooth Muscle ◽

Airway Smooth Muscle ◽

Inflammatory Mediators ◽

Airway Hyperresponsiveness ◽

Molecular Mechanisms ◽

Normal Subjects ◽

Smooth Muscle Contraction ◽

Deep Inspiration ◽

Contractile Apparatus ◽

Muscle Shortening

It is now accepted that a host of cytokines, chemokines, growth factors, and other inflammatory mediators contributes to the development of nonspecific airway hyperresponsiveness in asthma. Yet, relatively little is known about how inflammatory mediators might promote airway structural remodeling or about the molecular mechanisms by which they might exaggerate smooth muscle shortening as observed in asthmatic airways. Taking a deep inspiration, which provides relief of bronchodilation in normal subjects, is less effective in asthmatic subjects, and some have speculated that this deficiency stems directly from an abnormality of airway smooth muscle and results in airway hyperresponsiveness to constrictor agonists. Here, we consider some of the mechanisms by which inflammatory mediators might acutely or chronically induce changes in the contractile apparatus that in turn might contribute to hyperresponsive airways in asthma.

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Airway narrowing and response to simulated deep inspiration in bronchial segments from subjects with fixed airflow obstruction

Journal of Applied Physiology ◽

10.1152/japplphysiol.00439.2019 ◽

2020 ◽

Vol 128 (4) ◽

pp. 757-767

Author(s):

Alvenia Cairncross ◽

Robyn L. Jones ◽

John G. Elliot ◽

Peter K. McFawn ◽

Alan L. James ◽

...

Keyword(s):

Extracellular Matrix ◽

Smooth Muscle ◽

Airway Smooth Muscle ◽

Volume Fraction ◽

Airflow Obstruction ◽

Deep Inspiration ◽

Airway Wall ◽

Airway Narrowing ◽

Fixed Airflow Obstruction

The volume fraction of extracellular matrix (ECM) within the layer of airway smooth muscle (ASM) is increased in subjects with fixed airflow obstruction. We postulated that changes in ECM within the ASM layer will impact force transmission during induced contraction and/or in response to externally applied stresses like a deep inspiration (DI). Subjects were patients undergoing lung resection surgery who were categorized as unobstructed ( n = 12) or “fixed” obstructed ( n = 6) on the basis of preoperative spirometry. The response to a DI, assessed by the ratio of isovolumic flows from maximal and partial inspirations (M/P), was also measured preoperatively. M/P was reduced in the obstructed group ( P = 0.02). Postoperatively, bronchial segments were obtained from resected tissue, and luminal narrowing to acetylcholine and bronchodilation to simulated DI were assessed in vitro. Airway wall dimensions and the volume fraction of ECM within the ASM were quantified. Maximal airway narrowing to acetylcholine ( P = 0.01) and the volume fraction of ECM within the ASM layer ( P = 0.02) were increased in the obstructed group, without a change in ASM thickness. Whereas bronchodilation to simulated DI in vitro was not different between obstructed and unobstructed groups, it was correlated with increased M/P (bronchodilation/less bronchoconstriction) in vivo ( P = 0.03). The volume fraction of ECM was inversely related to forced expiratory volume in 1 s FEV1 %predicted ( P = 0.04) and M/P ( P = 0.01). Results show that in subjects with fixed airflow obstruction the mechanical behavior of the airway wall is altered and there is a contemporaneous shift in the structural composition of the ASM layer. NEW & NOTEWORTHY Cartilaginous airways from subjects with fixed airflow obstruction have an increase in the volume fraction of extracellular matrix within the airway smooth muscle layer. These airways are also intrinsically more reactive to a contractile stimulus, which is expected to contribute to airway hyperresponsiveness in this population, often attributed to geometric mechanisms. In view of these results, we speculate on how changes in extracellular matrix may impact airway mechanics.

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Length oscillation mimicking periodic individual deep inspirations during tidal breathing attenuates force recovery and adaptation in airway smooth muscle

Journal of Applied Physiology ◽

10.1152/japplphysiol.00676.2010 ◽

2010 ◽

Vol 109 (5) ◽

pp. 1476-1482 ◽

Cited By ~ 12

Author(s):

Abdul Raqeeb ◽

Dennis Solomon ◽

Peter D. Paré ◽

Chun Y. Seow

Keyword(s):

Smooth Muscle ◽

Airway Smooth Muscle ◽

Prolonged Exposure ◽

Dynamic Environment ◽

Muscle Length ◽

Deep Inspiration ◽

Tidal Breathing ◽

Maximal Force ◽

Force Recovery ◽

Static Conditions

Airway smooth muscle (ASM) is able to generate maximal force under static conditions, and this isometric force can be maintained over a large length range due to length adaptation. The increased force at short muscle length could lead to excessive narrowing of the airways. Prolonged exposure of ASM to submaximal stimuli also increases the muscle's ability to generate force in a process called force adaptation. To date, the effects of length and force adaptation have only been demonstrated under static conditions. In the mechanically dynamic environment of the lung, ASM is constantly subjected to periodic stretches by the parenchyma due to tidal breathing and deep inspiration. It is not known whether force recovery due to muscle adaptation to a static environment could occur in a dynamic environment. In this study the effect of length oscillation mimicking tidal breathing and deep inspiration was examined. Force recovery after a length change was attenuated in the presence of length oscillation, except at very short lengths. Force adaptation was abolished by length oscillation. We conclude that in a healthy lung (with intact airway-parenchymal tethering) where airways are not allowed to narrow excessively, large stretches (associated with deep inspiration) may prevent the ability of the muscle to generate maximal force that would occur under static conditions irrespective of changes in mean length; mechanical perturbation on ASM due to tidal breathing and deep inspiration, therefore, is the first line of defense against excessive bronchoconstriction that may result from static length and force adaptation.

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Elastase alters contractility and promotes an inflammatory synthetic phenotype in airway smooth muscle tissues

AJP Lung Cellular and Molecular Physiology ◽

10.1152/ajplung.00334.2017 ◽

2018 ◽

Vol 314 (4) ◽

pp. L626-L634 ◽

Cited By ~ 7

Author(s):

Angelia D. Lockett ◽

Yidi Wu ◽

Susan J. Gunst

Keyword(s):

Extracellular Matrix ◽

Smooth Muscle ◽

Airway Smooth Muscle ◽

Inflammatory Cells ◽

Contractile Force ◽

Airway Hyperreactivity ◽

Inflammatory Phenotype ◽

Increased Sensitivity

Neutrophil elastase is secreted by inflammatory cells during airway inflammation and can elicit airway hyperreactivity in vivo. Elastase can degrade multiple components of the extracellular matrix. We hypothesized that elastase might disrupt the connections between airway smooth muscle (ASM) cells and the extracellular matrix and that this might have direct effects on ASM tissue responsiveness and inflammation. The effect of elastase treatment on ASM contractility was assessed in vitro in isolated strips of canine tracheal smooth muscle by stimulation of tissues with cumulatively increasing concentrations of acetylcholine (ACh) and measurement of contractile force. Elastase treatment potentiated contractile responses to ACh at low concentrations but suppressed the maximal contractile force generated by the tissues without affecting the phosphorylation of myosin regulatory light chain (RLC). Elastase also promoted the secretion of eotaxin and the activation of Akt in ASM tissues and decreased expression of smooth muscle myosin heavy chain, consistent with promotion of a synthetic inflammatory phenotype. As the degradation of matrix proteins can alter integrin engagement, we evaluated the effect of elastase on the assembly and activation of integrin-associated adhesion junction complexes in ASM tissues. Elastase led to talin cleavage, reduced talin binding to vinculin, and suppressed activation of the adhesome proteins paxillin, focal adhesion kinase, and vinculin, indicating that elastase causes the disassembly of adhesion junction complexes and the inactivation of adhesome signaling proteins. We conclude that elastase promotes an inflammatory phenotype and increased sensitivity to ACh in ASM tissues by disrupting signaling pathways mediated by integrin-associated adhesion complexes.

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Inhibition of dihydropyridine-sensitive calcium entry in hypoxic relaxation of airway smooth muscle

AJP Lung Cellular and Molecular Physiology ◽

10.1152/ajplung.1995.268.2.l201 ◽

1995 ◽

Vol 268 (2) ◽

pp. L201-L206 ◽

Cited By ~ 2

Author(s):

C. Vannier ◽

T. L. Croxton ◽

L. S. Farley ◽

C. A. Hirshman

Keyword(s):

Smooth Muscle ◽

Airway Smooth Muscle ◽

Muscle Tone ◽

Bay K 8644 ◽

O2 Concentration ◽

Voltage Dependent ◽

Progressive Hypoxia ◽

Carbamyl Choline

Hypoxia dilates airways in vivo and reduces active tension of airway smooth muscle in vitro. To determine whether hypoxia impairs Ca2+ entry through voltage-dependent channels (VDC), we tested the ability of dihydropyridines to modulate hypoxia-induced relaxation of KCl- and carbamyl choline (carbachol)-contracted porcine bronchi. Carbachol- or KCl-contracted bronchial rings were exposed to progressive hypoxia in the presence or absence of 1 microM BAY K 8644 (an L-type-channel agonist). In separate experiments, rings were contracted with carbachol or KCl, treated with nifedipine (a VDC antagonist), and finally exposed to hypoxia. BAY K 8644 prevented hypoxia-induced relaxation in KCl-contracted bronchi. Nifedipine (10(-5) M) totally relaxed KCl- contracted bronchi. Carbachol-contracted bronchi were only partially relaxed by nifedipine but were completely relaxed when the O2 concentration of the gas was reduced from 95 to 0%. These data indicate that hypoxia can reduce airway smooth muscle tone by limiting entry of Ca2+ through a dihydropyridine-sensitive pathway, but that other mechanisms also contribute to hypoxia-induced relaxation of carbachol-contracted bronchi.

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