Integrins and integrin-related proteins in cardiac fibrosis

Chen, Chao; Li, Ruixia; Ross, Robert S.; Manso, Ana Maria

doi:10.1016/j.yjmcc.2015.11.010

Cited by 124 publications

(94 citation statements)

References 201 publications

(202 reference statements)

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“…Cardiomyocytes specifically interact with fibronectin on the cell surface via integrins which has been reviewed in this issue [73] and elsewhere [74, 75]. Though there are no studies that directly assess the functional role of fibronectin in the heart, findings from mouse models targeting members of the integrin complex suggest that cardiomyocyte disruption of fibronectin related interactions have detrimental effects on cardiac electrophysiology and function [74].…”

Section: Mechanisms Of Cardiomyocyte-fibroblast Communicationmentioning

confidence: 99%

Myocyte-fibroblast communication in cardiac fibrosis and arrhythmias: Mechanisms and model systems

Pellman¹,

Zhang²,

Sheikh

2016

Journal of Molecular and Cellular Cardiology

126

103

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Development of cardiac fibrosis and arrhythmias is controlled by the activity of and communication between cardiomyocytes and fibroblasts in the heart. Myocyte-fibroblast interactions occur via both direct and indirect means including paracrine mediators, extracellular matrix interactions, electrical modulators, mechanical junctions, and membrane nanotubes. In the diseased heart, cardiomyocyte and fibroblast ratios and activity, and thus myocyte-fibroblast interactions, change and are thought to contribute to the course of disease including development of fibrosis and arrhythmogenic activity. Fibroblasts have a developing role in modulating cardiomyocyte electrical and hypertrophic activity, however gaps in knowledge regarding these interactions still exist. Research in this field has necessitated the development of unique approaches to isolate and control myocyte-fibroblast interactions. Numerous methods for 2D and 3D co-culture systems have been developed, while a growing part of this field is in the use of better tools for in vivo systems including cardiomyocyte and fibroblast specific Cre mouse lines for cell type specific genetic ablation. This review will focus on (i) mechanisms of myocyte-fibroblast communication and their effects on disease features such as cardiac fibrosis and arrhythmias as well as (ii) methods being used and currently developed in this field.

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Section: Mechanisms Of Cardiomyocyte-fibroblast Communicationmentioning

confidence: 99%

Myocyte-fibroblast communication in cardiac fibrosis and arrhythmias: Mechanisms and model systems

Pellman¹,

Zhang²,

Sheikh

2016

Journal of Molecular and Cellular Cardiology

126

103

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“…Fibrotic diseases are defined by excessive deposition of fibrotic ECM molecules, increased tissue stiffness, and can occur in most any tissue although fibrosis of the liver, lung, kidney, and heart represent the major impacts of fibrosis on human health. Given the increased ECM present in fibrotic tissues, it is not surprising that integrins figure predominantly in the pathology of fibrosis [97-99]. Adding to this, it has become apparent that Notch is also an important regulator of fibrosis in the lung, liver, kidney, and skin [100, 101].…”

Section: Crosstalk Between Notch and Integrinsmentioning

confidence: 99%

Notch: A multi-functional integrating system of microenvironmental signals

LaFoya

Munroe

Mia

et al. 2016

Developmental Biology

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The Notch signaling cascade is an evolutionarily ancient system that allows cells to interact with their microenvironmental neighbors through direct cell-cell interactions, thereby directing a variety of developmental processes. Recent research is discovering that Notch signaling is also responsive to a broad variety of stimuli beyond cell-cell interactions, including: ECM composition, crosstalk with other signaling systems, shear stress, hypoxia, and hyperglycemia. Given this emerging understanding of Notch responsiveness to microenvironmental conditions, it appears that the classical view of Notch as a mechanism enabling cell-cell interactions, is only a part of a broader function to integrate microenvironmental cues. In this review, we summarize and discuss published data supporting the idea that the full function of Notch signaling is to serve as an integrator of microenvironmental signals thus allowing cells to sense and respond to a multitude of conditions around them.

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“…39 The cytosolic β1 integrin subunit is known to be activated in response to stretch and its expression is enhanced by the activity of Ang II. 39 The cytosolic β1 integrin subunit is known to be activated in response to stretch and its expression is enhanced by the activity of Ang II.…”

Section: Integrin Signallingmentioning

confidence: 99%

The slow force response to stretch: Controversy and contradictions

et al. 2019

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When exposed to an abrupt stretch, cardiac muscle exhibits biphasic active force enhancement. The initial, instantaneous, force enhancement is well explained by the Frank-Starling mechanism. However, the cellular mechanisms associated with the second, slower phase remain contentious. This review explores hypotheses regarding this "slow force response" with the intention of clarifying some apparent contradictions in the literature. The review is partitioned into three sections. The first section considers pathways that modify the intracellular calcium handling to address the role of the sarcoplasmic reticulum in the mechanism underlying the slow force response. The second section focuses on extracellular calcium fluxes and explores the identity and contribution of the stretch-activated, nonspecific, cation channels as well as signalling cascades associated with G-protein coupled receptors. The final section introduces promising candidates for the mechanosensor(s) responsible for detecting the stretch perturbation. K E Y W O R D SAnrep effect, cardiac mechanosensitivity, signalling pathway, slow force response

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Integrins and integrin-related proteins in cardiac fibrosis

Cited by 124 publications

References 201 publications

Myocyte-fibroblast communication in cardiac fibrosis and arrhythmias: Mechanisms and model systems

Myocyte-fibroblast communication in cardiac fibrosis and arrhythmias: Mechanisms and model systems

Notch: A multi-functional integrating system of microenvironmental signals

The slow force response to stretch: Controversy and contradictions

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