Covalent and Density-Controlled Surface Immobilization of E-Cadherin for Adhesion Force Spectroscopy

Fichtner, Dagmar; Lorenz, Bärbel; Engin, Sinem; Deichmann, Christina; Oelkers, Marieelen; Janshoff, Andreas; Menke, André; Wedlich, Doris; Franz, Clemens M.

doi:10.1371/journal.pone.0093123

Cited by 41 publications

(62 citation statements)

References 54 publications

(75 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…2), albeit at levels much reduced when compared to RGD-conjugated gels (HAVDI attachment ~10% of RGD attachment). This is consistent with previous reports showing that the first two extracellular domains of N-Cadherin (in which the HAVDI sequence resides) allow for weak adhesive interactions when compared to the full ectodomain 41 . Next, we examined 1 mM: 1 mM peptide combinations of HAVDI and RGD across a physiologic range of substrate stiffness, and noted no significant difference in spread area between HAVDI/RGD and scram/RGD groups (Fig.…”

Section: Tunable Hydrogels Presenting Cell-cell and Cell-ecm Ligandssupporting

confidence: 93%

N-cadherin adhesive interactions modulate matrix mechanosensing and fate commitment of mesenchymal stem cells

et al. 2016

View full text Add to dashboard Cite

During mesenchymal development, the microenvironment gradually transitions from one that is rich in cell-cell interactions to one that is dominated by cell-extracellular-matrix (ECM) interactions. Because these cues cannot readily be decoupled in vitro or in vivo, how they converge to regulate mesenchymal stem cell (MSC) mechanosensing is not fully understood. Here, we show that a hyaluronic acid hydrogel system enables, across a physiological range of ECM stiffness, the independent co-presentation of the HAVDI adhesive motif from the EC1 domain of N-Cadherin and the RGD adhesive motif from fibronectin. Decoupled presentation of these cues revealed that HAVDI ligation (at constant RGD ligation) reduced the contractile state and thereby nuclear YAP/TAZ localization in MSCs, resulting in altered interpretation of ECM stiffness and subsequent changes in downstream cell proliferation and differentiation. Our findings reveal that, in an evolving developmental context, HAVDI/N-Cadherin interactions can alter stem cell perception of the stiffening extracellular microenvironment.

show abstract

Section: Tunable Hydrogels Presenting Cell-cell and Cell-ecm Ligandssupporting

confidence: 93%

N-cadherin adhesive interactions modulate matrix mechanosensing and fate commitment of mesenchymal stem cells

et al. 2016

View full text Add to dashboard Cite

show abstract

“…While classic trans cadherin bonds are mediated by homophilic strand swapping of an N-terminal tryptophan residue into a hydrophobic pocket of its binding partner 13 , we previously demonstrated that the trans tip-link bond has a far more extensive, amphiphilic "handshake" interface involving ~30 amino acids in the first two extracellular (EC) domains of each protein 8 . Although the dissociation constant of a single tip-link bond is approximately the same as for classic cadherins 8,[14][15][16][17][18] , little is known about how the tip-link bond responds to force.…”

Section: Main Textmentioning

confidence: 99%

“…1f). Compared with classic cadherins (mean lifetime ≈ 0.75 s, fβ ≈ 5.5 pN) [14][15][16][17][18] , the single tip-link bond is significantly more resistant to mechanical force (Fig. 1g).…”

Section: Main Textmentioning

confidence: 99%

The Dynamic Strength of the Hair-Cell Tip Link Reveals Mechanisms of Hearing and Deafness

Mulhall

Ward

Yang

et al. 2019

Preprint

View full text Add to dashboard Cite

Our senses of hearing and balance rely on the extraordinarily sensitive molecular machinery of the inner ear to convert deflections as small as the width of a single carbon atom 1,2 into electrical signals that the brain can process 3 . In humans and other vertebrates, transduction is mediated by hair cells 4 , where tension on tip links conveys force to mechanosensitive ion channels 5 . Each tip link comprises two helical filaments of atypical cadherins bound at their N-termini through two unique adhesion bonds 6-8 . Tip links must be strong enough to maintain a connection to the mechanotransduction channel under the dynamic forces exerted by sound or head movement-yet might also act as mechanical circuit breakers, releasing under extreme conditions to preserve the delicate structures within the hair cell. Previous studies have argued that this connection is exceptionally static, disrupted only by harsh chemical conditions or loud sound 9-12 . However, no direct mechanical measurements of the full tip-link connection have been performed. Here we describe the dynamics of the tiplink connection at single-molecule resolution and show how avidity conferred by its double stranded architecture enhances mechanical strength and lifetime, yet still enables it to act as a dynamic mechanical circuit breaker. We also show how the dynamic strength of the connection is facilitated by strong cisdimerization and tuned by extracellular Ca 2+ , and we describe the unexpected etiology of a hereditary human deafness mutation. Remarkably, the connection is several thousand times more dynamic than previously thought, challenging current assumptions about tip-link stability and turnover rate, and providing insight into how the mechanotransduction apparatus conveys mechanical information. Our results reveal fundamental mechanisms that underlie mechanoelectric transduction in the inner ear, and provide a foundation for studying multi-component linkages in other biological systems.

show abstract

“…Traditionally, cell-cell adhesion is described as being achieved by the symmetric interactions of the first extracellular domains (EC1) of cadherins on neighbouring cells (trans-interaction) [63,66]; cadherins on the same cell also interact with each other (cis-interaction) through the EC1 domain of one and the EC2 domain of the other [63,66,67]. More recently, it has been described that optimal cell-cell adhesion (50-70 pN) is achieved by all five EC domains of E-cadherin, and with a cellcell separation of 5-11 nm [64] ( figure 1). E-, P-and N-cadherin were the first cadherins identified, and can all mediate cell-cell adhesion in this fashion [62,68]: -E-cadherin (cadherin-1, 120 kDa): the main mediator of cell -cell adhesion in epithelial tissues and expressed by most normal epithelial cells [19,60,61,[68][69][70].…”

Section: Cadherinsmentioning

confidence: 99%

“…Traditionally, cadherins on neighbouring cells adhere via EC1 domains, although more recent research suggests that all five EC domains are required for optimal adhesion [64]. Figure 2.…”

Section: Cadherin Switchingmentioning

confidence: 99%

Cell adhesion and urothelial bladder cancer: the role of cadherin switching and related phenomena

Bryan

2015

Phil. Trans. R. Soc. B

View full text Add to dashboard Cite

Cadherins are mediators of cell-cell adhesion in epithelial tissues. E-cadherin is a known tumour suppressor and plays a central role in suppressing the invasive phenotype of cancer cells. However, the abnormal expression of N-and P-cadherin ('cadherin switching', CS) has been shown to promote a more invasive and m alignant phenotype of cancer, with P-cadherin possibly acting as a key mediator of invasion and metastasis in bladder cancer. Cadherins are also implicated in numerous signalling events related to embryonic development, tissue morphogenesis and homeostasis. It is these wide ranging effects and the serious implications of CS that make the cadherin cell adhesion molecules and their related pathways strong candidate targets for the inhibition of cancer progression, including bladder cancer. This review focuses on CS in the context of bladder cancer and in particular the switch to P-cadherin expression, and discusses other related molecules and phenomena, including EpCAM and the development of the cancer stem cell phenotype.

show abstract

Covalent and Density-Controlled Surface Immobilization of E-Cadherin for Adhesion Force Spectroscopy

Cited by 41 publications

References 54 publications

N-cadherin adhesive interactions modulate matrix mechanosensing and fate commitment of mesenchymal stem cells

N-cadherin adhesive interactions modulate matrix mechanosensing and fate commitment of mesenchymal stem cells

The Dynamic Strength of the Hair-Cell Tip Link Reveals Mechanisms of Hearing and Deafness

Cell adhesion and urothelial bladder cancer: the role of cadherin switching and related phenomena

Contact Info

Product

Resources

About