A cell adhesive peptide from tropoelastin promotes sequential cell attachment and spreading via distinct receptors

Lee, Pearl; Yeo, Giselle C.; Weiss, Anthony S.

doi:10.1111/febs.14114

Cited by 32 publications

(48 citation statements)

References 85 publications

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“…In contrast, we show that fibronectin in solution does not promote MSC proliferation, possibly due to poor cell recognition as its cell receptor binding sites become exposed only upon adsorption to a surface such as a collagen matrix (37). The effects of tropoelastin in solution are likely enabled by the inherent accessibility (35,38) of its cell binding regions (32,39,40). Before this work, soluble signaling factors derived from ECM proteins, including fibronectin, laminin, collagen, and elastin, were thought to be limited to peptides released by partial proteolysis, termed matrikines (41,42).…”

Section: Discussionmentioning

confidence: 75%

Soluble matrix protein is a potent modulator of mesenchymal stem cell performance

Yeo

Weiss

2019

Proc. Natl. Acad. Sci. U.S.A.

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We challenge the conventional designation of structural matrix proteins primarily as supporting scaffolds for resident cells. The extracellular matrix protein tropoelastin is classically regarded as a structural component that confers mechanical strength and resilience to tissues subject to repetitive elastic deformation. Here we describe how tropoelastin inherently induces a range of biological responses, even in cells not typically associated with elastic tissues and in a manner unexpected of typical substrate-dependent matrix proteins. We show that tropoelastin alone drives mesenchymal stem cell (MSC) proliferation and phenotypic maintenance, akin to the synergistic effects of potent growth factors such as insulin-like growth factor 1 and basic fibroblast growth factor. In addition, tropoelastin functionally surpasses these growth factors, as well as fibronectin, in allowing substantial media serum reduction without loss of proliferative potential. We further demonstrate that tropoelastin elicits strong mitogenic and cell-attractive responses, both as an immobilized substrate and as a soluble additive, via direct interactions with cell surface integrins αvβ3 and αvβ5. This duality of action converges the long-held mechanistic dichotomy between adhesive matrix proteins and soluble growth factors and uncovers the powerful, untapped potential of tropoelastin for clinical MSC expansion and therapeutic MSC recruitment. We propose that the potent, growth factor-like mitogenic and motogenic abilities of tropoelastin are biologically rooted in the need for rapid stem cell homing and proliferation during early development and/or wound repair.

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Section: Discussionmentioning

confidence: 75%

Soluble matrix protein is a potent modulator of mesenchymal stem cell performance

Yeo

Weiss

2019

Proc. Natl. Acad. Sci. U.S.A.

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“…This sequence works synergistically with integrins, where GAG‐binding allows the engagement of the α v integrin family to induce cell spreading . Domains that contribute to integrin binding reside in regions adjacent to the GAG‐binding sequence spanning domains 17 and 18 . We propose that the flexibility of the central region may therefore facilitate cell–receptor interactions by exposing relevant domains.…”

Section: Resultsmentioning

confidence: 94%

“…Second, the variability in domain positioning may promote cellular interaction. Earlier work suggests that the central region of the molecule interacts with cell surface receptors including glycosaminoglycans (GAGs) and integrins, promoting cell binding and cell spreading . In particular, domains 17 and 18 contain a glycosaminoglycan‐binding site responsible for cell adhesion.…”

Section: Resultsmentioning

confidence: 99%

“…In particular, domains 17 and 18 contain a glycosaminoglycan‐binding site responsible for cell adhesion. This sequence works synergistically with integrins, where GAG‐binding allows the engagement of the α v integrin family to induce cell spreading . Domains that contribute to integrin binding reside in regions adjacent to the GAG‐binding sequence spanning domains 17 and 18 .…”

Section: Resultsmentioning

confidence: 99%

“…Spherule formation through coacervation begins at the cell surface by surface‐tethered tropoelastin molecules, until released for integration into the growing elastic fiber. Tropoelastin aggregates adhere to the cell surface through GAG‐ and integrin–mediated interactions at specific interaction sites . Spherules are deposited on a microfibrillar scaffold where they are stabilized by cross‐links facilitated by lysyl oxidase and eventually integrated into a mature elastic fiber.…”

Section: Introductionmentioning

confidence: 99%

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Tropoelastin is a Flexible Molecule that Retains its Canonical Shape

Tarakanova

Yeo

Baldock

et al. 2018

Macromolecular Bioscience

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in elastic tissues including blood vessels, skin, and lungs. [1,2] The mature form of the secreted human tropoelastin monomer is 60 kDa [3] and is composed of an alternating pattern of repetitive, hydrophobic glycine-, valine-, and proline-rich domains spread out between lysine-containing cross-linking domains. [4] Traditionally described as a largely disordered molecule, recent studies suggest that tropoelastin is a flexible molecule with a distinct nanostructure [5][6][7] that determines its structural and cell-adhesive properties.Tropoelastin's distinct nanostructure determines its propensity to assemble into higher-order structures (Figure 1) through elastogenesis. [8] Elastogenesis begins with self-assembly of the ≈15 nm monomers, a process called coacervation. [9] Self-assembly, naturally occurring at physiological pH and salt conditions at 37 °C, results in spherical structures from 200 nm to 6 µm in diameter. [9][10][11] Spherule formation through coacervation begins at the cell surface by surface-tethered tropoelastin molecules, until released for integration into the growing elastic fiber. Tropoelastin aggregates adhere to the cell surface through GAG-and integrin-mediated interactions at specific interaction sites. [12][13][14][15][16][17][18] Spherules are deposited on a microfibrillar scaffold where they are stabilized Tropoelastin Tropoelastin is the dominant building block of elastic fibers, which form a major component of the extracellular matrix, providing structural support to tissues and imbuing them with elasticity and resilience. Recently, the atomistic structure of human tropoelastin is described, obtained through accelerated sampling via replica exchange molecular dynamics simulations. Here, principal component analysis is used to consider the ensemble of structures accessible to tropoelastin at body temperature (37 °C) at which tropoelastin naturally self-assembles into aggregated coacervates. These coacervates are relevant because they are an essential intermediate assembly stage, where tropoelastin molecules are then cross-linked at lysine residues and integrated into growing elastic fibers. It is found that the ensemble preserves the canonical tropoelastin structure with an extended molecular body flanked by two protruding legs, and identifies variations in specific domain positioning within this global shape. Furthermore, it is found that lysine residues show a large variation in their location on the tropoelastin molecule compared with other residues. It is hypothesized that this perturbation of the lysines increases their accessibility and enhances cross-linking. Finally, the principal component modes are extracted to describe the range of tropoelastin's conformational fluctuation to validate tropoelastin's scissor-twist motion that was predicted earlier.The ORCID identification number(s) for the author(s) of this article can be found under https://doi.

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Elastin‐Like Recombinamers: Deconstructing and Recapitulating the Functionality of Extracellular Matrix Proteins Using Recombinant Protein Polymers

Acosta

Quintanilla‐Sierra

Mbundi

et al. 2020

Adv Funct Materials

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In the development of tissue engineering strategies to replace, remodel, regenerate, or support damaged tissue, the development of bioinspired biomaterials that recapitulate the physicochemical characteristics of the extracellular matrix has received increased attention. Given the compositional heterogeneity and tissue-to-tissue variation of the extracellular matrix, the design, choice of polymer, crosslinking, and nature of the resulting biomaterials are normally depended on intended application. Generally, these biomaterials are usually made of degradable or nondegradable biomaterials that can be used as cell or drug carriers. In recent years, efforts to endow reciprocal biomaterial-cell interaction properties in scaffolds have inspired controlled synthesis, derivatization, and functionalization of the polymers used. In this regard, elastin-like recombinant proteins have generated interest and continue to be developed further owing to their modular design at a molecular level. In this review, the authors provide a summary of key extracellular matrix features relevant to biomaterials design and discuss current approaches in the development of extracellular matrix-inspired elastin-like recombinant protein based biomaterials.

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A cell adhesive peptide from tropoelastin promotes sequential cell attachment and spreading via distinct receptors

Cited by 32 publications

References 85 publications

Soluble matrix protein is a potent modulator of mesenchymal stem cell performance

Soluble matrix protein is a potent modulator of mesenchymal stem cell performance

Tropoelastin is a Flexible Molecule that Retains its Canonical Shape

Elastin‐Like Recombinamers: Deconstructing and Recapitulating the Functionality of Extracellular Matrix Proteins Using Recombinant Protein Polymers

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