Thermodynamic and Hydrodynamic Properties of Human Tropoelastin

Toonkool, Prachumporn; Regan, David G.; Kuchel, Philip W.; Morris, Mitchell; Weiss, Anthony S.

doi:10.1074/jbc.m103391200

Cited by 41 publications

(19 citation statements)

References 40 publications

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“…Supplemental Figure S2 shows the hydrodynamic radius (Rh) vs. intensity distribution of all silk-tropoelastin samples in 0.1-wt% solution (SE0, SE10, SE25, SE50, SE75, SE90, and SE100). Notably, scattered light at a hydrodynamic radius (Rh) of around 6 nm with a predicted molecular weight of 59±12 kDa for sample SE0 is due to pure tropoelastin monomers in solution, as previously reported 35, 36 . In contrast, pure silk (SE100) showed strong intensity of scattered light at Rh of 57.1±9.1 nm and a predicted molecular weight of 427±84 kDa, indicating that silk monomers and some small silk aggregates were formed in solution 12, 22 .…”

Section: Resultssupporting

confidence: 79%

Charge‐Tunable Autoclaved Silk‐Tropoelastin Protein Alloys That Control Neuron Cell Responses

Tang-Schomer

Huang

et al. 2013

Adv Funct Materials

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Tunable protein composites are important for constructing extracellular matrix mimics of human tissues with control of biochemical, structural, and mechanical properties. Molecular interaction mechanisms between silk fibroin protein and recombinant human tropoelastin, based on charge, are utilized to generate a new group of multifunctional protein alloys (mixtures of silk and tropoelastin) with different net charges. These new biomaterials are then utilized as a biomaterial platform to control neuron cell response. With a +38 net charge in water, tropoelastin molecules provide extraordinary elasticity and selective interactions with cell surface integrins. In contrast, negatively charged silk fibroin protein (net charge −36) provides remarkable toughness and stiffness with morphologic stability in material formats via autoclaving-induced beta-sheet crystal physical crosslinks. The combination of these properties in alloy format extends the versatility of both structural proteins, providing a new biomaterial platform. The alloys with weak positive charges (silk/tropoelastin mass ratio 75/25, net charge around +16) significantly improved the formation of neuronal networks and maintained cell viability of rat cortical neurons after 10 days in vitro. The data point to these protein alloys as an alternative to commonly used poly-L-lysine (PLL) coatings or other charged synthetic polymers, particularly with regard to the versatility of material formats (e.g., gels, sponges, films, fibers). The results also provide a practical example of physically designed protein materials with control of net charge to direct biological outcomes, in this case for neuronal tissue engineering.

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Section: Resultssupporting

confidence: 79%

Charge‐Tunable Autoclaved Silk‐Tropoelastin Protein Alloys That Control Neuron Cell Responses

Tang-Schomer

Huang

et al. 2013

Adv Funct Materials

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“…Results from previous experiments proposed a nucleationcondensation model for coacervation of full-length tropoelastin SHEL⌬26A at 37°C (21). This model, together with the putative dominant role for domains 18, 20, 24, and 26 during coacervation, suggested that even though SHEL17-27 did not coacervate at 37°C, it may have been able to self-polymerize as part of the nucleation phase prior to coacervation.…”

Section: Resultsmentioning

confidence: 99%

“…These results indicated a greater capacity for intermolecular interactions by SHEL17-27 compared with individual hydrophobic domains. It is possible that at a sufficiently high concentration, SHEL17-27 could form a high molecular weight oligomer that may be representative of the nucleating species for the nucleation-condensation model described for tropoelastin (21). These oligomers, however, may not necessarily be dimers and do not account for the coacervation of full-length tropoelastin under physiologically relevant conditions at 37°C.…”

Section: Discussionmentioning

confidence: 99%

Hydrophobic Domains of Human Tropoelastin Interact in a Context-dependent Manner

Toonkool¹,

Jensen

Maxwell

et al. 2001

Journal of Biological Chemistry

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Tropoelastin is the soluble precursor of elastin, the major component of the extracellular elastic fiber. Tropoelastin undergoes self-association via an inverse temperature transition termed coacervation, which is a crucial step in elastogenesis. Coacervation of tropoelastin takes place through multiple intermolecular interactions of its hydrophobic domains. Previous work has implicated those hydrophobic domains located near the center of the polypeptide as playing a dominant role in coacervation. Short constructs of domains 18, 20, 24, and a mutated form of domain 26 were largely disordered at 20°C but displayed increased order on heating that was consistent with the formation of ␤-structures. However, their conformational transitions were not sensitive to physiological temperature in contrast to the observed behavior of the native domain 26. A polypeptide consisting of domains 17-27 of tropoelastin coacervated at temperatures above 60°C, whereas individually expressed hydrophobic regions were not capable of coacervation. We conclude that coacervation depends on the hydrophobicity of the molecule and, by inference, the number of hydrophobic domains. Tropoelastin mutants were constructed to contain a Pro 3 Ala mutation in domain 26, separate deletions of domains 18 and 26, and a displacement of domain 26. These constructs displayed unequal capacities for coacervation, even when they contained the same number of hydrophobic regions and comparable levels of secondary structure. Thus, the capability for coacervation is determined by contributions from individual hydrophobic domains for which function should be considered in the context of their positions in the intact tropoelastin molecule.

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“…Elastin resilience is afforded by the formation of insoluble fibers, the first step of which involves the selfalignment of elastin monomers, tropoelastin, in a temperature-induced transition known as coacervation, through the association of hydrophobic domains (1,2). Although highly (Ͼ75%) non-polar in character, tropoelastin remains predominantly monomeric and structurally disordered in solution (3)(4)(5) and critically, retains substantial backbone hydration and flexibility even when assembled (6) and cross-linked into mature, polymeric elastic arrays (7)(8)(9)(10)(11)(12)(13).…”

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confidence: 99%

Proline Periodicity Modulates the Self-assembly Properties of Elastin-like Polypeptides

Muiznieks

Keeley

2010

Journal of Biological Chemistry

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Elastin is a self-assembling protein of the extracellular matrix that provides tissues with elastic extensibility and recoil. The monomeric precursor, tropoelastin, is highly hydrophobic yet remains substantially disordered and flexible in solution, due in large part to a high combined threshold of proline and glycine residues within hydrophobic sequences. In fact, proline-poor elastin-like sequences are known to form amyloidlike fibrils, rich in ␤-structure, from solution. On this basis, it is clear that hydrophobic elastin sequences are in general optimized to avoid an amyloid fate. However, a small number of hydrophobic domains near the C terminus of tropoelastin are substantially depleted of proline residues. Here we investigated the specific contribution of proline number and spacing to the structure and self-assembly propensities of elastin-like polypeptides. Increasing the spacing between proline residues significantly decreased the ability of polypeptides to reversibly self-associate. Real-time imaging of the assembly process revealed the presence of smaller colloidal droplets that displayed enhanced propensity to cluster into dense networks. Structural characterization showed that these aggregates were enriched in ␤-structure but unable to bind thioflavin-T. These data strongly support a model where proline-poor regions of the elastin monomer provide a unique contribution to assembly and suggest a role for localized ␤-sheet in mediating self-assembly interactions.Elastin is the extracellular matrix protein responsible for the elasticity of vertebrate arterial vessels, connective tissues, lung, and skin. Elastin resilience is afforded by the formation of insoluble fibers, the first step of which involves the selfalignment of elastin monomers, tropoelastin, in a temperature-induced transition known as coacervation, through the association of hydrophobic domains (1, 2). Although highly (Ͼ75%) non-polar in character, tropoelastin remains predominantly monomeric and structurally disordered in solution (3-5) and critically, retains substantial backbone hydration and flexibility even when assembled (6) and cross-linked into mature, polymeric elastic arrays (7-13).Maintenance of structural heterogeneity and dynamics of the elastin backbone is achieved in large part by a high proportional composition of both proline (14%) and glycine (35%) residues within hydrophobic sequences (6, 14). These residues are commonly arranged into repeated motifs based on recurring sequence elements such as PGV and GVA. This includes a seven-fold tandem PGVGVA repeat in domain 24 of the native human elastin sequence (15). Contrary to enhancing coacervation or elastomeric properties, the multiple substitution of glycine residues for prolines within tandem repeat sequences (e.g. PGVGVA to GGVGVA) results in the formation of amyloid-like fibrils, rich in ␤-structure, from solution (6, 14). These structures are conformationally more restricted than native elastomeric sequences as a result of the tighter packing of residues into extended...

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Thermodynamic and Hydrodynamic Properties of Human Tropoelastin

Cited by 41 publications

References 40 publications

Charge‐Tunable Autoclaved Silk‐Tropoelastin Protein Alloys That Control Neuron Cell Responses

Charge‐Tunable Autoclaved Silk‐Tropoelastin Protein Alloys That Control Neuron Cell Responses

Hydrophobic Domains of Human Tropoelastin Interact in a Context-dependent Manner

Proline Periodicity Modulates the Self-assembly Properties of Elastin-like Polypeptides

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