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Journal ArticleDOI

A novel strategy to enhance interfacial adhesion in fiber-reinforced calcium phosphate cement

TL;DR: The aim of the present work was to improve the interfacial adhesion between fibers and matrix to obtain tougher biocompatible fiber-reinforced calcium phosphate cements (FRCPCs), which resulted in an increase of the work of fracture (several hundred-fold increase), while the elastic modulus and bending strength were maintained similar to the materials without additives.
Abstract: Calcium phosphate cements (CPCs) are extensively used as synthetic bone grafts, but their poor toughness limits their use to non-load-bearing applications. Reinforcement through introduction of fibers and yarns has been evaluated in various studies but always resulted in a decrease in elastic modulus or bending strength when compared to the CPC matrix. The aim of the present work was to improve the interfacial adhesion between fibers and matrix to obtain tougher biocompatible fiber-reinforced calcium phosphate cements (FRCPCs). This was done by adding a polymer solution to the matrix, with chemical affinity to the reinforcing chitosan fibers, namely trimethyl chitosan (TMC). The improved wettability and chemical affinity of the chitosan fibers with the TMC in the liquid phase led to an enhancement of the interfacial adhesion. This resulted in an increase of the work of fracture (several hundred-fold increase), while the elastic modulus and bending strength were maintained similar to the materials without additives. Additionally the TMC-modified CPCs showed suitable biocompatibility with an osteoblastic cell line.

Summary (2 min read)

Introduction

  • Synthetic bone grafts, but their poor toughness limits their use to nonload-bearing applications.
  • Reinforcement through introduction of fibers and yarns has been evaluated in various studies but always resulted in a decrease in elastic modulus or bending strength when compared to the CPC matrix.
  • The aim of the present work was to improve the interfacial adhesion between fibers and matrix to obtain tougher biocompatible fiberreinforced calcium phosphate cements .
  • This was done by adding a polymer solution to the matrix, with chemical affinity to the reinforcing chitosan fibers, namely trimethyl chitosan (TMC).
  • Additionally the TMC-modified CPCs showed suitable biocompatibility with an osteoblastic cell line.

A novel strategy to enhance interfacial adhesion in fiber-reinforced calcium phosphate

  • An improvement of the mechanical performance of these materials, and particularly a mitigation of their brittle behavior, would significantly extend the applicability of CPCs.
  • For the last 15 years, several strategies have been evaluated to reinforce CPCs with fibers (Canal & Ginebra 2011; Krüger & Groll 2012).
  • The excellent adhesion between the PMMA particles and the PMMA matrix is due to the chemical affinity between the liquid and the solid phase.
  • Thus, the aim of this work was to develop a biocompatible fiber-reinforced CPC with improved mechanical properties using chitosan as common polymer in the matrix and in the fibers, with the hypothesis that having an additive of similar nature would increase the chemical interactions between matrix and fibers, which would in turn result in a higher toughness.

2.1 Fiber reinforced calcium phosphate cements

  • Fiber-reinforced calcium phosphate cements were prepared by mixing a solid phase containing α-tricalcium phosphate (α-TCP) and chitosan fibers with a liquid phase.
  • The solid phase consisted of in-house made α-TCP obtained by solid-state reaction of a 2:1 molar mixture of calcium hydrogen phosphate (CaHPO4, Sigma–Aldrich C7263) and calcium carbonate (CaCO3, Sigma–Aldrich C4830) at 1400 °C for 15 h followed by quenching in air.
  • Detailed powder characteristics are described elsewhere (Espanol et al. 2009).
  • To prepare FRCPCs, chitosan fibers were mixed with the CPCs powder.
  • In all cases the specimens were set in Ringer’s solution (0.15 M sodium chloride solution) for 7 days at 37ºC.

2.2 Physico-chemical characterization

  • The static contact angle of chitosan films with water or 1 w/v % TMC solution as wetting liquids was evaluated.
  • It was not possible to measure the contact angle on CPCs –and their composites with chitosan fibers– due to their inherent microporosity and hydrophilicity.
  • The assay consists in determining the time needed for the Gillmore needle to fail to make a perceptible circular indentation on the cement surface, counting as time zero the start of mixing.
  • The cement’s phase composition was calculated with a semi-quantitative analysis (Chung 1974), which consisted in integrating the area of the three peaks with highest intensity and taking into account the reference intensity constant of their corresponding components.
  • The specimens were tested in wet conditions, right after extraction from the setting liquid (ASTM 2008).

2.3 Biological characterization

  • Pre-osteoblastic MG-63 cells (purchased from ATCC) were used to evaluate the effect of trimethyl chitosan modification of the cement matrix on the proliferation of the cells in direct contact with the materials.
  • Afterwards the samples were rinsed in sterile PBS and pre-incubated for 1 h with supplemented media at 37°C.
  • The absorbance values were transformed to cell number by using a standard curve.
  • The number of viable cells was visualized after 1, 3 and 7 days using live/dead staining kit (Life Technologies, USA).
  • The morphology of the MG-63 cells cultured on the cement specimens as well as the cement microstructures were visualized by Field Emission Scanning Electron Microscopy (FE-SEM, device: FIB Zeiss Neon40).

3. Results

  • The crystalline phases of the end-products of the cementitious reaction were analyzed after 7 days (Fig. 2, Table 3).
  • The addition of TMC in the liquid phase did not modify the toughness (measured as WOF) of the samples without fibers (C ≈ TMC).
  • Interestingly, the elastic modulus (Fig. 3b) of the cement containing both chitosan matrix and 8 wt% chitosan fibers (TMC-8f) was similar to that of a cement containing only TMC solution in the matrix, which highlights the relevance of adding TMC in the matrix to increase the fiber-matrix adhesion.
  • The pH of the media in contact with TMC samples was hardly modified, especially after 2 days and on, being between 7 and 7.4 for all the samples (Fig. 5b), so this is not expected to influence cell adhesion or proliferation.
  • The FRCPCs had a significantly improved toughness (measured as work of fracture) and at the same time the elastic modulus and bending strength were maintained in comparison to samples containing chitosan only as fibers or only as additive.

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TL;DR: In this article, the current state of knowledge and existing research on robocasting of calcium phosphate scaffolds are presented, and a meta-analysis of the compressive strength of these scaffolds is provided.

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Abstract: Calcium phosphate cements (CPCs) are frequently used as synthetic bone substitute materials due to their favorable osteocompatibility and handling properties. However, CPCs alone are inherently brittle and exhibit low strength and toughness, which restricts their clinical applicability to non-load bearing sites. Mechanical reinforcement of CPCs using fibers has proven to be an effective strategy to toughen these cements by transferring stress from the matrix to the fibers through frictional sliding at the interface. Therefore, tailoring the fiber-matrix affinity is paramount in designing highly toughened CPCs. However, the mechanistic correlation between this interaction and the macromechanical properties of fiber-reinforced CPCs has hardly been investigated to date. The aim of this study was to tailor the fiber-matrix interface affinity by modifying the surface of poly(vinyl alcohol) (PVA) fibers and correlate their interfacial properties to macromechanical properties (i.e. fracture toughness, work-of-fracture and tensile strength) of CPCs. Results from single fiber pullout tests reveal that the surface modification of PVA fibers increased their hydrophilicity and improved their affinity to the CPC matrix. This observation was evidenced by an increase in the interfacial shear strength and a reduction in the critical fiber embedment length (i.e. maximum embedded length from which a fiber can be pulled out without rupture). This increased interface affinity facilitated energy dissipation during fracture of CPCs subjected to macromechanical three-point flexure and tensile tests. The fracture toughness also significantly improved, even for CPCs reinforced with fibers of lengths greater than their critical fiber embedment length, suggesting that other crack-arresting mechanisms also play an important role in mechanically reinforcing CPCs. Overall, these basic insights will improve the understanding of the correlation between micro- and macromechanical characteristics of fiber-reinforced CPCs.

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Abstract: Bone tissue engineering aims to restore and maintain the function of bone by means of biomaterial-based scaffolds. This review specifically focuses on the use of fibers in biomaterials used for bone tissue engineering as suitable environment for bone tissue repair and regeneration. We present a bioinspired rationale behind the use of fibers in bone tissue engineering and provide an overview of the most common fiber fabrication methods, including solution, melt, and microfluidic spinning. Subsequently, we provide a brief overview of the composition of fibers that are used in bone tissue engineering, including fibers composed of (i) natural polymers (e.g., cellulose, collagen, gelatin, alginate, chitosan, and silk, (ii) synthetic polymers (e.g., polylactic acid [PLA], polycaprolactone, polyglycolic acid [PGA], polyethylene glycol, and polymer blends of PLA and PGA), (iii) ceramic fibers (e.g., aluminium oxide, titanium oxide, and zinc oxide), (iv) metallic fibers (e.g., titanium and its alloys, copper and magnesium), and (v) composite fibers. In addition, we review the most relevant fiber modification strategies that are used to enhance the (bio)functionality of these fibers. Finally, we provide an overview of the applicability of fibers in biomaterials for bone tissue engineering, with a specific focus on mechanical, pharmaceutical, and biological properties of fiber-functionalized biomaterials for bone tissue engineering. Impact statement Natural bone is a complex composite material composed of an extracellular matrix of mineralized fibers containing living cells and bioactive molecules. Consequently, the use of fibers in biomaterial-based scaffolds offers a wide variety of opportunities to replicate the functional performance of bone. This review provides an overview of the use of fibers in biomaterials for bone tissue engineering, thereby contributing to the design of novel fiber-functionalized bone-substituting biomaterials of improved functionality regarding their mechanical, pharmaceutical, and biological properties.

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TL;DR: The effort to enhance CPC's poor mechanical properties with micro-platelet reinforcement and impart antibacterial functionalities in composites with the aim to inhibit surgical site infections (SSI) was successful.
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TL;DR: Compared with the bone of adults, that of children had a lower modulus of elasticity, a lower bending strength, and a lower ash content, but the children's bone deflected more and absorbed more energy before breaking.
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  • ...derivative (Domard et al. 1986), was added to the cement liquid phase, and chitosan fibers were...

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