原位复合法制备层状结构的壳聚糖/羟基磷灰石纳米材料

用原位复合法制备了高性能的壳聚糖/羟基磷灰石(CS/HA)纳米复合材料.用预先沉积的壳聚糖膜将含有羟基磷灰石前驱体的壳聚糖溶液与凝固液隔离,同时控制壳聚糖沉积与羟基磷灰石前驱体转化为羟基磷灰石的过程,使其缓慢且有序地进行.当pH值改变时,质子化的壳聚糖分子链在负电层诱导下有序沉积并形成层状结构与羟基磷灰石原位生成CS/HA,并实现二者分子级复合.XRD和TEM测试证实原位生成的磷酸盐是羟基磷灰石,且其颗粒长约为100nm,宽30～50nm.SEM结果表明,用原位复合法制备的材料具有层状结构,CS/HA(质量比100/5)纳米复合材料弯曲强度高达86MPa,比松质骨的高3～4倍,相当于密质骨的1/2,有望用于可承重部位的组织修复材料.     

庆大霉素对羟基磷灰石/壳聚糖复合材料性能的影响

羟基磷灰石/壳聚糖-庆大霉素(HA/CS-G)缓释材料为骨髓炎的定点缓释给药提供了一种有效的局部药物缓释体系。为了研究抗生素对羟基磷灰石/壳聚糖材料性能的影响,采用共沉淀法制备了HA/CS-G缓释材料。利用红外光谱(IR)、X射线衍射(XRD)和扫描电子显微镜(SEM)对材料进行了表征。以不载药的羟基磷灰石/壳聚糖(HA/CS)为对照,研究了庆大霉素对HA/CS复合材料抑菌性能、力学性能和降解性能等的影响。实验结果表明,HA/CS-G有良好的抑菌效果。负载庆大霉素后HA/CS的机械强度明显增强,而材料的降解速率有所下降。本文采用的二次成型技术显著增大了材料的机械强度。     

碳纳米管/壳聚糖复合微球的原位仿生矿化及表征

对碳纳米管(CNTs)进行酸化处理, 采用乳化交联法制备CNTs/壳聚糖(CS)复合微球, 在其表面诱导羟基磷灰石仿生合成, 研究了CNTs对复合微球仿生矿化的影响, 并与纯CS微球的仿生矿化进行了对比. 利用扫描电子显微镜(SEM)、 X射线衍射仪(XRD)、 溶胀率和含水率测试等考察了复合微球矿化前后的形貌特征、 物相结构及稳定性. 结果表明, 在相同时间下, CNTs/CS复合微球表面纳米羟基磷灰石的形成能力明显优于纯CS微球, 且形态稳定性更高. 细胞实验结果表明, 与MG63细胞共培养7 d时, 矿化复合微球细胞增殖明显.     

羟基磷灰石/聚乙烯醇/壳聚糖水凝胶在模拟体液中的力学性能

从仿生学角度出发,将自制的人工角膜支架材料羟基磷灰石/聚乙烯醇/壳聚糖(n-HA/PVA/CS)浸泡在模拟体液中,对材料的含水率及力学性能进行了测试,并利用扫描电镜、X射线衍射仪、电感耦合等离子体原子发射光谱仪及热重分析仪研究了材料在模拟体液中的形貌、晶体结构、元素组成及热稳定性.结果表明,在模拟体液中,n-HA/PVA/CS复合水凝胶的含水率为80%~86%,具有较高的拉伸强度,能承受正常眼压,且热稳定性较好.在浸泡后期,n-HA/CS/PVA复合材料对Ca2+的吸附和释放达到动态平衡;而其表面含有微量的纳米羟基磷灰石沉积,有利于纤维细胞的长入.     

钛基多孔HA/SiO2复合涂层的制备及性能研究

为了制得表面多孔且与基材结合强度高的羟基磷灰石(HA)涂层,实验中以正丁醇为分散介质,以SiO2粉末为添加剂,纯钛片为基材,电泳沉积制备羟基磷灰石/二氧化硅/壳聚糖/(HA/SiO2/CS)复合涂层,经后续热处理得到多孔HA/SiO2复合涂层,采用扫描电镜(SEM)、傅立叶红外光谱仪(FT-IR)、X射线衍射仪(XRD)、万能材料试验机对涂层的表面形貌、组成、结构和结合强度进行测试和表征,并通过模拟体液(SBF)浸泡法对复合涂层的生物活性进行评价.结果表明:当悬浮液中的HA/SiO2/CS质量比为1∶1∶1时,制得的HA/SiO2/CS涂层经700℃热处理后获得的HA/SiO2复合涂层孔洞分布均匀,大孔孔径在10～15μm,小孔孔径在1～5μm;涂层与基材的结合强度达到25.5 MPa;多孔HA/SiO2复合涂层在SBF中浸泡7 d后,涂层表面碳磷灰石化;说明实验中添加SiO2所制得的多孔HA/SiO2复合涂层与钛基材结合强度高,且具有良好的生物活性.     

温敏性壳聚糖共聚膜的制备与细胞吸附/脱附行为

将丙烯酸(AAc)与壳聚糖(CS)反应, 合成了壳聚糖大单体(CS-AAc), 再用CS-AAc与N-异丙基丙烯酰胺(NIPAAm)共聚, 制备P(CS-AAc-NIPAAm)共聚物. 通过红外光谱和X射线光电子能谱等分析证实了产物的结构和组成. 对P(CS-AAc-NIPAAm)共聚膜的动态接触角及对细胞的吸附与脱附行为研究发现, 共聚膜表现出良好的温度敏感性, 其表面成功地种植了成纤维细胞(L929). 当环境温度降低后, 共聚膜表面细胞自动脱附, 从而避免了使用酶解法脱附细胞造成的细胞功能损伤.     

多孔载药纳米羟基磷灰石/聚酰胺/壳聚糖复合材料的制备与性能

以纳米羟基磷灰石(n-HA)、聚酰胺(PA)、壳聚糖(CS)为原料,以聚乙烯吡咯烷酮(PVP)与氯化钠(Na Cl)为致孔剂采用溶液共混法和粒子致孔法,载入抗生素红霉素(EM),研制一种新型多孔载药纳米羟基磷灰石/聚酰胺/壳聚糖/红霉素复合骨组织修复材料。研究了其孔隙率、抗压强度、X射线衍射谱图、红外光谱图、SEM和药物释放曲线,探讨了CS含量及红霉素释放量对材料性能的影响。结果表明,当PVA/Na Cl为1:6时,材料总孔隙率为72%和抗压强度为0.71MPa,扫描电镜显示多孔n-HA/PA/CS复合材料孔的直径在100~500μm之间,适合血管、骨组织的长入以及营养物质的运输。当CS的含量从0增到30%时复合材料药物的释放量从41.6%增到82.4%,表明可降解材料CS的加入有利于药物溶出。     

脉冲电化学沉积法制备羟基磷灰石/壳聚糖复合涂层的研究

采用脉冲电化学沉积法在钛金属表面制备出羟基磷灰石/壳聚糖(HA/CS)复合涂层,实现CS与HA在微观尺寸上的复合与杂化.比较了脉冲电位与恒电位模式下复合涂层的形成,研究了电位高低及壳聚糖浓度对复合涂层性能的影响.结果表明,与恒电位模式比较,脉冲电位下制备的涂层较均匀、结晶性好、CS含量高,并且HA与CS杂化程度高.脉冲...     

三醋酸纤维素/壳聚糖反渗透膜的制备及性能研究

以壳聚糖(CS)为抗菌剂和三醋酸纤维素(CTA)为基膜材料,通过液-液共混和相转化成膜技术制备了三醋酸纤维素/壳聚糖共混反渗透膜(CTA/CS-RO),以改善醋酸纤维素反渗透膜的抗菌性能.采用傅里叶红外光谱、X-射线光电子能谱、扫描电子显微镜、水接触角、X-射线衍射光谱等对其结构和性能进行表征.结果表明,CTA/CS-RO中CS与CTA之间存在氢键作用,并且CS随着双扩散过程向膜表面迁移;膜厚度随着CS含量的递增而减小,横断面结构由指状孔转变成海绵状.CS的添加有利于共混膜亲水性、水通量和力学性能的提高.当CS含量为0.75%~1.00%时,膜样品在保持较高的盐截留率(R90%)的同时其断裂伸长率和结晶度没有显著变化.动态接触抗菌测试结果表明,CTA/CS-RO对大肠杆菌和金黄色葡萄球菌均具有抑菌作用.特别地,当CS含量为0.75%~1.00%时,膜样品对大肠杆菌和金黄色葡萄球菌的抑菌率分别为65%~72.5%和16%~51%.综合分析,CTA/CS共混反渗透膜制备过程中CS的加入量保持在0.75%~1.00%时膜的综合性能最优.     

聚醚醚酮复合材料表面生物活性涂层的制备与性能

以聚醚醚酮/钡玻璃粉(PEEK-BGF)复合材料为基体, 通过硅烷偶联剂, 在复合材料表面构建具有生物活性的纳米羟基磷灰石(nHA)和甲基丙烯酸酯基的光固化树脂复合涂层. 采用扫描电子显微镜(SEM)和X射线光电子能谱(XPS)分析了材料表面形貌和元素分布, 测试了涂层与复合材料之间的粘接强度. 通过检测大鼠成骨细胞总蛋白含量和碱性磷酸酶表达水平, 评价新型光固化纳米羟基磷灰石/聚甲基丙烯酸酯(nHA/PMMA)复合涂层的生物活性. 研究结果表明, nHA填充的光固化复合材料形成粗糙的表面, 随着nHA的填充量提高, 涂层表面生物学活性得到提高.     

Effect of molecular weight on the exponential growth and morphology of hyaluronan/chitosan multilayers: a surface plasmon resonance spectroscopy and atomic force microscopy investigation

The layer-by-layer growth of multilayer assemblies of two polysaccharides, the polyanion hyaluronan (HA) and the polycation chitosan (CH), was investigated using atomic force microscopy (AFM) and surface plasmon resonance (SPR) spectroscopy, with primary emphasis on the effect of the polysaccharide molecular weights on the film thickness and surface morphology. The HA/CH multilayers exhibit an exponential increase of the optical film thickness with the number of deposited bilayers. We show that the multilayer thickness at a given stage depends on the size of both CH, the diffusing polyelectrolyte, and HA, the non-diffusing species. Assemblies (12 bilayers) of high molecular weight polysaccharides (HA, 360,000; CH, 160,000) were twice as thick (approximately 900 nm vs approximately 450 nm) as those obtained with low molecular weight polymers (HA, 30,000; CH, 31,000), as assessed by AFM scratch tests. The exponential growth rate is the same for the high and low molecular weight pairs; the larger film thicknesses observed by SPR and by AFM arising from an earlier onset of the steep exponential growth phase in the case of the high molecular weight pair. In all cases, isolated islets form during the deposition of the first CH layer onto the underlying HA. Upon further film growth, individual islets coalesce into larger vermiculate features. The transition from distinct islands to vermiculate structures depends on the molecular weights of the polysaccharides and the lower molecular weight construct presents larger worm-like surface domains than the high molecular weight pair.     

Polysaccharide films built by simultaneous or alternate spray: a rapid way to engineer biomaterial surfaces

We investigated polysaccharide films obtained by simultaneous and alternate spraying of a chitosan (CHI) solution as polycation and hyaluronic acid (HA), alginate (ALG), and chondroitin sulfate (CS) solutions as polyanions. For simultaneous spraying, the film thickness increases linearly with the cumulative spraying time and passes through a maximum for polyanion/CHI molar charge ratios lying between 0.6 and 1.2. The size of polyanion/CHI complexes formed in solution was compared with the simultaneously sprayed film growth rate as a function of the polyanion/CHI molar charge ratio. A good correlation was found. This suggests the importance of polyanion/polycation complexation in the simultaneous spraying process. Depending on the system, the film topography is either liquid-like or granular. Film biocompatibility was evaluated using human gingival fibroblasts. A small or no difference is observed in cell viability and adhesion between the two deposition processes. The CHI/HA system appears to be the best for cell adhesion inducing the clustering of CD44, a cell surface HA receptor, at the membrane of cells. Simultaneous or alternate spraying of CHI/HA appears thus to be a convenient and fast procedure for biomaterial surface modifications.     

Chitosan adsorption on hydroxyapatite and its role in preventing acid erosion

Polymer adsorption onto an artificial saliva (AS) layer is investigated using quartz-crystal microbalance with dissipation (QCM-D) and chitosan as the model polymer. QCM-D is utilized in an innovative manner to monitor in situ adsorption of chitosan (CH) onto a hydroxyapatite (HA) coated crystal and to examine the ability of the adsorbed layer to "protect" the HA upon sequential exposure to acidic solutions. After deposition of a thin AS layer (16nm), the total thickness on the HA substrate increases to 37nm upon exposure to CH at pH 5.5 for 10min. Correspondingly, the surface charge changes from negative (i.e., AS) to positive, consistent with the adsorption the polycationic CH onto or into the AS layer. Upon exposure to an oxidizing agent, the chitosan cross-links and collapses as noted by a decrease in thickness to 10nm and an increase in the shear modulus by an order of magnitude. Atomic force microscopy (AFM) is used to determine the surface morphology and RMS roughness of the coated and HA surfaces after citric acid challenges. Both physisorbed and cross-linked chitosan are demonstrated to limit and prevent the erosion of HA, respectively.     

Layer by layer buildup of polysaccharide films: physical chemistry and cellular adhesion aspects

The formation ofpolysaccharide films based on the alternate deposition of chitosan (CHI) and hyaluronan (HA) was investigated by several techniques. The multilayer buildup takes place in two stages: during the first stage, the surface is covered by isolated islets that grow and coalesce as the construction goes on. After several deposition steps, a continuous film is formed and the second stage of the buildup process takes place. The whole process is characterized by an exponential increase of the mass and thickness of the film with the number of deposition steps. This exponential growth mechanism is related to the ability of the polycation to diffuse "in" and "out" of the whole film at each deposition step. Using confocal laser microscopy and fluorescently labeled CHI, we show that such a diffusion behavior, already observed with poly(L-lysine) as a polycation, is also found with CHI, a polycation presenting a large persistence length. We also analyze the effect of the molecular weight (MW) of the diffusing polyelectrolyte (CHI) on the buildup process and observe a faster growth for low MW chitosan. The influence of the salt concentration during buildup is also investigated. Whereas the CHI/HA films grow rapidly at high salt concentration (0.15 M NaCl) with the formation of a uniform film after only a few deposition steps, it is very difficult to build the film at 10(-4) M NaCl. In this latter case, the deposited mass increases linearly with the number of deposition steps and the first deposition stage, where the surface is covered by islets, lasts at least up to 50 bilayer deposition steps. However, even at these low salt concentrations and in the islet configuration, CHI chains seem to diffuse in and out of the CHI/HA complexes. The linear mass increase of the film with the number of deposition steps despite the CHI diffusion is explained by a partial redissolution of the CHI/HA complexes forming the film during different steps of the buildup process. Finally, the uniform films built at high salt concentrations were also found to be chondrocyte resistant and, more interestingly, bacterial resistant. Therefore, the (CHI/HA) films may be used as an antimicrobial coating.     

Novel Method to Graft Chitosan on the Surface of Hydroxyapatite Nanoparticles via ＂Click＂ Reaction

In order to tune the surface properties of hydroxyapatite（HA） nanoparticles and prevent them from ag- gregation, an efficient method was proposed to graft chitosan（CS） molecules on the surface of HA via ＂click＂ reac- tion. Thermal gravimetric analysis（TGA） shows that CS was successfully grafted on the surface of HA nanoparticles and the grafting amount was about 8.9 g of CS on per hundred grams of HA. The grafted chitosan chains can prevent HA nanoparticles from aggregation and greatly enhance the colloidal stability of HA in water. The 3-（4,5-dimethylthiazoyl-2-yl）-2,5-diphenyltetrazolium bromide（MTT） assay demonstrats that the cytotoxicity of CS modified HA（HA-CS） is negligible and thus HA-CS may find potential application in biomedical fields.     

Interaction between myoglobin and hyaluronic acid in their layer-by-layer assembly: quartz crystal microbalance and cyclic voltammetry studies

Myoglobin (Mb), with different net surface charges at different pH in buffers and negatively charged hyaluronic acid (HA) at pH 5.0 in solutions were alternately adsorbed onto various solid surfaces and successfully assembled into {Mb/HA}(n) layer-by-layer films. The Mb in {Mb/HA}(n) films showed a quasi-reversible cyclic voltammetry (CV) response for its heme Fe(III)/Fe(II) redox couple. Quartz crystal microbalance (QCM) and CV were used to confirm the film growth and characterize the films. The interaction between Mb and HA and the influencing factors for Mb adsorption on HA surface, such as pH, Mb concentration, and ionic strength, were investigated in detail. The assembly driving force for {Mb/HA}(n) films, especially for the films assembled with like-charged Mb and HA, was found to be of electrostatic origin, while the secondary interaction such as hydrophobic interaction also plays an important role in some circumstances. Although the growth of {Mb(pH 7.0)/HA}(n) and {Mb(pH 9.0)/HA}(n) films was linear with the adsorption step, the exponential growth of {Mb(pH 5.0)/HA}(n) films was observed, especially when the films became thick. This exponential increase of mass and thickness with deposition step for {Mb(pH 5.0)/HA}(n) films was most probably attributed to the diffusion mechanism in which some HA molecules could diffuse in to and out of the whole films during the film assembly. Atomic force microscopy (AFM) results supported this speculation. UV-vis and IR spectroscopies of {Mb/HA}(n) films, combined with the comparative CV experiments of {Mb/HA}(n) and {catalase/HA}(n) films, suggest that Mb in the {Mb/HA}(n) multilayer films retains its near-native structure.     

Preparation and Characterization of Chitosan-Coated DBD Plasma-Treated Natural Rubber Latex Medical Surgical Gloves with Antibacterial Activities

The natural rubber latex (NRL) film taken from medical surgical gloves was surface-modified with a dielectric barrier discharge (DBD) plasma treatment under an air environment. The results showed that surface hydrophilicity of the NRL film increased after the plasma treatment due to the presence of oxygen-containing polar groups on the plasma-treated surface. An increase in plasma treatment time increased the surface roughness of the NRL film, and eventually decreased the mechanical properties. From the obtained results, the optimum plasma treatment time of 20?s was chosen. After immersion in a chitosan solution, the amount of chitosan deposited on the plasma-treated NRL film increased with increasing chitosan concentrations. The chitosan coating smoothed the surface of the plasma-treated NRL film and also improved the mechanical properties. The highest antibacterial activities of the chitosan-coated DBD plasma-treated NRL film against both Staphylococcus aureus and Escherichia coli were achieved when a 2?%(w/v) chitosan solution was used for the coating.     

Loading behavior of {chitosan/hyaluronic acid}n layer-by-layer assembly films toward myoglobin: an electrochemical study

When {CS/HA}n layer-by-layer films assembled by oppositely charged chitosan (CS) and hyaluronic acid (HA) were immersed in myoglobin (Mb) solution at pH 5.0, Mb was gradually loaded into the {CS/HA}n films, designated as {CS/HA}n-Mb. The cyclic voltammetric (CV) peak pair of Mb FeIII/FeII redox couple for {CS/HA}n-Mb films on pyrolytic graphite (PG) electrodes was used to investigate the loading behavior of {CS/HA}n films toward Mb. The various influencing factors, such as the number of bilayers (n), the pH of Mb loading solution, and the ionic strength of solution, were investigated by different electrochemical methods and other techniques. The results showed that the main driving force for the bulk loading of Mb was most probably the electrostatic interaction between oppositely charged Mb in solution and HA in the films, while other interactions such as hydrogen bonding and hydrophobic interaction may also play an important role. Other polyelectrolyte multilayer (PEM) films with different components were compared with {CS/HA}n films in permeability and Mb loading, and electroactive probes with different size and surface charge were compared in their incorporation into PEM films. The results suggest that due to the unique structure of CS and HA, {CS/HA}n films with relatively low charge density are packed more loosely and more easily swelled by water, and have better permeability, which may lead to the higher loading amount and shorter loading time for Mb. The protein-loaded PEM films provide a new route to immobilize redox proteins on electrodes and realize the direct electrochemistry of the proteins.     

Cell outer membrane mimetic modification of a cross-linked chitosan surface to improve its hemocompatibility

A novel strategy has been developed to improve the hemocompatibility of chitosan surface by cell outer membrane mimetic structure able to reduce protein adsorption and cell adhesion. Phosphorylcholine dichloride was synthesized and grafted onto a glutaraldehyde-cross-linked chitosan (CS-GA) film surface to prepare phosphorylcholine-coated CS-GA film (CS-GA-PC) through a heterogeneous reaction process. The spectroscopic and contact angle characterization show that a cell outer membrane mimetic structure was formed on the cross-linked chitosan surface, and the significantly improved hemocompatibility of the modified surface was shown by a suppression of 94% on platelet adhesion, a suppression of 60–70% for bovine plasma fibrinogen and bovine serum albumin adsorptions. These results demonstrated that this cell outer membrane mimetic surface modification with phosphorylcholine dichloride is a promising strategy to improve the hemocompatibility of chitosan.     

The Influence of Polysaccharides/TiO2 on the Model Membranes of Dipalmitoylphosphatidylglycerol and Bacterial Lipids

The aim of the study was to determine the bactericidal properties of popular medical, pharmaceutical, and cosmetic ingredients, namely chitosan (Ch), hyaluronic acid (HA), and titanium dioxide (TiO₂). The characteristics presented in this paper are based on the Langmuir monolayer studies of the model biological membranes formed on subphases with these compounds or their mixtures. To prepare the Langmuir film, 1,2-dipalmitoyl-sn-glycero-3-phospho-rac-(1-glycerol) (DPPG) phospholipid, which is the component of most bacterial membranes, as well as biological material-lipids isolated from bacteria Escherichia coli and Staphylococcus aureus were used. The analysis of the surface pressure-mean molecular area (π-A) isotherms, compression modulus as a function of surface pressure, C_S⁻¹ = f(π), relative surface pressure as a function of time, π/π₀ = f(t), hysteresis loops, as well as structure visualized using a Brewster angle microscope (BAM) shows clearly that Ch, HA, and TiO₂ have antibacterial properties. Ch and TiO₂ mostly affect S. aureus monolayer structure during compression. They can enhance the permeability of biological membranes leading to the bacteria cell death. In turn, HA has a greater impact on the thickness of E. coli film.