表面分子印迹磁性纳米粒子的制备及其血红蛋白传感应用

以Fe₃O₄磁性纳米粒子为载体、多巴胺（DA）为功能单体、血红蛋白（Hb）为模板分子,用氯铂酸氧化DA生成聚多巴胺（PDA）,同时氯铂酸还原为铂纳米粒子（PtNPs）,与Hb一起负载于Fe₃O₄纳米粒子表面,洗脱Hb后合成了表面分子印迹磁性纳米粒子（印迹Fe₃O₄/PDA-PtNPs）. 将印迹Fe₃O₄/PDA-PtNPs修饰于磁性玻碳基底表面,制得印迹Fe₃O₄/PDA-PtNPs修饰电极. 实验结果表明,印迹Fe₃O₄/PDA-PtNPs具有良好的水溶性,粒径分布均匀,生成的PtNPs具有良好的导电性和刚性. 用印迹Fe₃O₄/PDA-PtNPs构建的传感器对Hb具有良好的识别性,在0.14 ~ 2.7 μg·mL^-1 Hb浓度范围与交流阻抗变化值呈良好的线性关系,检出限（S/N=3）为0.05 μg·mL^-1.     

An in vitro Study on Transition from NO-Hemoglobin to Methemoglobin： Oxygen Effect

The nitrosyl-hemoglobin (HbNO) is the carrier of nitric oxide (NO) which is the important messenger molecule displaying multiple physiologic and pathophysiologic roles. However it is still not clear for the fate of HbNO molecules during the venous-arterial transit. In this letter, the HbNO transition in vitro was studied by using the electron paramagnetic resonance (EPR) spectra. It was found that HbNO molecules were stable when oxygen did not exist in the system but not stable in aerobic conditions. The absorption spectra further revealed that the methemoglobin (metHb) was the product of HbNO in aerobic environment, showing that the HbNO changed to metHb when there were enough oxygen molecules in the system.     

Comb‐Like Amphiphilic Polycarbonates with Different Lengths of Cationic Branches for Enhanced siRNA Delivery

Owing to the biodegradability and good biocompatibility polycarbonates show the versatile class of applications in biomedical fields. While their poor functional ability seriously limited the development of functional polycarbonates. Herein, a new Br‐containing cyclic carbonate (MTC‐Br) and a polycarbonate atom transfer radical polymerization (ATRP) macro‐initiator (PEG‐PMTC‐Br) is synthesized. Then, by initiating the side‐chain ATRP of 2‐(dimethyl amino)ethyl methacrylate (DMAEMA) on PEG‐PMTC‐Br, a series of comb‐like amphiphilic cationic polycarbonates, PEG‐b‐(PMTC‐g‐PDMAEMA) (GMDMs), with different lengths of cationic branches are successfully prepared. All these poly(ethylene glycol)‐b‐(poly((5‐methyl‐2‐oxo‐1,3‐dioxane‐5‐yl) methyl 2‐bromo‐2‐methylpropanoate/1,3‐dioxane‐2‐one)‐g‐poly(2‐dimethyl aminoethyl methacrylate) (GMDMs) self‐assembled nanoparticles (NPs) (≈180 nm, +40 mV) can well bind siRNA to form GMDM/siRNA NPs. The gene silence efficiency of GMDM/siRNA high to 80%, which is even higher than the commercial transfection reagent lipo2000 (76%). But GMDM/siRNA shows lower cell uptake than lipo2000. So, the high gene silence ability of GMDM/siRNA NPs can be attributed to the strong intracellular siRNA trafficking capacity. Therefore, GMDM NPs are potential siRNA vectors and the successful preparation of comb‐like polycarbonates also provides a facile way for diverse side‐chain functional polycarbonates, expanding the application of polycarbonates.     

Hyperbranched copolymer micelles as delivery vehicles of doxorubicin in breast cancer cells

Four types of drug nanoparticles (NPs) based on amphiphilic hyperbranched block copolymers were developed for the delivery of the chemotherapeutic doxorubicin (DOX) to breast cancer cells. These carriers have their hydrophobic interior layer composed of the hyperbranched aliphatic polyester, Boltorn^® H30 or Boltorn^® H40, that are polymers of poly 2,2‐bis (methylol) propionic acid (bis‐MPA), while the outer hydrophilic shell was composed of about 5 poly(ethylene glycol) (PEG) segments of 5 or 10 kDa molecular weight. A chemotherapeutic drug DOX, was further encapsulated in the interior of these polymer micelles and was shown to exhibit a controlled release profile. Dynamic light scattering and transmission electron microscopy analysis confirmed that the NPs were uniformly sized with a mean hydrodynamic diameter around 110 nm. DOX‐loaded H30‐PEG10k NPs exhibited controlled release over longer periods of time and greater cytotoxicity compared with the other materials developed against our tested breast cancer cell lines. Additionally, flow cytometry and confocal scanning laser microscopy studies indicated that the cancer cells could internalize the DOX‐loaded H30‐PEG10k NPs, which contributed to the sustained drug release, and induced more apoptosis than free DOX did. These findings indicate that the H30‐PEG10k NPs may offer a very promising approach for delivering drugs to cancer cells. © 2011 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2012     

Self-suspended Pure Polydiacetylene Nanoparticles with Selective Response to Lysine and Arginine

We demonstrate a very convenient access to self-suspended pure poly(10,12-pentacosadiynoic acid) (PDA) nanoparticles (NPs) simply by adding the ethanol solution of diacetylene monomer to water, followed by UV irradiation. The as-obtained PDA NPs are of high purity because no any initiator, catalyst or stabilizer was used during the whole process. The stabilizer-free PDA NPs are stable in the aqueous suspension. Due to the high purity and stability, the PDA NPs can respond sensitively and selectively to lysine and arginine among 18 kinds of water soluble natural amino acids; without the competitive interaction from the stabilizer, the sensitivity was enhanced.     

Poly(ethylene glycol)/poly(ethyl cyanoacrylate) amphiphilic triblock copolymer nanoparticles as delivery vehicles for dexamethasone

Amphiphilic triblock copolymers, poly(ethyl cyanoacrylate)‐b‐poly(ethylene glycol)‐b‐poly(ethyl cyanoacrylate) (PECA‐b‐PEG‐b‐PECA), were synthesized via oxyanion‐initiated polymerization with sodium alcoholate‐terminated PEG as macroinitiator. PECA‐b‐PEG‐b‐PECA were characterized by gel permeation chromatography system, ¹H NMR and FTIR. The results indicate that the copolymerization is well controlled with narrow molecular weight distribution. The dexamethasone (DXM)‐loaded PECA‐b‐PEG‐b‐PECA nanoparticles (NPs) were prepared by nanoprecipitation technique and then characterized by Laser Particle Size Analyzer, ¹H NMR and transmission electron microscopy. The drug‐loaded PECA‐b‐PEG‐b‐PECA NPs are of spherical shape with average size of less than 100 nm. The drug‐loaded amount (DLA) and encapsulation efficiency of DLNPs were investigated by HPLC. The results show that DXM can be effectively incorporated into PECA‐b‐PEG‐b‐PECA NPs, which provides an optional delivery system for DXM and other hydrophobic drugs. © 2008 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 46: 7809–7815, 2008     

Mitigation of Inflammatory Immune Responses with Hydrophilic Nanoparticles

While hydrophobic nanoparticles (NPs) have been long recognized to boost the immune activation, whether hydrophilic NPs modulate an immune system challenged by immune stimulators and how their hydrophilic properties may affect the immune response is still unclear. To answer this question, three polymers, poly(ethylene glycol) (PEG), poly(sulfobetaine) (PSB) and poly(carboxybetaine) (PCB), which are commonly considered hydrophilic, are studied in this work. For comparison, nanogels with uniform size and homogeneous surface functionalities were made from these polymers. Peripheral blood mononuclear cells (PBMCs) stimulated by lipopolysaccharide (LPS) and an LPS‐induced lung inflammation murine model were used to investigate the influence of nanogels on the immune system. Results show that the treatment of hydrophilic nanogels attenuated the immune responses elicited by LPS both in vitro and in vivo. Moreover, we found that PCB nanogels, which have the strongest hydration and the lowest non‐specific protein binding, manifested the best performance in alleviating the immune activation, followed by PSB and PEG nanogels. This reveals that the immunomodulatory effect of hydrophilic materials is closely related to their hydration characteristics and their ability to resist non‐specific binding in complex media.     

Target‐Specific Capture of Environmentally Relevant Gaseous Aldehydes and Carboxylic Acids with Functional Nanoparticles

Aldehyde and carboxylic acid volatile organic compounds (VOCs) present significant environmental concern due to their prevalence in the atmosphere. We developed biodegradable functional nanoparticles comprised of poly(d,l ‐lactic acid)‐poly(ethylene glycol)‐poly(ethyleneimine) (PDLLA‐PEG‐PEI) block co‐polymers that capture these VOCs by chemical reaction. Polymeric nanoparticles (NPs) preparation involved nanoprecipitation and surface functionalization with branched PEI. The PDLLA‐PEG‐PEI NPs were characterized by using TGA, IR, ¹H NMR, elemental analysis, and TEM. The materials feature 1°, 2°, and 3° amines on their surface, capable of capturing aldehydes and carboxylic acids from gaseous mixtures. Aldehydes were captured by a condensation reaction forming imines, whereas carboxylic acids were captured by acid/base reaction. These materials reacted selectively with target contaminants obviating off‐target binding when challenged by other VOCs with orthogonal reactivity. The NPs outperformed conventional activated carbon sorbents.     

低氧亲和力血红蛋白类氧载体的制备及大鼠动脉血压响应

氧亲和力是血红蛋白氧载体非常重要的参数之一,但其高低还没有统一的认识,有一种理论认为低氧亲和力是造成高血压的原因。为了进一步研究氧亲和力与血压之间的关系,本文制备了两种低氧亲和力的血红蛋白氧载体。用高碘酸钠氧化棉子糖（高碘酸钠：棉籽糖=6：1,摩尔比）,得到氧化均一的开环棉子糖;以其作为交联剂聚合脱氧猪血红蛋白,在聚合1 h得到了低氧亲和力（P50 = 43.1 torr）主要为分子内交联的64 kDa的血红蛋白,在聚合2 4 h得到了低氧亲和力（P50 = 51.5 torr）平均分子量为600 kDa的聚合血红蛋白;分别进行大鼠50%等容量换血实验,前者显著引起血压升高而后者血压平稳,证实高血压主要和64 kDa血红蛋白有关,低氧亲和力不是造成高血压的主要原因。     

Nanoparticle Capping Agent Controlled Electron‐Transfer Dynamics in Ionic Liquids

Herein, we report a change in the mechanism of the oxidation of silver nanoparticles (Ag NPs) with the molecular weight of a poly(ethylene) glycol (PEG) capping agent. Characterisation of the modified nanoparticles is undertaken using dynamic light scattering and UV/Vis spectroscopy. Electrochemical analyses reveal that the oxidation of 6000 molecular weight (MW) PEG is consistent with a polymer‐gated mechanism, whilst for 2000 MW PEG the polymer does not hinder the oxidation. The 10,000 MW PEG Ag NPs are rendered almost electrochemically inactive. This study demonstrates the ability to alter and better understand the electron‐transfer mechanism in a room temperature ionic liquid (RTIL) by systematically altering the capping agent.     

Purification and identification of PEGlated hemoglobin, a potential blood substitute, by chromatography and capillary electrophoresis

Summary Bovine hemoglobin (Hb) has been chemically modified, by reaction of its lysine residues with the active ester of poly(ethylene glycol) (PEG,M _w=5000), to produce a potential blood substitute for human therapy. Covalent attachment of PEG chain to the protein produced a heterogeneous mixture of Hb from the mixture. This paper describes the use of cation-exchange chromatography (IEC), in flow-through mode, and size-exclusion chromatography (SEC) for purification of the PEG-Hb mixture. The highly modified Hb flowed through the IEC column in the loading buffer without adsorption by the chromatographic medium. SEC was then used for further purification. These two steps were suitable for pilot-scale preparation or for analytical chromatography. The purified product was assessed by high-performance capillary electrophoresis (HPCE), which was also used to optimize the chromatographic parameters.     

Tailored Synthesis of Octopus‐type Janus Nanoparticles for Synergistic Actively‐Targeted and Chemo‐Photothermal Therapy

A facile, reproducible, and scalable method was explored to construct uniform Au@poly(acrylic acid) (PAA) Janus nanoparticles (JNPs). The as‐prepared JNPs were used as templates to preferentially grow a mesoporous silica (mSiO₂) shell and Au branches separately modified with methoxy‐poly(ethylene glycol)‐thiol (PEG) to improve their stability, and lactobionic acid (LA) for tumor‐specific targeting. The obtained octopus‐type PEG‐Au‐PAA/mSiO₂‐LA Janus NPs (PEG‐OJNP‐LA) possess pH and NIR dual‐responsive release properties. Moreover, DOX‐loaded PEG‐OJNP‐LA, upon 808 nm NIR light irradiation, exhibit obviously higher toxicity at the cellular and animal levels compared with chemotherapy or photothermal therapy alone, indicating the PEG‐OJNP‐LA could be utilized as a multifunctional nanoplatform for in vitro and in vivo actively‐targeted and chemo‐photothermal cancer therapy.     

Structure‐Based Rational Design of Prodrugs To Enable Their Combination with Polymeric Nanoparticle Delivery Platforms for Enhanced Antitumor Efficacy

Drug‐loaded nanoparticles (NPs) are of particular interest for efficient cancer therapy due to their improved drug delivery and therapeutic index in various types of cancer. However, the encapsulation of many chemotherapeutics into delivery NPs is often hampered by their unfavorable physicochemical properties. Here, we employed a drug reform strategy to construct a small library of SN‐38 (7‐ethyl‐10‐hydroxycamptothecin)‐derived prodrugs, in which the phenolate group was modified with a variety of hydrophobic moieties. This esterification fine‐tuned the polarity of the SN‐38 molecule and enhanced the lipophilicity of the formed prodrugs, thereby inducing their self‐assembly into biodegradable poly(ethylene glycol)‐block‐poly(d,l ‐lactic acid) (PEG‐PLA) nanoparticulate structures. Our strategy combining the rational engineering of prodrugs with the pre‐eminent features of conventionally used polymeric materials should open new avenues for designing more potent drug delivery systems as a therapeutic modality.     

新型耐甲醇氧还原电催化剂——氮掺杂中空碳微球@铂纳米粒子复合材料

通过模板法制备了一种新型耐甲醇氧还原电催化剂——氮掺杂中空碳微球@铂纳米粒子复合材料(HNCMS@PtNPs)。首先,将铂纳米粒子负载于氨基化二氧化硅微球上,获得PtNPs/SiO₂复合材料。然后通过多巴胺自聚合反应在PtNPs/SiO₂复合材料上包裹聚多巴胺(PDA)膜,将其在氮气气氛中直接进行碳化处理并通过氢氟酸溶液刻蚀去除SiO₂,获得了内嵌有PtNPs的氮掺杂中空碳微球,标记为HNCMS@PtNPs复合材料。采用扫描电子显微镜、透射电子显微镜、X射线衍射仪、拉曼光谱仪、比表面积分析仪和X射线光电子能谱仪对HNCMS@PtNPs复合材料的形貌和结构进行了表征。采用循环伏安法和线性扫描伏安法研究了HNCMS@PtNPs复合材料的电催化氧还原性能。结果表明：HNCMS@PtNPs催化剂的Pt载量高达11.9%(w,质量分数),对氧还原反应具有高电催化活性、高稳定性和优良的抗甲醇性能,是一种具有应用潜力的直接甲醇燃料电池(DMFCs)阴极电催化剂。     

In vitro macrophage uptake and in vivo biodistribution of long-circulation nanoparticles with poly(ethylene-glycol)-modified PLA (BAB type) triblock copolymer

The effect of the PEG-grafted degree in the range of 0–30% on the in vitro macrophage uptake and in vivo biodistribution of poly(ethylene glycol)–poly(lactic acid)–poly(ethylene glycol) (PELE) nanoparticles (NPs) were investigated in this paper. The prepared NPs were characterized in terms of size, zeta potential, hydrophilicity, poly(vinyl alcohol) (PVA) residual on nanoparticles surfaces as well as drug loading. The macrophage uptake and biodistribution including plasma clearance kinetics following intravenous administration in mice of the NPs labeled by 6-coumarin were evaluated. The results showed that, except for the particles size, the hydrophilicity, superficial charges and in vitro phagocytosis amount of NPs are dependent on the PEG content in the copolymers greatly. The higher of the PEG content, the more hydrophilicity and the nearer to neutral surface charge was observed. And the prolonged circulation half-life (t_1/2) of the PELE NPs in plasma was also strongly depended on the PEG content with the similar trend. In particular for PELE30 (containing 30% of PEG content) NPs, with the lowest phagocytosis uptake accompanied the highest hydrophilicity and approximately neutral charge, it had the longest half-life in vivo with almost 12-fold longer and accumulation in the reticuloendothelial system organs close to 1/2-fold lower than those of reference PLA. These results demonstrated that the PELE30 NPs with neutral charge and suitable size has a promising potential as a long-circulating oxygen carrier system with desirable biocompatibility and biofunctionality.     

Direct electrochemistry and electrocatalysis of hemoglobin in a multilayer {nanogold/PDDA}n inorganic–organic hybrid film

A new amperometric biosensor for hydrogen peroxide (H₂O₂) has been developed that is based on direct electrochemistry and electrocatalysis of hemoglobin (Hb) in a multilayer inorganic–organic hybrid film. o-Phenylenediamine (PDA) was electropolymerized onto a glassy carbon electrode (GCE), and then negatively charged nanogold particles and positively charged poly(diallyldimethylammonium chloride) (PDDA) were alternately assembled on the PDA/GCE surface. Finally, Hb was electrostatically adsorbed on the surface of gold nanoparticles. The electrochemical behavior of the resulting biosensor (Hb/{nanogold/PDDA}_n/PDA/GCE) was assessed and optimized. The performance and factors influencing the biosensor were studied in detail. Under optimal conditions, the immobilized Hb displayed good electrocatalytic response to the H₂O₂ reduction ranging from 1.3 μM to 1.4 mM with a detection limit of 0.8 μM (at 3δ). In addition, the biosensor exhibited rapid response, good reproducibility, and long-term stability. Electronic supplementary material to this paper is available in electronic form at Correspondence: Dianyong Tang, Department of Chemistry and Life Science, Leshan Teachers College, Sichuan (Leshan) 614000, P.R. China     

Solvent selection for matrix‐assisted laser desorption/ionization time‐of‐flight mass spectrometric analysis of synthetic polymers employing solubility parameters

The principle relating to the selection of a proper matrix, cationization reagent, and solvent for matrix‐assisted laser desorption/ionization time‐of‐flight mass spectrometry (MALDI‐TOF MS) of synthetic polymers is still a topic of research. In this work we focused on the selection of a suitable MALDI solvent. Polystyrene PS7600 and poly(ethylene glycol) PEG4820 were analyzed by MALDI‐TOF MS using various solvents which were selected based on the Hansen solubility parameter system. For polystyrene (PS), dithranol was used as the matrix and silver trifluoroacetate as the cationization reagent whereas, for poly(ethylene glycol) (PEG), the combination of 2,5‐dihydroxybenzoic acid and sodium trifluoroacetate was used for all experiments. When employing solvents which dissolve PS and PEG, reliable MALDI mass spectra were obtained while samples in non‐solvents (solvents which are not able to dissolve the polymer) failed to provide spectra. It seems that the solubility of the matrix and the cationization reagent are less important than the polymer solubility. Copyright © 2010 John Wiley & Sons, Ltd.     

Preparation of poly(ethylene glycol)-modified poly(amido amine) dendrimers encapsulating gold nanoparticles and their heat-generating ability

Loading of HAuCl4 in poly(amido amine) G4 dendrimers having poly(ethylene glycol) (PEG) grafts at all chain ends and subsequent reduction with NaBH4 yielded PEG-modified dendrimers encapsulating gold nanoparticles (Au NPs) of ca. 2 nm diameter. The Au NPs held in the dendrimers were stable in aqueous solutions and dissolved readily, even after freeze-drying. Despite their small particle size, the heat-generating ability of Au NPs held in the dendrimer was comparable to that of widely used Au NPs with ca. 11 nm diameter under visible light irradiation. The observed excellent colloidal stability, high heat-generating ability and their biocompatible surface confirm that the PEG-modified dendrimers encapsulating Au NPs are a promising tool for photothermal therapy and imaging.     

磁性印迹纳米粒子固定血红蛋白修饰磁性电极构建过氧化氢传感器

采用表面印迹技术,以磁性二氧化硅纳米粒子（Fe₃O₄@SiO₂ NPs）作为载体、血红蛋白（Hb）为模板分子、正硅酸乙酯（TEOS）为印迹聚合物单体,制备了Hb印迹Fe₃O₄@SiO₂的磁性印迹纳米粒子（MMIPs NPs）. MMIPs NPs具有磁性内核和血红蛋白印迹壳层的核壳结构,可以富集并固定Hb. 使用壳聚糖将MMIPs NPs固定于磁性电极表面,构建血红蛋白类酶生物传感器,研究了Hb对过氧化氢（H₂O₂）的催化活性. MMIPS NPS相比于磁性非印迹纳米粒子（MNIPS NPS）,催化电流增加了14.3%. 采用磁性电极,MMIPS NPS、Hb和O₂的顺磁性使得该类酶生物传感器对H₂O₂的催化电流增加了60.0%. 血红蛋白类酶生物传感器电流响应与H₂O₂浓度在25 ~ 200 μmol·L^-1间呈线性关系,检出限为3 μmol·L^-1（S/N=3）,表明该类酶传感器对H₂O₂具有良好的催化性能.     

Ultrastable and Highly Catalytically Active N‐Heterocyclic‐Carbene‐Stabilized Gold Nanoparticles in Confined Spaces

Controlling the size and surface functionalization of nanoparticles (NPs) can lead to improved properties and applicability. Herein, we demonstrate the efficiency of the metal‐carbene template approach (MCTA) to synthesize highly robust and soluble three‐dimensional polyimidazolium cages (PICs) of different sizes, each bearing numerous imidazolium groups, and use these as templates to synthesize and stabilize catalytically active, cavity‐hosted, dispersed poly‐N‐heterocyclic carbene (NHC)‐anchored gold NPs. Owing to the stabilization of the NHC ligands and the effective confinement of the cage cavities, the as‐prepared poly‐NHC‐shell‐encapsulated AuNPs displayed promising stability towards heat, pH, and chemical regents. Most notably, all the Au@PCCs (PCC=polycarbene cage) exhibited excellent catalytic activities in various chemical reactions, together with high stability and durability.