基于炔烃参与的多组分聚合构建氧化还原双重响应型高分子药物载体

为了拓展多组分聚合方法在药物载体领域应用,基于铜催化的炔烃多组分聚合设计合成含有二硒键的氧化还原响应型两亲性聚合物,与阿霉素(DOX)在水溶液中通过自组装方式构建纳米载药胶束.通过实验技术手段对纳米载药胶束表征可知,纳米载药胶束的粒径在130 nm左右,临界胶束浓度(CMC)值为0.23 mg/mL,在人体正常生理条件下结构稳定.肿瘤中含有浓度较高的活性氧(ROS)或谷胱甘肽(GSH),聚合物主链中二硒键在氧化还原条件下断裂,导致聚合物降解,DOX从纳米载药胶束中逐渐释放,且累积释放量可达100%,并发现该类载药胶束在GSH环境中药物释放性能优于ROS环境.该工作通过多组分聚合方式可以便捷构建氧化还原双重响应型的两亲性聚合物,在肿瘤微环境中表现出特异的降解性能,为开发设计智能响应型高分子药物载体提供新的思路.     

载体化络合催化开环歧化聚合合成梳形接枝共聚物研究

由环戊二烯（CPD）及烯丙基氯（AC）经聚合物支载三氟化硼催化的Diels-Alder反应合成了5-氯甲基-2-降冰片烯（NB-CH2Cl),锂代后用以引发甲基丙烯酸甲酯（MMA）及苯乙烯（S）的活性阴离子聚合,合成了带聚合物取代基的降冰片烯大分子单体NB-PMMA及NB-PS。在聚合物支载钌卡宾络合物催化作用下进行所合成大分子单体的开环歧化聚合反应（ROMP）,合成了二种接枝于开环歧化聚降冰片烯（PNB）主链的梳形接技共聚物PNB-g-PMMA及PNB-g-PS。实验结果表明所研制聚合物支载硼、钌络合物催化性能明显优于对应非支载活性种。     

双亲水性超支化接枝共聚物的pH响应性药物释放

首先利用阳离子开环聚合合成了超支化聚缩水甘油醚（HPG）,然后通过酯化反应制备了低接枝率的大分子引发剂HPG-Br,并进一步引发甲基丙烯酸-2-（N,N-二甲氨基）乙酯（DMAEMA）单体的原子转移自由基聚合,合成了低接枝率的双亲水性超支化接枝共聚物HPG-g-PDMAEMA,用1HNMR和GPC对聚合物结构进行了表征.并采用芘荧光探针法,HNMR和DLS研究了HPG-g-PDMAEMA在不同pH水溶液中的组装行为.以1香豆素102为模型药物研究了HPG-g-PDMAEMA聚合物在不同pH条件下的药物释放行为,发现在pH连续振荡刺激下HPG-g-PDMAEMA聚合物胶束对药物分子能实现部分＂可逆＂的释放和再包载.     

pH敏感两亲性嵌段聚合物的合成及其对新型抗生物膜药物的控释研究

采用ATRP技术,以PEG Br为大分子引发剂,2-二异丙氨基乙基甲基丙烯酸酯(DPA)为单体,合成了一种pH敏感两亲性嵌段聚合物PEG-b-PDPA,其结构经¹H NMR和GPC确证。采用超声乳化法制备了包载新型抗生物膜药物的聚合物载药胶束（1）,并研究了其结构和性能。结果表明：1的粒径均一、结构稳定,载药率和包封率分别为13.25%和79.50%。在酸性条件下（pH 5.5）, 1解组装并释放包裹在疏水“核层”的抗生物膜药物。     

聚L-谷氨酸担载胰岛素口服微球的制备与评价

以聚L-谷氨酸为载体材料, 采用无水乳液法制备了口服胰岛素微球, 微球直径在5~20 μm, 载药质量分数为5%~9%. 载药微球具有良好的pH敏感释放行为, 在胃模拟液中2 h释放量约为5%, 在肠道模拟液中2 h释放90%以上. 考察聚合物分子量、溶液浓度、理论投药量及混合材料对微球释放行为的影响.     

荧光标记pH敏感胶束的制备及其药物控释

利用原子转移自由基聚合方法（ATRP）合成了pH敏感的两亲性嵌段共聚物mPEG-b-PDPA_n（聚合度n=100-200）及荧光修饰的嵌段聚合物异硫氰酸荧光素-聚乙二醇-聚N,N-二异丙胺基甲基丙烯酸乙酯（FITCPEG₄₅-PDPA₁₀₀）。采用溶剂挥发的方法制备胶束,此胶束呈现均一的球形分布,平均粒径180-240 nm（0.3 mg·mL^-1）。以阿霉素（DOX）为模拟药物,其胶束载药量约11%（w,质量分数）左右,外环境pH对载药胶束的粒径和体外释放行为有显著影响。在弱酸环境下,胶束核质子化发生膨胀甚至解体,在2-3 h内药物可释放80%左右。体外毒性试验表明,空白胶束与人类肝癌细胞（Huh7）有良好的生物相容性。同时,与此细胞共同孵育5 h的荧光聚合物胶束体现了较好的转染效果。因此,这类荧光标记胶束可能会为实时跟踪化疗药物的输送或分布打开新的视角。     

基于透明质酸的缺氧响应型胶束的制备及性能研究

以透明质酸（HA）及硝基咪唑（NI）衍生物为原料,通过酰胺反应合成了一种两亲性接枝聚合物（HA-NI）.该聚合物具有缺氧响应性和肿瘤靶向性.利用傅里叶红外光谱（FT-IR）和核磁共振（NMR）对接枝聚合物的结构进行了表征,同时基于¹H NMR计算出接枝聚合物中NI的取代度.HA-NI在水中自组装形成胶束,利用动态光散射仪（DLS）表征胶束大小并对胶束的稳定性进行了研究,利用原子力显微镜（AFM）和透射电镜（TEM）观察胶束形貌.载药胶束的载药率（DL）和包封率（EE）通过紫外-可见吸收光谱（UV）测试并计算得到.胶束的缺氧响应性利用DLS、AFM、TEM、UV等探究.实验证明,该聚合物胶束具有缺氧响应性并对药物表现出良好的控制释放能力,在常氧环境下,胶束稳定存在;而在缺氧环境下,胶束散开,药物快速且完全地释放.     

双重敏感mPEG-PDPA-P(AAm-co-AN)聚合物自组装体的药物递送

设计合成了一种新型两亲性三嵌段ABC聚合物聚乙二醇单甲醚-聚甲基丙烯酸二异丙胺基乙酯-聚(丙烯酰胺-co-丙烯腈)(mPEG-PDPA-P(AAm-co-AN))。该聚合物具有pH敏感嵌段PDPA和温度敏感嵌段P(AAm-co-AN)，临界溶解温度(UCST)较高，且可以通过改变单体比例来调节UCST。在室温、中性环境下，该聚合物通过自组装形成刺激响应型胶束，可用于抗肿瘤药物的控释研究。温度升高诱导聚合物胶束向不对称囊泡结构转变，pH降低促使聚合物形成更加松散的胶束。在体外释药探究中，聚合物胶束对亲水药物阿霉素(DOX)和疏水药物槲皮素都具有良好的载药效果，在37℃、pH=7.4的条件下泄漏量低，随着温度升高和pH降低，胶束释放药物的速率和释放量明显增加。     

PtBA-g-PPEGMEMA接枝共聚物的合成及其包埋阿霉素的研究

通过可逆加成-裂解链转移聚合和原子转移自由基聚合,制备了以聚丙烯酸叔丁酯为主链、以聚(聚乙二醇单甲醚甲基丙烯酸酯)为侧链的两亲性接枝共聚物PtBA-g-PPEGMEMA,该方法克服了以往通过聚合物修饰来引入接枝点时所存在的接枝点密度不高和不可控的局限性.接着,以PtBA-g-PPEGMEMA为载体,对抗肿瘤药物阿霉素进行了负载,制备得到了尺寸为164.8nm的纳米载药胶束.其释放试验表明,该体系具有缓释特征.     

ATRP和点击化学结合法制备PDMAAm—PDMS—PDMAAm嵌段聚合物

采用原子转移自由基聚合（ATRP）法制得了端基分别为烯丙基和溴原子的聚二甲基丙烯酰胺（PDMAAm），经叠氮基亲核取代后与端炔基聚二甲基硅氧烷进行点击反应，得到两亲三嵌段聚合物。利用^1HNMR、FTIR、GPC等测试方法对聚合物的结构进行了表征。结果表明：采用ATRP法合成的PDMAAm均聚物分子量分布较窄，通过点击化学法将热力学不相容的亲水性PDMAAm链段及疏水性聚二甲基硅氧烷（PDMS）链段制备PDMAAmPDMS—PDMAAm嵌段聚合物，是一种高效易行的方法。     

Characteristic differences in the formation of complex coacervate core micelles from neodymium and zinc-based coordination polymers

In this paper we compare the formation of complex coacervate core micelles (C3Ms) from two different tricompontent mixtures, namely neodymium, the bisligand L2EO4 and the poly(cation)-block-poly(neutral) diblock copolymer P2MVP41-b-PEO205, and zinc, L2EO4 and P2MVP41-b-PEO205 mixed systems. Three sets of titration experiments were carried out for each system: (i) titration of diblock copolymer P2MVP41-b-PEO205 with the stoichiometric mixture of metal ions and bisligands, (ii) titration of a mixture of diblock copolymer and bisligand with metal ions, and (iii) titration of a mixture of diblock copolymer and metal ions with bisligands. In all the above three cases, micelles are found to form either in a broad range of charge ratios or in a broad range of metal/bisligand ratios. Upon addition of Nd2-(L2EO4)3 coordination polymer to P2MVP41-b-PEO205 solution, and upon addition of Nd3+ to a mixture of L2EO4 and P2MVP41-b-PEO205, micelles are found to form immediately after the first addition, whereas micelles show up in the similar zinc system only after a certain threshold Zn-(L2EO4) or Zn2+ concentration. This difference can be traced to the different structures of the Nd2-(L2EO4)3 and Zn-(L2EO4) coordination compounds. At very low concentrations, Zn-(L2EO4) are ring-like oligomers, but Nd2-(L2EO4)3 are larger networks. The network structure favors the formation of coacervate micellar core with P2MVP41-b-PEO205. Moreover, excess of Nd3+ ions will break up the C3Ms, while the same amount of Zn2+ has hardly any effect on the C3Ms. The breakdown of C3Ms by Nd3+ is due to the charge inversion of the coordination complex with increasing [Nd3+]/[L2EO4] ratio, which results in repulsive interaction between the coordination complex and the diblock copolymer, whereas no such interaction can occur in the zinc system.     

Light‐driven and aggregation‐induced emission from side‐chain azoindazole polymers

The well‐defined azoindazole‐containing homopolymer, poly(6‐{6‐[(4‐dimethylamino) phenylazo]‐indazole}‐hexyl methacrylate) (PDHMA), and amphiphilic diblock copolymer, poly({6‐[6‐(4‐dimethylamino)phenylazo]‐indazole}‐hexyl methacrylate)‐b‐poly(2‐(dimethylamino)ethylmethacrylate) (PDHMA_m‐b‐PDMAEMA_n), were successfully prepared via reversible addition‐fragmentation chain transfer polymerization technique. The homopolymer and amphiphilic diblock copolymer in CH₂Cl₂ exhibited intense fluorescence emission accompanied by trans–cis photoisomerization of azoindazole group under UV irradiation. The experiment results indicated that the intense fluorescence emission may be attributed to an inhibition of photoinduced electron transfer of the cis form of azoindazole. On the other hand, the intense fluorescence emission of amphiphilic diblock copolymers in water‐tetrahydrofuran mixture was observed, which increased with the volume ratio of water in the mixed solvent. The self‐aggregation behaviors of three amphiphilic diblock copolymers were examined by transmission electron microscopy, laser light scattering, and UV–vis spectra. The restriction of intramolecular rotation of the azoindazole groups in aggregates was considered as the main cause of aggregation‐induced fluorescence emission. © 2011 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2011.     

Biocompatible poly(ethylene glycol)‐poly(γ‐cholesterol‐L‐glutamate) copolymers: Synthesis,characterization, and in vitro studies

A novel amphiphilic poly(ethylene glycol)‐block‐poly(γ‐cholesterol‐L ‐glutamate) (mPEG–PCHLG) diblock copolymer has been synthesized. The mPEG–PCHLG copolymer has good biocompatibility and low toxicity. The mPEG–PCHLG copolymers could aggregate into nanoparticles with PCHLG blocks as the hydrophobic core and PEG blocks as the hydrophilic shell through emulsion solvent evaporation method. The copolymers were characterized by nuclear magnetic resonance spectroscopy, mass spectrum, Fourier transform infrared spectroscopy, and gel permeation chromatography. The particle sizes, size distributions, and zeta potentials of nanoparticles can also be determined by dynamic light scattering and transmission electron microscopy. This work provides a new and facile approach to prepare amphiphilic block copolymer nanoparticles with controllable performances. This novel copolymer may have potential applications in drug delivery and bioimaging applications.© 2012 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2012     

Preparation and characterization of poly(2‐methacryloyloxyethyl phosphorylcholine)‐block‐poly(D,L‐lactide) polymer nanoparticles

A poly(D,L ‐lactide)–bromine macroinitiator was synthesized for use in the preparation of a novel biocompatible polymer. This amphiphilic diblock copolymer consisted of biodegradable poly(D,L ‐lactide) and 2‐methacryloyloxyethyl phosphorylcholine and was formed by atom transfer radical polymerization. Polymeric nanoparticles were prepared by a dialysis process in a select solvent. The shape and structure of the polymeric nanoparticles were determined by ¹H NMR, atomic force microscopy, and ζ‐potential measurements. The results of cytotoxicity tests showed the good cytocompatibility of the lipid‐like diblock copolymer poly(2‐methacryloyloxyethyl phosphorylcholine)‐block‐poly(D,L ‐lactide). © 2006 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 45: 688–698, 2007     

一种两亲性嵌段共聚物胶束的制备及其对叶酸的负载和控制释放

采用可逆加成-断裂链转移(RAFT)聚合合成了以丙烯酸异丁酯(IBA)、甲基丙烯酸2-二甲氨乙酯(DMAEMA)无规共聚嵌段与聚丙烯酸-2-羟丙酯(PHPA)组成的两亲性两嵌段共聚物(P( IBA-co-DMAEMA)-b-PHPA),并用凝胶渗透色谱(GPC)、核磁共振波谱(1H-NMR)及红外光谱(FTIR)对其进...     

Synthesis and characterization of a biodegradable amphiphilic copolymer based on branched poly(ϵ‐caprolactone) and poly(ethylene glycol)

A novel biodegradable amphiphilic copolymer with hydrophobic poly(ε‐caprolactone) branches containing cholic acid moiety and a hydrophilic poly(ethylene glycol) chain was synthesized. The copolymer was characterized by FTIR, ¹H NMR, gel permeation chromatography (GPC), differential scanning calorimetry (DSC), polarizing light microscopy (PLM), and wide‐angle X‐ray diffraction (WAXD) analysis. The amphiphilic copolymer could self‐assemble into micelles in an aqueous solution. The critical micelle concentration of the amphiphilic copolymer was determined by fluorescence spectroscopy. A nanoparticle drug delivery system with a regularly spherical shape was prepared with high encapsulation efficiency. The in vitro drug release from the drug‐loaded polymeric nanoparticles was investigated. Because of the branched structure of the hydrophobic part of the copolymer and the relatively fast degradation rate of the copolymer, an improved release behavior was observed. © 2007 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 45: 5256–5265, 2007     

Controlled supramolecular assembly of micelle-like gold nanoparticles in PS-b-P2VP diblock copolymers via hydrogen bonding

We report a facile strategy to synthesize amphiphilic gold (Au) nanoparticles functionalized with a multilayer, micelle-like structure consisting of a Au core, an inner hydroxylated polyisoprene (PIOH) layer, and an outer polystyrene shell (PS). Careful control of enthalpic interactions via a systematic variation of structural parameters, such as number of hydroxyl groups per ligand (N(OH)) and styrene repeating units (N(PS)) as well as areal chain density of ligands on the Au-core surface (Σ), enables precise control of the spatial distribution of these nanoparticles. This control was demonstrated in a lamellae-forming poly(styrene-b-2-vinylpyridine) (PS-b-P2VP) diblock copolymer matrix, where the favorable hydrogen-bonding interaction between hydroxyl groups in the PIOH inner shell and P2VP chains in the PS-b-P2VP diblock copolymer matrix, driving the nanoparticles to be segregated in P2VP domains, could be counter balanced by the enthalphic penalty of mixing of the PS outer brush with the P2VP domains. By varying N(OH), N(PS), and Σ, the nanoparticles could be positioned in the PS or P2VP domains or at the PS/P2VP interface. In addition, the effect of additives interfering with the hydrogen-bond formation between hydroxyl groups on Au nanoparticles and P2VP chains in a diblock copolymer matrix was investigated, and an interesting pea-pod-like segregation of Au nanoparticles in PS domains was observed.     

Synthesis of chiral amphiphilic diblock copolymers via consecutive RAFT polymerizations and their aggregation behavior in aqueous solution

Two chiral amphiphilic diblock copolymers with different relative lengths of the hydrophobic and hydrophilic blocks, poly(6‐O‐p‐vinylbenzyl‐1,2:3,4‐Di‐O‐isopropylidene‐D ‐galactopyranose)‐b‐poly(N‐isopropylacrylamide) or poly(VBCPG)‐b‐poly(NIPAAM) and poly(20‐(hydroxymethyl)‐pregna‐1,4‐dien‐3‐one methacrylate)‐b‐poly(N‐isopropylacrylamide) or poly(MAC‐HPD)‐b‐poly(NIPAAM) were synthesized via consecutive reversible addition‐fragmentation chain‐transfer polymerizations of VBCPG or MAC‐HPD and NIPAAM. The chemical structures of these diblock copolymers were characterized by ¹H nuclear magnetic resonance spectroscopy. These amphiphilic diblock copolymers could self‐assemble into micelles in aqueous solution, and the morphologies of micelles were investigated by transmission electron microscopy. By comparison with the lower critical solution temperatures (LCST) of poly(NIPAAM) homopolymer in deionized water (32 °C), a higher LCST of the chiral amphiphilic diblock copolymer (poly(VBCPG)‐b‐poly(NIPAAM)) was observed and the LCST increased with the relative length of the poly(VBCPG) block in the copolymer from 35 to 47 °C, respectively. © 2008 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 46: 7690–7701, 2008     

两亲性嵌段共聚物mPEG-b-PCL/FA的合成及其药物释放性能

以苯甲醇为引发剂,在辛酸亚锡催化下引发ε-环己内酯(ε-CL )开环聚合,合成了聚己内酯(PCL).分别利用端甲氧基聚乙二醇(mPEG)、PCL及叶酸(FA)与三氯三嚎中不同的氯反应,得到两亲性嵌段共聚物mPEG-b-PCL/FA;采用傅立叶变换红外光谱仪和核磁共振谱仪等表征了mPEG-b-PCL/FA的组成和结构;采...     

Synthesis,characterization, and property of amphiphilic fluorinated abc‐type triblock copolymers

Novel amphiphilic fluorinated ABC‐type triblock copolymers composed of hydrophilic poly(ethylene oxide) monomethyl ether (MeOPEO), hydrophobic polystyrene (PSt), and hydrophobic/lipophobic poly(perfluorohexylethyl acrylate) (PFHEA) were synthesized by atom transfer radical polymerization (ATRP) using N,N,N′,N″,N″‐pentamethyldiethylenetriamine (PMDETA)/CuBr as a catalyst system. The bromide‐terminated diblock copolymers poly(ethylene oxide)‐block‐polystyrene (MeOPEO‐b‐PSt‐Br) were prepared by the ATRP of styrene initiated with the macroinitiator MeOPEO‐Br, which was obtained by the esterification of poly(ethylene oxide) monomethyl ether (MeOPEO) with 2‐bromoisobutyryl bromide. A fluorinated block of poly(perfluorohexylethyl acrylate) (PFHEA) was then introduced into the diblock copolymer by a second ATRP process to synthesize a novel ABC‐type triblock copolymer, poly(ethylene oxide)‐block‐polystyrene‐block‐poly(perfluorohexylethyl acrylate) (MeOPEO‐b‐PSt‐b‐PFHEA). These block copolymers were characterized by means of proton nuclear magnetic resonance (¹H NMR) and gel permeation chromatography (GPC). Water contact angle measurements revealed that the polymeric coating of the triblock copolymer (MeOPEO‐b‐PSt‐b‐PFHEA) shows more hydrophobic than that of the corresponding diblock copolymer (MeOPEO‐b‐PSt). Bovine serum albumin (BSA) was used as a model protein to evaluate the protein adsorption property and the triblock copolymer coating posseses excellent protein‐resistant character prior to the corresponding diblock copolymer and polydimethylsiloxane. These amphiphilic fluoropolymers can expect to have potential applications for antifouling coatings and antifouling membranes. © 2011 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2011