Nitroxide mediated living radical polymerization of styrene onto poly (vinyl chloride)

Nitroxide‐mediated ‘living’ free radical polymerisation (LREP) was employed for the first time to prepare graft copolymer by having arylated poly (vinyl chloride) (PVC‐Ph) as a backbone and polystyrene (PS) as branches. The graft copolymerization of styrene was initiated by arylated PVC carrying 2,2,6,6‐tetramethyl‐1‐piperidinyloxy (TEMPO) groups as a macroinitiator. Thus, the arylated PVC was prepared in the mild conditions and these reaction conditions could overcome the problem of gelation and crosslinking in polymers. Then, 1‐hydroxy TEMPO was synthesized by the reduction of TEMPO with sodium ascorbate. This functional nitroxyl compound was coupled with brominated arylated PVC (PVC‐Ph‐Br). The resulting macro‐initiator (PVC‐Ph‐TEMPO) for ‘living’ free radical polymerization was then heated in the presence of styrene to form graft copolymer. DSC, GPC, ¹HNMR, and FT‐IR spectroscopy were employed to investigate the structure of the polymers. Copyright © 2007 John Wiley & Sons, Ltd.     

Synthesis of well‐defined multigraft copolymers by a two‐step living radical polymerization with nitroxyl‐functionalized poly(methyl methacrylate)

Novel multigraft copolymers of poly(methyl methacrylate‐graft‐polystyrene) (PMMA‐g‐PS) in which the number of graft PS side chains was varied were prepared by a subsequent two‐step living radical copolymerization approach. A polymerizable 4‐vinylbezenyl 2,2,6,6‐tetramethyl‐1‐piperidinyloxy (TEMPO) monomer (STEMPO), which functioned as both a monomer and a radical trapper, was placed in a low‐temperature atom transfer radical polymerization (60°C) process of methyl methacrylate with ethyl 2‐bromopronionate (EPNBr) as an initiator to gain ethyl pronionate‐capped prepolymers with TEMPO moieties, PMMA‐STEMPOs. The number of TEMPO moieties grafted on the PMMA backbone could be designed by varying STEMPO/EPNBr, for example, the ratios of 1/2, 2/3, or 3/4 gained one, two, or three graft TEMPO moieties, respectively. The resulting prepolymers either as a macromolecular initiator or a trapper copolymerized with styrene in the control of stable free‐radical polymerization at an elevated temperature (120 °C), producing the corresponding multigraft copolymers, PMMA‐g‐PSs. The nitroxyl‐functionalized PMMA prepolymers produced a relatively high initiation efficiency (>0.8) as a result of the stereohindrance and slow diffusion of TEMPO moieties connected on the long PMMA backbone. The polymerization kinetics in two processes showed a living radical polymerization characteristic. The molecular structures of these prepolymers and graft copolymers were well characterized by combining Fourier transform infrared spectroscopy, gel permeation chromatography, chemical element analysis, and ¹H NMR. © 2002 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 40: 1876–1884, 2002     

Deactivation reactions in the modeled 2,2,6,6‐tetramethyl‐1‐piperidinyloxy‐mediated free‐radical polymerization of styrene: A comparative study with the 2,2,6,6‐tetramethyl‐1‐piperidinyloxy/acrylonitrile system

The competitiveness of the combination and disproportionation reactions between a 1‐phenylpropyl radical, standing for a growing polystyryl macroradical, and a 2,2,6,6‐tetramethyl‐1‐piperidinyloxy (TEMPO) radical in the nitroxide‐mediated free‐radical polymerization of styrene was quantitatively evaluated by the study of the transition geometry and the potential energy profiles for the competing reactions with the use of quantum‐mechanical calculations at the density functional theory (DFT) UB3‐LYP/6‐311+G(3df, 2p)//(unrestricted) Austin Model 1 level of theory. The search for transition geometries resulted in six and two transition structures for the radical combination and disproportionation reactions, respectively. The former transition structures, mainly differing in the out‐of‐plane angle of the N? O bond in the transition structure TEMPO molecule, were correlated with the activation energy, which was determined to be in the range of 8.4–19.4 kcal mol^?1 from a single‐point calculation at the DFT UB3‐LYP/6‐311+G(3df, 2p)//unrestricted Austin Model 1 level. The calculated activation energy for the disproportionation reaction was less favorable by a value of more than 30 kcal mol^?1 in comparison with that for the combination reaction. The approximate barrier difference for the TEMPO addition and disproportionation reaction was slightly smaller for the styrene polymerization system than for the acrylonitrile polymerization system, thus indicating that a β‐proton abstraction through a TEMPO radical from the polymer backbone could diminish control over the radical polymerization of styrene with the nitroxide even more than in the latter system. © 2006 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 45: 232–241, 2007     

Modification of cellulose by graft polymerization for use in drug delivery systems

Cellulose-based biodegradable polymers—as microspheres or hydrogels—are suitable for drug delivery systems. In this work, cellulose microfibers were converted to cellulose esters for subsequent graft copolymerization either by free radical or atom transfer radical polymerization (ATRP). For the former, carboxymethyl cellulose (CMC) was prepared and then modified through grafting of poly(hydroxyethyl acrylate) or polyacrylamide. ATRP was achieved by chloroacetylation of cellulose followed by graft copolymerization of hydroxyethyl acrylate or acrylamide monomers. The degree of substitution for CMC and chloroacetylated cellulose (CAC) was determined by the method described in US Pharmacopeia NF24 and by titration method, respectively. CMC, CAC, and the grafted copolymers were characterized by Fourier transform infrared spectroscopy, differential scanning calorimetry, thermal gravimetric analysis, X-ray diffraction, and atomic force microscopy; the latter technique clearly shows the chain growth of the synthetic polymers on the backbone surface. Furthermore, cephalexin antibiotic was loaded on the copolymers, and the resultant in vitro drug release studied in three different media (buffer solutions with pH equal to 3, 6.1, and 8).     

“Living” radical graft polymerization of styrene to styrene butadiene rubber (SBR) with 2,2,6,6‐tetramethyl‐1‐piperidinyloxy (TEMPO)

Well‐defined graft copolymers with styrene butadiene rubber (SBR) backbones and polystyrene branches were synthesized by living free radical polymerization (LFRP) techniques. Thus 1‐ benzoyl‐2‐phenyl‐2‐(2′,2′,6′,6′‐tetramethyl‐piperidinyl‐1′‐oxy)ethane (BZ‐TEMPO) was synthesized and hydrolyzed to the corresponding 1‐hydroxyl derivative. This functional nitroxyl compound was coupled with brominated SBR (SBR‐Br). The resulting macroinitiator (SBR‐TEMPO) for “living” free radical polymerization was then heated in the presence of styrene for the formation of the controlled graft copolymer. ¹H‐NMR and IR spectroscopy were used to investigate the structure of the polymers. Copyright © 2004 John Wiley & Sons, Ltd.     

Biodegradable brushlike graft polymers. I. Polymerization of ϵ‐caprolactone onto water‐soluble hydroxypropyl cellulose as the backbone by the protection of the trimethylsilyl group

After the protection of partial hydroxyl groups with trimethylsilyl (TMS) groups, hydroxypropyl cellulose becomes soluble in organic solvents, and the number of hydroxyl groups as initiating groups can be controlled. As a result, a new brushlike graft poly(?‐caprolactone) can be prepared with hydroxypropyl cellulose as the backbone polymer by homogeneous ring‐opening graft polymerization and deprotection. The protection and deprotection of the TMS group during the entire procedure were carefully monitored with Fourier transform infrared (FTIR) and NMR, and the final graft copolymers were characterized with FTIR, ¹H NMR, ¹³C NMR, gel permeation chromatography, and differential scanning calorimetry. © 2002 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 41: 273–280, 2003     

Controlled radical polymerization in the presence of N‐oxyls

Recent development in controlled radical polymerization has provided a tool to combine a relatively robust radical polymerization technique with structural control. This contribution focuses on stable free radical polymerization in the presence of nitroxides. The influence of 2,2,6,6‐tetramethyl‐piperidine‐N‐oxyl (TEMPO) and temperature on the copolymerization of styrene and acrylonitrile will be discussed. In the second part a new class of nitroxide stable free radicals will be presented that shows enhanced performance in styrene polymerizations.     

长链烷酸接枝羟丙基纤维素相变材料的制备及其性能

采用酯化的方法将具有相变特征的长链脂肪酸接枝到羟丙基纤维素主链上, 得到了一系列性能稳定, 温度范围适宜的高分子固-固相变材料, 并利用傅里叶红外光谱(FT-IR)、核磁共振(NMR)、差示扫描量热仪(DSC)、热失重分析仪(TGA)和X射线散射等技术手段对其化学结构及相变行为进行了研究。 结果表明, 该材料呈现出可逆的固-固相转变特性, 相变温度范围可通过改变脂肪酸的长度调节。 利用棕榈酸、硬脂酸和花生酸获得的相变材料焓值达到60 J/g, 所获得的材料在250 ℃以内不发生热分解。 通过将两种长链脂肪酸混合同时接枝到羟丙基纤维素主链上, 所得产物的吸/放热温度随着混合脂肪酸组分含量的变化而变化, 同时X射线散射的结果也证明羟丙基纤维素混合酯的分子间距是位于其两种单一酯之间的。这一结果为制备一定温度范围内任意相变温度的高分子固-固相变材料提供了简便的方法。     

Bromine isotopic signature facilitates de novo sequencing of peptides in free‐radical‐initiated peptide sequencing (FRIPS) mass spectrometry

We recently showed that free‐radical‐initiated peptide sequencing mass spectrometry (FRIPS MS) assisted by the remarkable thermochemical stability of (2,2,6,6‐tetramethyl‐piperidin‐1‐yl)oxyl (TEMPO) is another attractive radical‐driven peptide fragmentation MS tool. Facile homolytic cleavage of the bond between the benzylic carbon and the oxygen of the TEMPO moiety in o‐TEMPO–Bz–C(O)–peptide and the high reactivity of the benzylic radical species generated in ?Bz–C(O)–peptide are key elements leading to extensive radical‐driven peptide backbone fragmentation. In the present study, we demonstrate that the incorporation of bromine into the benzene ring, i.e. o‐TEMPO–Bz(Br)–C(O)–peptide, allows unambiguous distinction of the N‐terminal peptide fragments from the C‐terminal fragments through the unique bromine doublet isotopic signature. Furthermore, bromine substitution does not alter the overall radical‐driven peptide backbone dissociation pathways of o‐TEMPO–Bz–C(O)–peptide. From a practical perspective, the presence of the bromine isotopic signature in the N‐terminal peptide fragments in TEMPO‐assisted FRIPS MS represents a useful and cost‐effective opportunity for de novo peptide sequencing. Copyright © 2015 John Wiley & Sons, Ltd.     

Nickel‐Catalyzed Barton Decarboxylation and Giese Reactions: A Practical Take on Classic Transforms

Two named reactions of fundamental importance and paramount utility in organic synthesis have been reinvestigated, the Barton decarboxylation and Giese radical conjugate addition. N ‐hydroxyphthalimide (NHPI) based redox‐active esters were found to be convenient starting materials for simple, thermal, Ni‐catalyzed radical formation and subsequent trapping with either a hydrogen atom source (PhSiH₃) or an electron‐deficient olefin. These reactions feature operational simplicity, inexpensive reagents, and enhanced scope as evidenced by examples in the realm of peptide chemistry.     

Thermal self‐initiation of styrene in the presence of TEMPO radicals: Bulk and miniemulsion

In TEMPO (2,2,6,6,‐tetramethyl‐1‐piperidinyloxy) controlled styrene radical polymerizations, the thermal self‐initiation reaction of styrene monomer is one of the main sources for the deviations from ideal living polymerization. However, it is also important because it continuously generates radicals to compensate for the loss of radicals caused by the termination reactions and thereby maintains a reasonable reaction rate. In this report, different initial TEMPO concentrations were used in styrene miniemulsion polymerizations without any added initiator. The consumption rate of TEMPO or radical generation rate was calculated from the length of the induction period and the increasing total number of polymer chains. It was found that there is little difference between the miniemulsions and the corresponding bulk systems in terms of the length of the induction period, which increases linearly with initial TEMPO concentration. After the induction period, the consumption rate of TEMPO or radical generation rate was reduced to a lower level, and a faster initial polymerization rate was found in the bulk system compared to the corresponding miniemulsion system. © 2004 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 42: 4921–4932, 2004     

Synthesis of functional polyethylene graft copolymers by nitroxide‐mediated living radical polymerization

This paper describes a new method to prepare graft copolymers, such as polyethylene‐g‐polystyrene (PE‐g‐PS), with a relatively well‐controlled reaction mechanism. The chemistry involves a transformation process from the metallocene copolymerization of ethylene and m,p‐methylstyrene (m,p‐MS) to nitroxide‐mediated “living” free radical polymerization (LRFP) of styrene. The metallocene catalysis produces ethylene‐co‐m,p‐methylstyrene (EMS) random copolymers. Next, 1‐hydroxyl‐2,2,6,6‐tetramethylpiperidine (HO‐TEMPO) was synthesized by the reduction of TEMPO with sodium ascorbate. The macroinitiator (EMS‐TEMPO) was synthesized with the bromination reaction of EMS, and the following nucleofilic reaction with this functional nitroxyl compound. The resulting macroinitiator (EMS‐TEMPO) for LRFP was then heated in the presence of styrene to form graft copolymer. DSC, ¹H‐NMR, FTIR spectroscopy were employed to investigate the structure of the polymers. The results of Molau test showed that PE‐g‐PS could be a potential good compatilizer. Copyright © 2008 John Wiley & Sons, Ltd.     

Decomposition of model alkoxyamines in simple and polymerizing systems. I. 2,2,6,6‐tetramethylpiperidinyl‐ N‐oxyl‐based compounds

The thermal decomposition of five alkoxyamines labeled TEMPO–R, where TEMPO was 2,2,6,6‐tetramethylpiperidinyl‐N‐oxyl and R was cumyl (Cum), 2‐tert‐butoxy‐carbonyl‐2‐propyl (PEst), phenylethyl (PhEt), 1‐tert‐butoxy‐carbonylethyl (EEst), or 1‐methoxycarbonyl‐3‐methyl‐3‐phenylbutyl (Acrylate‐Cum), was studied with ¹H NMR in the absence and presence of styrene and methyl methacrylate. The major products were alkenes and the hydroxylamine 1‐hydroxy‐2,2,6,6‐tetramethyl‐ piperidine (TEMPOH), and in monomer‐containing solutions, unimeric and polymeric alkoxyamines and alkenes were also found. Furthermore, the reactions between TEMPO and the radicals EEst and PEst were studied with chemically induced dynamic nuclear polarization. In comparison with coupling, TEMPO reacted with the radicals Cum, PEst, PhEt, and EEst and their unimeric styrene adducts by disproportionation to alkenes and TEMPOH only to a minor extent (0.6–3%) but with the radical adducts to methyl methacrylate to a considerable degree (≥20%). Parallel to the radical cleavage, TEMPO–EEst (but not the other alkoxyamines or TEMPO–Acrylate‐Cum) underwent substantial nonradical decay. The consequences for TEMPO‐mediated living radical polymerizations are discussed. © 2001 John Wiley & Sons, Inc. J Polym Sci Part A: Polym Chem 39: 3604–3621, 2001     

Porphyrin derivatives act as vinylene monomers in TEMPO‐mediated radical copolymerization with styrene

In this article, we offer clear evidence for the radical copolymerizability of porphyrin rings in 2,2,6,6‐tetramethyl‐1‐piperidinyloxy (TEMPO)‐mediated radical copolymerizations with styrene. The radical copolymerizations of styrene with 5,10,15,20‐tetrakis(pentafluorophenyl)porphyrin (H₂TFPP) was conducted using 1‐phenyl‐1‐(2,2,6,6‐tetramethyl‐1‐piperidinyloxy)ethane as an initiator. The refractive index (RI) traces for the size‐exclusion chromatography of the resulting copolymers were unimodal with narrow molecular weight distributions. The RI traces shifted toward higher molecular weight regions as the polymerization progressed, and the number‐average molecular weights were close to those calculated on the basis of the feed compositions and monomer conversions. These features were in good agreement with a TEMPO‐mediated mechanism. The traces recorded by the ultraviolet‐visible (UV‐vis) detector (430 nm) were identical to those obtained by the RI detector, indicating a statistical copolymerization of styrene with H₂TFPP. This also indicated that H₂TFPP acted as a monomer and not as a terminator or a chain‐transfer agent under the conditions used. A benzyl radical addition to H₂TFPP was conducted as a model reaction for the copolymerization using tributyltin hydride as a chain‐transfer agent, affording a reduced porphyrin, 2‐benzyl‐5,10,15,20‐tetrakis(pentafluorophenyl)chlorin 1 , via radical addition to the β‐pyrrole position. The UV‐vis spectrum of 1 was fairly similar to that of poly(styrene‐co‐H₂TFPP), indicating that H₂TFPP polymerized at its β‐pyrrole position in the TEMPO‐mediated radical polymerization. TEMPO‐mediated radical copolymerizations of styrene with several porphyrin derivatives were also demonstrated. © 2012 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2012     

Calcium phosphate mineralization controlled by carboxymethyl cellulose-g-polymethacrylic acid

Carboxymethyl cellulose-grafted polymethacrylic acid (CMC-g-PMAA) was synthesized by graft copolymerization process onto carboxymethyl cellulose backbone using methacrylic acid as a monomer and ammonium persulfate as a free radical initiator. CMC-g-PMAA was employed as dispersed template for controlling calcium phosphate mineralization from aqueous solutions at different copolymer contents and pHs. Hybrids with different morphologies and particles diameter were investigated by adjusting of preparation conditions. Synthesized hybrids were characterized by FT-IR, SEM, XRD, and particle size analyzer. Such functionalized hybrids with complex morphologies can be manipulated as a novel reinforcing fillers, ceramic precursors, or biomedical implants.     

Graft copolymerization of 2‐methacryloyloxyethyl phosphorylcholine to cellulose in homogeneous media using atom transfer radical polymerization for providing new hemocompatible coating materials

To develop new hemopurification systems based on cellulose membrane, we synthesized a graft copolymer of cellulose with poly(2‐methacryloyloxyethyl phosphorylcholine) (MPC) by a metal‐catalyzed atom transfer radical polymerization process in homogeneous media. First, cellulose was dissolved in a DMAc/LiCl solution system, and it reacted with 2‐bromoisobutyloyl bromide to produce macroinitiator (cell‐BiB). Then, MPC was polymerized to the cellulose backbone in a homogeneous DMSO/methanol mixture solution in the presence of cell‐BiB. Characterization with FT‐IR, NMR, and GPC measurements showed that there obtained a graft copolymer of cellulose backbone and poly(MPC) side chains (cell‐PMPC) with well‐defined structure, indicating a controlled/“living” radical polymerization. The proteins adsorption studies showed that cellulose membranes modified by the as‐prepared cell‐PMPC owns good protein adsorption resistance. © 2008 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 46: 3306–3313, 2008     

Photoinduced Deoxygenative Borylations of Aliphatic Alcohols

A photochemical method for converting aliphatic alcohols into boronic esters is described. Preactivation of the alcohol as a 2‐iodophenyl‐thionocarbonate enables a novel Barton–McCombie‐type radical deoxygenation that proceeds efficiently with visible light irradiation and without the requirement for a photocatalyst, a radical initiator, or tin or silicon hydrides. The resultant alkyl radical is intercepted by bis(catecholato)diboron, furnishing boronic esters from a diverse range of structurally complex alcohols.     

Synthesis and characterization of highly fluorescent polythiophene derivatives containing polystyrene sidearms

In this study, macroinitiators with different content of atom‐transfer radical polymerization (ATRP) functional group on polythiophene backbone were first prepared by the copolymerization of 3‐[1‐ethyl‐2‐(2‐bromopropionate)]thiophene and 3‐hexylthiophene with various feed ratio. Then poly [3‐hexyl‐2,5‐thienylene‐co‐3‐[1‐ ethyl‐2‐(2‐[poly(styrene)]propionate)]‐2,5‐thienylene] (PTTBr‐PS) with different graft density were obtained by ATRP of styrene from these macroinitiators in anisole. The degree of polymerization of PS sidearm (DP_PS) was controlled by polymerization time. The structures of obtained graft copolymers were characterized by gel permeation chromatography (GPC), nuclear magnetic resonance (¹H NMR) and differential scanning calorimetry (DSC). Introduction of the PS sidearms onto the backbone of polythiophene was an attempt to trap the polythiophene backbone in a “solution‐like” conformation, thus inhibit the packing of polythiophene backbone and result in the improvement of fluorescent property in solid state. This was verified by the UV–vis and fluorescence analyses. Besides, it was also found that the optical property of PTTBr‐PS graft copolymer was dominated by its graft density and independent on the degree of polymerization of its PS sidearm. © 2007 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 46: 1003–1013, 2008     

Graft copolymerization ofN‐vinyl‐pyrrolidone and acrylamide on cellulose derivatives: synthesis,characterization and study of their biological effect

Graft copolymers of carboxymethyl cellulose and hydroxyethyl cellulose with N‐vinyl‐2‐pyrrolidone and acrylamide have been synthesized by grafting copolymer of N‐vinyl‐2‐pyrrolidone and acrylamide onto a mixture of carboxymethyl cellulose and hydroxyethyl cellulose by a solution polymerization technique using a redox initiation system. The graft copolymers were characterized by ¹³C‐NMR spectroscopy and scanning electron microscopy. These graft copolymers have been tested for their biodegradability and biological activity. None of the graft copolymer solutions shows any microbial degradation up to 10 days. The reported results are evidence of the possibility of anti‐fungi effect. Copyright © 2002 John Wiley & Sons, Ltd.     

Disulfide bond cleavage in TEMPO-free radical initiated peptide sequencing mass spectrometry

The gas‐phase free radical initiated peptide sequencing (FRIPS) fragmentation behavior of o‐TEMPO‐Bz‐conjugated peptides with an intra‐ and intermolecular disulfide bond was investigated using MSⁿ tandem mass spectrometry experiments. Investigated peptides included four peptides with an intramolecular cyclic disulfide bond, Bactenecin (RLC RIVVIRVC R), TGF‐α (C HSGYVGVRC ), MCH (DFDMLRC MLGRVFRPC WQY) and Adrenomedullin (16–31) (C RFGTC TVQKLAHQIY), and two peptides with an intermolecular disulfide bond. Collisional activation of the benzyl radical conjugated peptide cation, which was generated through the release of a TEMPO radical from o‐TEMPO‐Bz‐conjugated peptides upon initial collisional activation, produced a large number of peptide backbone fragments in which the S? S or C? S bond was readily cleaved. The observed peptide backbone fragments included a‐, c‐, x‐ or z‐types, which indicates that the radical‐driven peptide fragmentation mechanism plays an important role in TEMPO‐FRIPS mass spectrometry. FRIPS application of the linearly linked disulfide peptides further showed that the S? S or C? S bond was selectively and preferentially cleaved, followed by peptide backbone dissociations. In the FRIPS mass spectra, the loss of ?SH or ?SSH was also abundantly found. On the basis of these findings, FRIPS fragmentation pathways for peptides with a disulfide bond are proposed. For the cleavage of the S? S bond, the abstraction of a hydrogen atom at C_β by the benzyl radical is proposed to be the initial radical abstraction/transfer reaction. On the other hand, H‐abstraction at C_α is suggested to lead to C? S bond cleavage, which yields [ion ± S] fragments or the loss of ?SH or ?SSH. Copyright © 2011 John Wiley & Sons, Ltd.