Polyacrylamides containing pendant aminobisphosphonate groups are synthesized via reversible addition‐fragmentation chain transfer (RAFT) polymerization and a multicomponent postpolymerization functionalization reaction. A Moedritzer–Irani reaction installs the phosphonic acid groups on well‐defined, RAFT‐generated polymers bearing a pendant amine. An alternate route to the same materials is developed utilizing a three‐component Kabachnik–Fields reaction and subsequent dealkylation. Kinetics of the RAFT polymerization of the polymer precursor are studied. Successful functionalization is demonstrated by NMR and FTIR spectroscopy and elemental analysis of the final polymers.
The superior capabilities of structured microreactors over batch reactors are demonstrated for reversible addition–fragmentation chain transfer (RAFT) solution polymerization of n‐butyl acrylate with the aid of simulations, explicitly accounting for the chain length distribution of all macrospecies types. Since perfect isothermicity can be established in a microreactor, less side products due to backbiting and β‐scission are formed compared to the batch operation in which ineffective heat removal leads to an undesirable temperature spike. For a given RAFT chain transfer agent (CTA), additional microstructural control results under microflow conditions by optimizing the reaction temperature, lowering the dilution degree, or decreasing the initial molar ratio of monomer to RAFT CTA.
A direct and facile route toward semitelechelic polymers, end‐functionalized with palladated sulfur–carbon–sulfur pincer (PdII‐pincer) complexes is reported that avoids any post‐polymerization step. Key to our methodology is the combination of reversible addition‐fragmentation chain‐transfer (RAFT) polymerization with functionalized chain‐transfer agents. This strategy yields Pd end‐group‐functionalized materials with monomodal molar mass dispersities (Đ ) of 1.18–1.44. The RAFT polymerization is investigated using a PdII‐pincer chain‐transfer agent for three classes of monomers: styrene, tert‐butyl acrylate, and N‐isopropylacrylamide. The ensuing PdII‐pincer end‐functionalized polymers are analyzed using 1H NMR spectroscopy, gel‐permeation chromatography, and elemental analysis. The RAFT polymerization methodology provides a direct pathway for the fabrication of PdII‐pincer functionalized polymers with complete end‐group functionalization.
A novel diblock copolymer consisting of poly(vinylferrocene) (PVFc) and poly(N,N‐diethylacrylamide) (PDEA) is synthesized via a combination of anionic and RAFT polymerization. The use of a novel route to hydroxyl‐end‐functionalized metallopolymers in anionic polymerization and subsequent esterification with a RAFT agent leads to a PVFc macro‐CTA ( = 3800 g mol−1; Đ = 1.17). RAFT polymerization with DEA affords block copolymers as evidenced by 1H NMR spectroscopy as well as size exclusion chromatography (6400 ≤ ≤ 33700 g mol−1; 1.31 ≤ Đ 1.28). Self‐assembly of the amphiphilic block copolymers in aqueous solution leads to micelles as shown via TEM. Importantly, the distinct thermo‐responsive and redox‐responsive character of the blocks is probed via dynamic light scattering and found to be individually and repeatedly addressable.
Copolymers of 2‐(methacrylamido)glucopyranose (MAG) and methacrylic acid (MAA) are synthesized by RAFT polymerization and then used as templates to prepare glycopolymer‐functionalized Ag nanoclusters (Gly‐Ag NCs) through microwave irradiation. Polymers and the resulting nanoclusters are characterized by NMR, GPC, UV‐Vis, SEM, TEM, AAS and fluorescence spectroscopy. The bio‐activity of the fluorescent Gly‐Ag NCs are further examined using GLUT‐1 over‐expressing cancer cells K562. Gly‐Ag NCs show efficient binding ability toward K562 cells and inhibit the cell viability in a dose dependent manner (IC50 = 0.65 μg mL–1), indicating their potential biological applications for both cancer imaging and targeted cancer therapy.
Advanced polymerization methodologies, such as reversible addition‐fragmentation transfer (RAFT), allow unprecedented control over star polymer composition, topology, and functionality. However, using RAFT to produce high throughput (HTP) combinatorial star polymer libraries remains, to date, impracticable due to several technical limitations. Herein, the methodology “rapid one‐pot sequential aqueous RAFT” or “rosa‐RAFT,” in which well‐defined homo‐, copolymer, and mikto‐arm star polymers can be prepared in very low to medium reaction volumes (50 µL to 2 mL) via an “arm‐first” approach in air within minutes, is reported. Due to the high conversion of a variety of acrylamide/acrylate monomers achieved during each successive short reaction step (each taking 3 min), the requirement for intermediary purification is avoided, drastically facilitating and accelerating the star synthesis process. The presented methodology enables RAFT to be applied to HTP polymeric bio/nanomaterials discovery pipelines, in which hundreds of complex polymeric formulations can be rapidly produced, screened, and scaled up for assessment in a wide range of applications.
The redox switchable formation of very well‐defined supramolecular graft polymers in aqueous solution driven by host–guest interactions between ferrocene (Fc) and cyclodextrin (CD) is presented. The Fc‐containing acrylic backbone copolymer (PDMA‐stat‐Fc) is prepared via reversible addition–fragmentation chain transfer (RAFT) copolymerization of N,N‐dimethylacrylamide (DMA) and the novel monomer N‐(ferrocenoylmethyl)acrylamide (NFMA). Via the RAFT process, copolymers containing variable Fc ratios (5‐10 mol%) are prepared, affording polymers of molecular masses of close to 11 000 g mol−1 and molar mass dispersities (Đ) of 1.2. The β‐cyclodextrin (β‐CD) containing building block is synthesized via RAFT‐polymerization, too, in order to afford a polymer with well‐defined molecular mass and low dispersity ( = 10 300 g mol−1, Đ = 1.1), employing a propargyl‐functionalized chain transfer agent for the polymerization of N,N‐diethylacrylamide (DEA). The polymerization product is subsequently terminated with β‐CD via the regiospecific copper (I)‐catalyzed 1,3‐cycloaddition (PDEA‐βCD). Host–guest interactions between Fc and CD lead to the formation of supramolecular graft‐polymers, verified via nuclear Overhauser enhancement spectroscopy (NOESY). Importantly, their redox‐responsive character is clearly confirmed via cyclic voltammetry (CV). The self‐assembly of the statistical Fc‐containing lateral polymer chain in aqueous solution leads to mono‐ and multi‐core micelle‐aggregates evidenced via TEM. Only diffused cloud‐like, non‐spherical nanostructures are observed after addition of PDEA‐βCD (TEM).
Enzymatic catalysis and control over macromolecular architectures from reversible addition‐fragmentation chain transfer polymerization (RAFT) are combined to give a new method of making polymers. Horseradish peroxidase (HRP) is used to catalytically generate radicals using hydrogen peroxide and acetylacetone as a mediator. RAFT is used to control the polymer structure. HRP catalyzed RAFT polymerization gives acrylate and acrylamide polymers with relatively narrow molecular weight distributions. The polymerization is rapid, typically exceeding 90% monomer conversion in 30 min. Complex macromolecular architectures including a block copolymer and a protein‐polymer conjugate are synthesized using HRP to catalytically initiate RAFT polymerization.
The preparation of physically crosslinked hydrogels from quasi ABA‐triblock copolymers with a water‐soluble middle block and hydrophobic end groups is reported. The hydrophilic monomer N‐acryloylmorpholine is copolymerized with hydrophobic isobornyl acrylate via a one‐pot sequential monomer addition through reversible addition fragmentation chain‐transfer (RAFT) polymerization in an automated parallel synthesizer, allowing systematic variation of polymer chain length and hydrophobic–hydrophilic ratio. Hydrophobic interactions between the outer blocks cause them to phase‐separate into larger hydrophobic domains in water, forming physical crosslinks between the polymers. The resulting hydrogels are studied using rheology and their self‐healing ability after large strain damage is shown.
Cationic polyelectrolytes showing an upper critical solution temperature (UCST) are synthesized by reversible addition‐fragmentation chain transfer (RAFT) polymerization in water at a temperature well above the UCST. The polymerization is well controlled by the RAFT process, with excellent pseudo‐first‐order kinetics. The cloud point is highly dependent on the polyelectrolyte concentration, molecular weight, and presence of added electrolyte. Alkylation of a neutral polymer is also conducted to obtain polyelectrolytes with different hydrophobic groups, which are shown to increase the cloud point.
Reversible addition–fragmentation chain transfer (RAFT) polymerization and characterization of an alkoxysilane acrylamide monomer using a trithiocarbonate chain transfer agent are described. Poly(N‐[3‐(trimethoxysilyl)propyl]acrylamide) (PTMSPAA) homopolymers are obtained with good control over the polymerization. A linear increase in the molecular weight is observed whereas the polydispersity values do not exceed 1.2 regardless of the monomer conversion. Moreover, PTMSPAA is used as a macro‐RAFT agent to polymerize N‐isopropylacrylamide (NIPAM). By varying the degree of polymerization of NIPAM within the block copolymer, different sizes of thermoresponsive particles are obtained. These particles are stabilized by the condensation of the alkoxysilane moieties of the polymers. Furthermore, a co‐network of silica and PTMSPAA is prepared using the sol–gel process. After drying, transparent mesoporous hybrids are obtained with a surface area of up to 400 m2 g−1.
Dopamine‐containing monomers, N‐3,4‐dihydroxybenzenethyl methacrylamide (DMA) and dimethylaminoethyl methacrylate (DMAEMA), are successfully copolymerized in a well‐controlled manner via ambient temperature single‐electron transfer initiation and propagation through the radical addition fragmentation chain transfer (SET‐RAFT) method. The controlled behaviors of the copolymerization are confirmed by the first‐order kinetic plots, the linear relationships between molecular weights, and the monomer conversions while keeping relatively narrow molecular weight distribution (Mw/Mn ≤ 1.45). Moreover, biomimetic self‐assembly of poly(N‐3,4‐dihydroxybenzenethyl methacrylamide‐co‐dimethylaminoethyl methacrylate) PDMA‐co‐PDMAEMA and inorganic particles are employed to prepare tunable honeycomb‐like porous hybrid particles (HPHPs) by regulating the predesigned chemical composition. In addition, the inorganic sacrificial templates are successfully selective etched for the formation of porous organic materials.
An efficient metal‐free homodifunctional bimolecular ring‐closure method is developed for the formation of cyclic polymers by combining reversible addition‐fragmentation chain transfer (RAFT) polymerization and self‐accelerating click reaction. In this approach, α,ω‐homodifunctional linear polymers with azide terminals are prepared by RAFT polymerization and postmodification of polymer chain end groups. By virtue of sym‐dibenzo‐1,5‐cyclooctadiene‐3,7‐diyne (DBA) as small linkers, well‐defined cyclic polymers are then prepared using the self‐accelerating double strain‐promoted azide–alkyne click (DSPAAC) reaction to ring‐close the azide end‐functionalized homodifunctional linear polymer precursors. Due to the self‐accelerating property of DSPAAC ring‐closing reaction, this novel method eliminates the requirement of equimolar amounts of telechelic polymers and small linkers in traditional bimolecular ring‐closure methods. It facilitates this method to efficiently and conveniently produce varied pure cyclic polymers by employing an excess molar amount of DBA small linkers.
This work provides a detailed insight into the synthesis of N‐(2‐hydroxypropyl)methacrylamide (HPMA) polymers employing the activated ester approach. In this approach, polypenta fluorophenyl methacrylate (PFPMA)‐activated ester polymers are synthesized by the reversible addition–fragmentation chain transfer (RAFT) polymerization and transferred into HPMA‐based systems by the use of 2‐hydroxypropylamine. To prove quantitative conversion in the absence of side reactions, special attention is devoted to investigate different reaction conditions by different analytical methods (1H, 19F, inverse‐gated 13C NMR, and zeta potential measurements). Furthermore the influence of common solvent impurities, such as water, is investigated. Besides differences in polymer tacticity, the poly(N‐(2‐hydroxypropyl) methacrylamide) (PHPMA) synthesized under water‐free conditions display the same properties like the conventional synthesized control‐PHPMA. However, 3% water content in the dimethylsulfoxide are already sufficient to yield PHPMA polymers with a negative zeta potential of –15.8 mV indication the presence of carboxylic groups due to partial hydrolysis of the activated ester.
A new, visible light‐catalyzed, one‐pot and one‐step reaction is successfully employed to design well‐controlled side‐chain functionalized polymers, by the combination of ambient temperature revisible addtion‐fragmentation chain transfer (RAFT) polymerization and click chemistry. Polymerizations are well controlled in a living way under the irradiation of visible light‐emitting diode (LED) light without photocatalyst and initiator, using the trithiocarbonate agent as iniferter (initiator‐transfer agent‐terminator) agent at ambient temperature. Fourier transfer infrared spectroscopy (FT‐IR), NMR, and matrix‐assisted laser desorption/ionization time‐of‐flight mass spectrometry (MALDI‐TOF‐MS) data confirm the successful one‐pot reaction. Compared to the reported zero‐valent metal‐catalyzed one‐pot reaction, the polymerization rate is much faster than that of the click reaction, and the visible light‐catalyzed one‐pot reaction can be freely and easily regulated by turning on and off the light.
Photoinitiated reversible addition‐fragmentation chain transfer (RAFT) dispersion polymerization of 2‐hydroxypropyl methacrylate is conducted in water at low temperature using thermoresponsive copolymers of 2‐(2‐methoxyethoxy) ethyl methacrylate and oligo(ethylene glycol) methacrylate (Mn = 475 g mol−1) as the macro‐RAFT agent. Kinetic studies confirm that quantitative monomer conversion is achieved within 15 min of visible‐light irradiation (405 nm, 0.5 mW cm−2), and good control is maintained during the polymerization. The polymerization can be temporally controlled by a simple “ON/OFF” switch of the light source. Finally, thermoresponsive diblock copolymer nano‐objects with a diverse set of complex morphologies (spheres, worms, and vesicles) are prepared using this particular formulation.
Hybrids with a silica network covalently bonded to a polymer are promising materials for bone repair. Previous work on synthesizing methyl methacrylate (MMA) based copolymers by reversible addition‐fragmentation chain transfer (RAFT) polymerization gives high tailorability of mechanical properties since sophisticated polymer structures can be designed. However, more flexible hybrids would be beneficial. Here, n‐butyl methacrylate (BMA) and methyl acrylate (MA) based hybrids are produced. Unlike MMA, BMA and MA hybrids do not show plastic deformation, and BMA hybrid has strain to failure of 33%. Although the new hybrids are more flexible, preosteoblast cells do not adhere on their surfaces, due to higher hydrophobicity and lower stiffness. Comonomer choice is crucial for bone regenerative hybrids.
Well‐defined poly[pentafluorophenyl (meth)acrylate] (PPFP(M)A) homopolymers are prepared by RAFT radical polymerization mediated by a novel chain transfer agent containing two cholesteryl groups in the R‐group fragment. Subsequent reaction with a series of small‐molecule amines in the presence of an appropriate Michael acceptor for ω‐group end‐capping yields a library of novel bischolesteryl functional hydrophilic homopolymers. Two examples of statistical copolymers are also prepared including a biologically relevant sugar derivative. Specific examples of these homopolymers are examined with respect to their ability to self assemble in aqueous media—a process driven entirely by the cholesteryl end groups. In all instances evaluated, and under the preparation conditions examined, the homopolymers aggregate clearly forming polymersomes spanning an impressive size range.
Carboxyl end‐functionalized poly[poly(ethylene glycol) methyl ether methacrylate] [P(PEGMEMA)] and its block copolymer with gemcitabine substituted poly(N‐hydroxysuccinimide methacrylate) [PGem‐block‐P(PEGMEMA)] are synthesized via reversible addition‐fragmentation transfer (RAFT) polymerization. Then, two polymers are grafted onto the surface of amine‐functionalized nanodiamonds to obtain [P(PEGMEMA)]‐grafted nanodiamonds (ND‐PEG) and [PGem‐block‐P(PEGMEMA)]‐grafted nanodiamonds (ND‐PF). Gemcitabine is physically absorbed to ND‐PEG to produce ND‐PEG (Gem). Two polymer‐grafted nanodiamonds (i.e., with physically absorbed gemcitabine ND‐PEG (Gem) and with chemically conjugated gemcitabine ND‐PF) are characterized using attenuated total reflectance infrared spectroscopy, dynamic light scattering, and thermogravimetric analysis. The drug release, cytotoxicity (to seed human pancreatic carcinoma AsPC‐1 cells), and cellular uptake of ND‐PEG (Gem) and ND‐PF are also investigated.
Under the validity of the degenerative transfer mechanism, the activation/deactivation process in reversible addition‐fragmentation chain transfer (RAFT) polymerization can be formally quantified by transfer coefficients, depending on the chemical structure of the participating radicals and dormant species. In the present work, the different literature methods to experimentally determine these RAFT transfer coefficients are reviewed and theoretically re‐evaluated. The accuracy of each method is mapped for a broad range of reaction conditions and RAFT transfer reactivities. General guidelines on when which method should be applied are formulated.
