Y‐shaped poly(ethylene glycol) and poly(trimethylene carbonate) amphiphilic copolymer: Synthesis and for drug delivery

New Y‐shaped (AB₂‐type) amphiphilic copolymers of poly(ethylene glycol) (PEG) with poly(trimethylene carbonate) (PTMC), PEG‐b‐(PTMC)₂, were successfully synthesized by the ring‐opening polymerization (ROP) of TMC with bishydroxy‐modified monomethoxy‐PEG (mPEG). First, a bishydroxy functional ROP initiator was synthesized by esterification of acryloyl bromide with mPEG, followed by Michael addition using excess diethanolamine. A series of Y‐shaped amphiphilic PEG‐(PTMC)₂ block copolymers were obtained via ROP of TMC using this PEG with bishydroxyl end groups as macroinitiator and ZnEt₂ as catalyst. The amphiphilic block copolymers with different compositions were characterized by gel permeation chromatography (GPC) and ¹H NMR, and their molecular weight was measured by GPC. The results showed that the molecular weight of Y‐shaped copolymers increased with the increase of the molar ratio of TMC to mPEG‐(OH)₂ initiator in feed while the PEG chain length was kept constant. The Y‐shaped copolymer mPEG‐(PTMC)₂ could self‐assemble into micelles in aqueous medium and the critical micelle concentration values of the micelles decrease with increase in hydrophobic PTMC block length of mPEG‐(PTMC)₂. The in vitro cytotoxicity and controlled drug release properties of the Y‐shaped amphiphilic block copolymers were also investigated. © 2008 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 46: 8131–8140, 2008     

Effect of dicationic gemini surfactants 16–s‐16 (s = 4, 5, 6) on the ninhydrin‐dipeptide (glycyl‐tyrosine) reaction

The effect of dicationic gemini surfactants H₃₃C₁₆(CH₃)₂N⁺‐(CH₂)_s‐N⁺(CH₃)₂ C₁₆H₃₃, 2Br^? (s= 4, 5, 6) on the reaction of a dipeptide glycyl–tyrosine (Gly–Tyr) with ninhydrin has been studied spectrophotometrically at 70°C and pH 5.0. The reaction follows first‐ and fractional‐order kinetics, respectively, in [Gly–Tyr] and [ninhydrin]. The gemini surfactant micellar media are comparatively more effective than their single chain–single head counterpart cetyltrimethylammonium bromide (CTAB) micelles. Whereas typical rate constant (k_Ψ) increase and leveling‐off regions, just like CTAB, are observed with geminis, the latter produces a third region of increasing k_Ψ at higher concentrations. This subsequent increase is ascribed to the change in the micellar morphology of the geminis. The pseudophase model of micelles was used to quantitatively analyze the k_Ψ ? [gemini] data, wherein the micellar‐binding constants K_S for [Gly–Tyr] and K_N for ninhydrin were evaluated. © 2012 Wiley Periodicals, Inc. Int J Chem Kinet 44: 800–809, 2012     

Synthesis and pH‐responsive assembly of methoxy poly(ethylene glycol)‐b‐poly(ε‐caprolactone) with pendant carboxyl groups

pH‐responsive methoxy poly(ethylene glycol)‐b‐poly(ε‐caprolactone) bearing pendant carboxyl groups mPEG‐b‐P(2‐CCL‐co‐6‐CCL) was synthesized based on our newly monomer benzyloxycarbonylmethly functionalized ε‐caprolactone. Their structure was confirmed by ¹H NMR, ¹³C NMR, and Fourier transform infrared spectrum spectra. In addition, SEC results indicated that the copolymers had a relatively narrow polydispersity. WXRD and DSC demonstrated that the introduction of carboxymethyl groups had significant effect on the crystallinity of the copolymers. Furthermore, the solution behavior of mPEG‐b‐P(2‐CCL‐co‐6‐CCL) has been studied by various methods. The results indicated that mPEG‐b‐P(2‐CCL‐co‐6‐CCL) had a rich pH‐responsive behavior and the micelles could be formed by pH induction, and the mPEG‐b‐P(2‐CCL‐co‐6‐CCL) could existed as unimers, micelles or large aggregates in different pH range accordingly. The mechanism of which was supposed to depend on the counteraction between the hydrophobic interaction from PCL and the ionization of the carboxyl groups along the polymer chain. Moreover, the mPEG‐b‐P(2‐CCL‐co‐6‐CCL) copolymers displayed good biocompatibility according to the preliminary cytotoxicity study. © 2013 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2014 , 52, 188–199     

Lactic acid‐ and carbonate‐based crosslinked polymeric micelles for drug delivery

Our objective was to synthesize and evaluate lactic acid‐ and carbonate‐based biodegradable core‐ and core‐corona crosslinkable copolymers for anticancer drug delivery. Methoxy poly(ethylene glycol)‐b‐poly(carbonate‐co‐lactide‐co‐5‐methyl‐5‐allyloxycarbonyl‐1,3‐dioxane‐2‐one) [mPEG‐b‐P(CB‐co‐LA‐co‐MAC)] and methoxy poly(ethylene glycol)‐b‐poly(acryloyl carbonate)‐b‐poly(carbonate‐co‐lactide) [mPEG‐b‐PMAC‐b‐P(CB‐co‐LA)] copolymers were synthesized by ring‐opening polymerization of LA, CB, and MAC using mPEG as an macroinitiator and 1,8‐diazabicycloundec‐7‐ene as a catalyst. These amphiphilic copolymers which exhibited low polydispersity and critical micelle concentration values (0.8–1 mg/L) were used to prepare micelles with or without drug and stabilized by crosslinking via radical polymerization of double bonds introduced in the core and interface to improve stability. mPEG₁₁₄‐b‐P(CB₈‐co‐LA₃₅‐co‐MAC_2.5) had a higher drug encapsulation efficiency (78.72% ± 0.15%) compared to mPEG₁₁₄‐b‐PMAC_2.5‐b‐P(CB₉‐co‐LA₃₉) (20.29% ± 0.11%).¹H NMR and IR spectroscopy confirmed successful crosslinking (～70%) while light scattering and transmission electron microscopy were used to determine micelle size and morphology. Crosslinked micelles demonstrated enhanced stability against extensive dilution with aqueous solvents and in the presence of physiological simulating serum concentration. Furthermore, bicalutamide‐loaded crosslinked micelles were more potent compared to non‐crosslinked micelles in inhibiting LNCaP cell proliferation irrespective of polymer type. Finally, these results suggest crosslinked micelles to be promising drug delivery vehicles for chemotherapy. © 2012 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2013     

Amphiphilic diblock copolymers bearing pendant aromatic acetal groups: Synthesis and tunable pH‐triggered assembly/disassembly transition behavior

A novel aromatic acetal‐based acid‐labile monomer 2‐phenyl‐5‐ethyl‐5‐acryloxymethyl‐1,3‐dioxacyclohexane (HEDPA) was synthesized and polymerized by reversible addition fragmentation chain transfer (RAFT) polymerization using alkynyl functional chain transfer agent (CTA‐Alk). Afterward, a series of amphiphilic diblock copolymers composed of fixed hydrophobic poly(2‐phenyl‐5‐ethyl‐5‐acryloxymethyl‐1,3‐dioxacyclohexane) (PDAEP) segments and various lengths of hydrophilic mPEG segments were prepared through click reaction between alkynyl‐terminated PDAEP and azido‐terminated mPEG. The self‐assembly behaviors of the diblock copolymers were investigated by dynamic light scattering (DLS), transmission electron microscopy (TEM), fluorescence spectroscopy, and ¹H NMR. These results indicated that the diblock copolymers could self‐assemble into nano‐sized micelles with PDAEP cores and PEG coronas in aqueous solution. DLS, fluorescence spectroscopy and UV–vis spectroscopy were used to monitor the pH‐triggered assembly/disassembly transition of the micelles. These results showed that the assembly/disassembly transition behaviors of the diblock copolymers micelles can be adjusted by changing the lengths of the mPEG segments. © 2015 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2016 , 54, 1537–1547     

Biodegradable and thermosensitive micelles of amphiphilic polyaspartamide derivatives containing aromatic groups for drug delivery

The preparation, characterization, release, and in vitro cytotoxicity of a biodegradable polymeric micellar formulation of paclictaxel (PTX) were investigated. The micelles based on thermosensitive and degradable amphiphilic polyaspartamide derivatives containing pendant aromatic structures (phe‐g‐PHPA‐g‐mPEG) were prepared by a quick heating method without using toxic organic solvent. Dynamic light‐scattering results show that the micelles are stable upon dilution under physiological conditions and the destabilization of the micelles is pH‐dependent and the phe‐g‐PHPA‐g‐mPEG polymers are biodegradable. PTX was loaded into the phe‐g‐PHPAs‐g‐mPEG micelles with encapsulation efficiency of >90%, resulting in a high drug loading content (up to 29%). PTX‐loaded micelles had a mean size around 70 nm with narrow size distribution (polydispersity index, <0.1). The PTX‐loaded micelles showed sustained drug release and obvious anticancer activity similar to Taxol against HepG2 cells, whereas blank micelles were nontoxic. The present results suggest that the thermosensitive and biodegradable phe‐g‐PHPA‐g‐mPEG micelles are a promising delivery system for the hydrophobic drugs. © 2013 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2013 , 51, 3917–3924     

ESR Studies on the Micellization Behaviors of a Series of Novel Asymmetric Gemini Surfactants

ＩｎｔｒｏｄｕｃｔｉｏｎＩｎｒｅｃｅｎｔｙｅａｒｓ ,ｂｉｓ(ｑｕａｔｅｒｎａｒｙａｍｍｏｎｉｕｍ)ｓｕｒｆａｃ ｔａｎｔｓｏｒｇｅｍｉｎｉｓｕｒｆａｃｔａｎｔｓ ,ｉｎｗｈｉｃｈｔｗｏｃａｔｉｏｎｉｃｓｕｒｆａｃ ｔａｎｔｍｏｉｅｔｉｅｓａｒｅｃｏｎｎｅｃｔｅｄｗｉｔｈｔｈｅａｍｍｏｎｉｕｍｈｅａｄｇｒｏｕｐｂｙａｐｌｏｙｍｅｔｈｙｌｅｎｅｃｈａｉｎ ,ｎａｍｅｌｙ ,ａｓｐａｃｅｒｈａｖｅｂｅｃｏｍｅｏｆｉｎｔｅｒｅｓｔｄｕｅｔｏｔｈｅｉｒｅｘｃｅｐｔｉｏｎａｌｓｕｒｆａｃｅａｃｔｉｖｉｔｙａｎｄｒｅｍ…     

Thermosensitive and photocleavable polyaspartamide derivatives for drug delivery

The development of novel thermo‐ and photo‐dual‐responsive biodegradable polymeric micelles based on amphiphilic polyaspartamide derivatives (NB‐g‐PHPA‐g‐mPEG) for anticancer drug delivery is reported. The obtained polymers containing hydrophobic photocleavable o‐nitrobenzyl groups exhibit thermo‐ and photosensitivity. The micelles and paclitaxel‐loaded micelles based on the thermo‐ and photo‐dual‐sensitive polymers were prepared by a quick heating method without using toxic organic solvent. The paclitaxel release from the drug‐loaded micelles can be triggered under photoirradiation. Enhancement of the anticancer activity against HeLa cells was observed for paclitaxel‐loaded NB‐g‐PHPA‐g‐mPEG micelles after light irradiation, while the empty NB‐g‐PHPA‐g‐mPEG micelles with or without irradiation did not show any toxicity. Therefore, the thermo‐ and photo‐dual‐responsive NB‐g‐PHPA‐g‐mPEG micelles have a promising future applied as a light controlled drug delivery system for anticancer drugs. © 2016 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2016 , 54, 2855–2863     

疏水相互作用引起Gemini表面活性剂柔性联接链的弯曲

为了理解gemini表面活性剂柔性烷基联接链在自组织过程中的特殊作用,我们合成了三种gemini表面活性剂烷基-a,w-二（二-十二烷基甲基溴化铵）（记为2C12-s-2C12×2Br (s=3, 6, 8)）。2C12-s-2C12×2Br在水表面构成铺展膜后,由于每个分子带有4根烷烃链,它们形成了稠密的烷烃尾链层。增强的烷烃尾链与联接链间的疏水相互作用促使联接链弯曲朝向空气一端,可发生弯曲的联接链长度要小于吸附在水溶液表面上的gemini表面活性剂C12-s-C12×2Br,后者每个分子只有2根烷烃链。由此可见,增强的烷烃尾链与联接链间的疏水相互作用可以有效地促进联接链的弯曲。     

Photo‐responsive amphiphilic poly(α‐hydroxy acids) with pendent o‐nitrobenzyl ester constructed via copper‐catalyzed azide‐alkyne cycloaddition reaction

Photo‐responsive block copolymer mPEG‐b‐poly(Tyr)‐g‐NB was prepared by introduction of o‐nitrobenzyl ester group into the side chain of amphiphilic poly(ethylene glycol)‐b‐poly(α‐hydroxy acids) (mPEG‐b‐poly(Tyr)) containing pendent alkynyl group via copper‐catalyzed azide‐alkyne cycloaddition reaction. The amphiphilic mPEG‐b‐poly(Tyr) was synthesized via the ring‐opening polymerization of O‐carboxyanhydrides, with monomethoxy poly(ethylene glycol) (mPEG) as macroinitiator. The molecular structure, self‐assembly, and photo‐controlled release of the obtained mPEG‐b‐poly(Tyr)‐g‐NB were thoroughly investigated. mPEG‐b‐poly(Tyr)‐g‐NB could self‐assemble into spherical micelles in water and showed disassembly under UV light irradiation, which was demonstrated by means of UV‐vis spectroscopy, scan electron microscopes, and dynamic light scattering measurement. Fluorescence emission measurements demonstrated that Nile red, encapsulated by micelles, can be released upon UV irradiation. This study provides a convenient way to construct smart poly(α‐hydroxy acids)‐based nanocarriers for controlled release of hydrophobic drugs. Copyright © 2015 John Wiley & Sons, Ltd.     

Formation of polymeric micelles with amino surfaces from amphiphilic AB‐type diblock copolymers composed of poly(glycolic acid lysine) segments and polylactide segments

Amphiphilic AB‐type diblock copolymers composed of hydrophobic poly(L ‐lactide) (PLA) segments and hydrophilic poly(glycolic acid lysine) [poly(Glc‐Lys)] segments with amino side‐chain groups self‐associated to form PLA‐based polymeric micelles with amino surfaces in an aqueous solution. The average diameter of the loose core–shell polymeric micelles for poly(Glc‐Lys) [number‐average molecular weight (M_n) = 1240]‐b‐PLA (M_n = 7000) obtained by a dimethyl sulfoxide/water dialysis method was estimated to be about 50 nm in water by dynamic light scattering measurements. The size and shape of the obtained polymeric micelles were further observed with transmission electron microscopy and atomic force microscopy. To investigate the possibility of applying the obtained PLA‐based polymeric micelles as bioabsorbable vehicles for hydrophobic drugs, we tested the entrapment of drugs in poly(Glc‐Lys) (M_n = 1240)‐b‐PLA (M_n = 7000) micelles and their release with doxorubicin as a hydrophobic drug. © 2002 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 40: 1426–1432, 2002     

Wormlike Micelle Formation and Rheological Behavior in the Aqueous Solutions of Mixed Sulfate Gemini Surfactant without Spacer Group and Dodecyltrimethylammonium Bromide

The rheological behavior of the aqueous solutions of mixed sulfate gemini surfactant with no spacer group, referred to as d‐C₁₂S, and dodecyltrimethylammonium bromide (C₁₂TABr) at a total concentration of 100 mmol·L⁻¹ but different molar ratios of C₁₂TABr to d‐C₁₂S (α₁) was investigated using steady rate and frequency sweep measurements. The wormlike micelles were formed over a narrow α₁ range of 0.20–0.27. The viscoelastic solutions exhibited Maxwell fluid behavior. At the optimum molar ratio of 0.25, the zero‐shear viscosity was as high as 600 Pa·s and the length of the mixed wormlike micelle was about 0.45–0.85 µm. The present result provides an example to construct long wormlike micelles by anionic gemini surfactant.     

Small-angle neutron-scattering study and micellar model of the gemini (phenylenedimethylene)bis(n-octylammonium)dibromide surfactant micelles in water

The microstructure of the micelles formed in aqueous solution by gemini surfactants with aromatic spacers, [Br(CH₃)₂N⁺(C _m H_{2 m +1})-(Ph)-(C _m H_{2 m +1})N⁺(CH₃)₂Br, m=8 and Ph = o-, m- or p-phenylenedimethylene] has been examined by small-angle neutron scattering. Aggregation of the gemini surfactants with an o-phenylenedimethylene spacer brings about formation of premicelles and small micelles at concentrations below the second critical micelle concentration, while above this concentration marked micellar growth and variation in shape occurs. It is suggested that the minimum aggregate formed at this critical micelle concentration may be the trimer or tetramer and that this result supports the mechanism of “gemini → submicelle → assembly” for micellar growth. Received: 8 September 1998 Accepted in revised form: 27 November 1998     

Novel glucose derived non-ionic gemini surfactants as reverse micellar systems for encapsulation of d- and l-enantiomers of some aromatic α-amino acids in n-hexane

Novel glucose-based non-ionic gemini amphiphiles comprising two sugar head groups, two hydrophobic tails having chain length of C₁₂, C₁₄, and C₁₈ and a –CH₂–Ar–CH₂– spacer have been synthesized. The head groups of the geminis consist of glucose entities (with reducing function blocked in cyclic acetal group) connected through C-6 to tertiary amines. These amphiphiles were explored as reverse micellar systems, for the encapsulation of d- and l-enantiomers of ultraviolet-absorbing aromatic α-amino acids histidine (H), phenylalanine (F), tyrosine (Y) and tryptophan (W) in n-hexane, without any added water. Reverse micellar studies revealed that aromatic α-amino acids were encapsulated in the sequence H?>?F?>?Y?>?W. In most cases, specifically for F, d-enantiomer was found better encapsulated than l-enantiomer in the reverse micellar probes of the gemini surfactants.     

Photoresponsive biodegradable poly(carbonate)s with pendent o‐nitrobenzyl ester

Photoresponsive amphiphilic diblock poly(carbonate)s mPEG₁₁₃‐b‐PMNC_n with pendent o‐nitrobenzyl ester group were synthesized through ring‐opening polymerization (ROP) using 1,8‐diazabi‐cyclo[5.4.0]undec‐7‐ene (DBU) as catalyst and monomethoxy poly(ethylene glycol) (mPEG) as macroinitiator. In aqueous solution, the copolymers can self‐assemble to spherical micelles with a PC core and a PEG shell. The critical micelle concentration (CMC), size, and morphology of the micelles were demonstrated by means of fluorescence spectroscopy, transmission electron microscopes (TEM), and dynamic light scattering (DLS). Under UV light irradiation, the amphiphilic copolymer micelles disassembled because of the photocleavage of o‐NB ester, and the light‐controlled release behaviors of payload Nile red were further proved. This study provides a convenient way to construct smart poly(carbonate)s nanocarriers for controlled drug release. © 2017 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2017 , 55, 2770–2780     

Copolymerizations of ethylene and polar comonomers with bis(phenoxyketimine) group IV complexes: Effects of the central metal properties

With triisobutylaluminum as a protection reagent, copolymerizations of ethylene with 10‐undecen‐1‐ol, 10‐undecenoic acid, and 5‐hexen‐1‐ol have been performed with bis[(3,5‐di‐^tBu? C₆H₂? 2‐O)? PhC?N(2‐F? C₆H₄)]ZrCl₂ ( a )/methylaluminoxane or bis[(3,5‐di‐^tBu? C₆H₂? 2‐O)? PhC?N(2‐F? C₆H₄)]TiCl₂ ( b )/methylaluminoxane as the catalyst. Both catalysts exhibit high activities of copolymerization in the presence of polar groups. The properties of the copolymers are strongly affected by the central metal properties of the catalysts. In comparison with complex a , titanium complex b appears to be less sensitive to polar monomers and more favorable for the preparation of higher molecular weight functionalized polyethylenes containing higher contents of polar groups. Studies on the polymerization temperature indicate that the catalytic activities decrease greatly with both complex a and complex b . The comonomer contents incorporated into the copolymers are slightly dependent on the polymerization temperature in the case of complex a , whereas in the case of complex b , the effect of the polymerization temperature is more distinct: an increase in the polymerization temperature can efficiently facilitate the incorporation of polar comonomers. © 2006 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 45: 59–68, 2007     

Temperature and pH dual‐sensitive polyaspartamide derivatives for antitumor drug delivery

The pH‐sensitive tertiary amino groups were introduced to synthesize temperature and pH dual‐sensitive degradable polyaspartamide derivatives (phe/DEAE‐g‐PHPA) containing pendant aromatic structures and ionizable tertiary amino groups. The thermo/pH‐responsive behavior of phe/DEAE‐g‐PHPA polymer can be tuned by adjusting the graft copolymer composition. Due to the pH sensitivity of the phe/DEAE‐g‐PHPA‐g‐mPEG polymer with hydrophilic long PEG chain, the micelles and the anticancer drug‐loaded micelles were prepared by a quick pH‐changing method without using toxic organic solvent. The obtained polymeric micelles, paclitaxel‐loaded micelles and doxorubicin‐loaded micelles were stable under physiological conditions. Both the drug‐loaded micelles showed much faster release at pH 5 than at pH 7.4. The doxorubicin‐loaded micelles showed obvious and better anticancer activity against both HepG2 and HeLa cells than free doxorubicin. Thus these nontoxic, dual thermo‐ and pH‐sensitive phe/DEAE‐g‐PHPA‐g‐mPEG micelles may be a promising anticancer drug delivery system. © 2015 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2016 , 54, 879–888     

Aggregation‐Induced Emission Active Probe for Light‐Up Detection of Anionic Surfactants and Wash‐Free Bacterial Imaging

Anionic surfactants are widely used in daily life and industries, but their residues can cause serious damage to the environment. The current detection methods for anionic surfactants suffer from various limitations and a new detection strategy is highly desirable. Based on 2‐(2‐hydroxyphenyl)benzothiazole fluorogen with aggregation‐induced emission characteristics, we have developed a fluorescent probe HBT‐C₁₈ for selective and sensitive detection of anionic surfactants. By in situ formation of catanionic aggregates or micelles with anionic surfactants, the emission intensity of the HBT‐C₁₈ probe can increase with increasing keto/enol emission ratio through restriction of intramolecular motion and excited‐state intramolecular proton‐transfer mechanisms. The probe can also be used for wash‐free imaging of bacteria enveloped by a negatively charged outer membrane. The results of this study provide a new strategy for sensitive detection of anionic surfactants and wash‐free bacterial imaging.     

Effects of additional salts on the interfacial tension of crude oil/zwitterionic gemini surfactant solutions

Zwitterionic gemini surfactants, which have the advantages of both zwitterionic and gemini surfactants, have been widely used in various disciplines. Sulfobetaine-type zwitterionic gemini surfactants consisting of 1,2-bis[N-methyl-N-(3-sulfopropyl)-alkylammonium]ethane (2C_nSb with 6, 8 and 10 carbon atoms) were evaluated for their interfacial activities at the water/crude oil interface. The 2C₁₀Sb molecules showed a remarkable ability to decrease the interface tension (IFT) of water/crude oil, and the degree of decrease was much greater than those in either zwitterionic or gemini surfactant systems by at least two orders of magnitude. Furthermore, the effects of salts (NaCl, CaCl₂, and MgCl₂) on the IFT of the 2C₁₀Sb system were thoroughly investigated. Interestingly, the delicate balance between the effects of additional cations and the intramolecular interactions of 2C₁₀Sb molecules played crucial roles in the interfacial arrangements of 2C₁₀Sb molecules, which were mainly dependent on the bonding abilities of the cations. Moreover, a zwitterionic surfactant and a cationic gemini surfactant were employed in control experiments to verify the proposed mechanisms.     

pH‐ and β‐cyclodextrin‐responsive micelles based on polyaspartamide derivatives as drug carrier

A novel kind of graft polymer poly(aspartic acid)‐ethanediamine‐g‐adamantane/methyloxy polyethylene glycol (Pasp‐EDA‐g‐Ad/mPEG) was designed and synthesized for drug delivery in this study. The chemical structure of the prepared polymer was confirmed by proton NMR. The obtained polymer can self‐assemble into micelles which were stable under a physiological environment and displayed pH‐ and β‐cyclodextrin (β‐CD)‐responsive behaviors because of the acid‐labile benzoic imine linkage and hydrophobic adamantine groups in the side chains of the polymer. The doxorubicin (Dox)‐loaded micelles showed a slow release under physiological conditions and a rapid release after exposure to weakly acidic or β‐CD environment. The in vitro cytotoxicity results suggested that the polymer was good at biocompatibility and could remain Dox biologically active. Hence, the Pasp‐EDA‐g‐Ad/mPEG micelles may be applied as promising controlled drug delivery system for hydrophobic antitumor drugs. © 2015 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2015 , 53, 1387–1395