Hydrophobic Segments Research Articles

Mannose/stearyl chloride doubly functionalized polyethylenimine as a nucleic acid vaccine carrier to promote macrophage uptake

Transmembrane transport remains a significant challenge for nucleic acid vaccine vectors. Promoting the ability of immune cells, such as macrophages, to capture foreign stimuli is also an effective approach to improving cross-presentation. In addition, polyethyleneimine (PEI) has gained attention in the field of nucleic acid vaccine carriers due to its excellent gene transfection efficiency and unique proton buffering effect. However, although high molecular weight PEI exhibits high efficiency, its high-density positive charges make it highly toxic, which limits its application. In this study, mannose/stearyl chloride functionalized polyethylenimine (SA-Man-PEI) was prepared by functionalizing PEI (molecular weight of 25 kDa) with mannose with immunomodulatory and phagocyte targeting effects, and an alkyl hydrophobic chain segment, which could easily promote cell uptake. Moreover, the functionalized-PEI retains a strong proton buffering effect, which helps the carrier escape from the lysosome. The particle sizes of the composite particles formed by SA-Man-PEI and ovalbumin (OVA) were below 200 nm, with good storage stability at both 4 °C and 37 °C. At a drug concentration of 2 μg/mL, the cell survival rate of functionalized-PEI was 19.2% higher than that of unfunctionalized PEI. In vitro macrophage endocytosis experiments showed that SA-Man-PEI could significantly enhance the macrophage uptake of composite particles, compared to unfunctionalized PEI or single-functionalized PEI. This study offers a new approach for developing PEI as a nucleic acid vaccine carrier, which could simultaneously enhance cell targeting and promote cell uptake.

Anchorage of bacterial effector at plasma membrane via selective phosphatidic acid binding to modulate host cell signaling.

Binding phospholipid is a simple, yet flexible, strategy for anchorage of bacterial effectors at cell membrane to manipulate host signaling responses. Phosphatidylinositol 4-phosphate and phosphatidylinositol 4,5-biphosphate are the only two phospholipid species known to direct bacterial effectors to establish inner leaflet localization at the plasma membrane. Here, selectivity of phosphatidic acid (PA) by bacterial effectors for the plasma membrane anchorage and its molecular entity was identified. C-terminal BID domain of Bartonella T4SS effectors (Beps) directed the plasma membrane localization of Beps in host cells through binding with PA. A hydrophobic segment of the 'HOOK' subdomain from BID is inserted into the bilayer to enhance the interaction of positively charged residues with the lipid headgroups. Mutations of a conserved arginine facilitating the electrostatic interaction, a conserved glycine maintaining the stability of the PA binding groove, and hydrophobic residues determining membrane insertion, prevented the anchorage of Beps at the plasma membrane. Disassociation from plasma membrane to cytosol attenuated the BepC capacity to induce stress fiber formation and cell fragmentation in host cells. The substitution of alanine with aspartic acid at the -1 position preceding the conserved arginine residue hindered BepD anchoring at the plasma membrane, a vital prerequisite for its ability to elicit IL-10 secretion in host macrophages. In conclusion, our findings reveal the PA-binding properties of bacterial effectors to establish plasma membrane localization and will shed light on the intricate mechanisms employed by bacterial effectors within host cells.

Hierarchical Structures of Amino Acid Derived Polyhydroxyurethanes: Promising Candidates as Drug Carriers and Cell Adhesive Scaffolds.

In this study, we examined the self-assembly of a series of biodegradable and biocompatible amino acid-based polyhydroxyurethanes (PHUs), investigating the structural influence of these polymers on their self-assembly and the resulting morphological features. The presence of hydrophilic and hydrophobic segments, along with carbonyl urethane, ester, and hydroxyl groups in the PHU backbone, facilitates intermolecular hydrogen bonding, enabling the formation of self-assemblies with hierarchical nanodimensional morphologies. We determined the critical aggregation concentration (CAC) and found that it largely depends on the PHU's structure. In-depth morphological studies demonstrated that the evolution of morphology proceeds in four steps: (1) the initial formation of micelles, which act as seeds at very low concentrations, (2) the elongation of these micelles into nanorod or nanopalette shapes below the CAC range, (3) the epitaxial growth of nanofibers at the CAC, and (4) the complete formation of fibrous mats above the CAC. Additionally, these hierarchical structures were utilized for the encapsulation and release of the drug doxorubicin (DOX). We observed that 75% of the encapsulated DOX was readily released in a mildly acidic environment, similar to the physiological conditions of cancer cells. Cellular uptake studies confirmed the effective uptake of the drug-loaded nanoassemblies into the cytoplasm of cells. Our studies also confirmed that these self-assembled structures can serve as effective cell adhesive scaffolds for tissue engineering applications.

Experimental and Simulation Study of Single-matrix, All-polymeric Thin-film Composite Membranes for CO2 Capture: Block vs Random Copolymers

High-performance, additive-free, all-polymeric thin-film composite (TFC) membranes were developed for CO₂ capture, focusing on a comparison between block and random copolymers (referred to as PTF) composed of hydrophobic poly(2,2,2-trifluoroethyl methacrylate) (PTFEMA) and CO2-philic polar poly(oxyethylene methacrylate) (POEM) chains. The PTF random copolymer, synthesized via free-radical polymerization (FRP), exhibited a disordered morphology. In contrast, the PTF block copolymer, synthesized via reversible addition-fragmentation chain transfer (RAFT) polymerization, formed a well-ordered hexagonally packed cylindrical structure, creating an amphiphilic, microphase-separated nanostructure. Molecular dynamics (MD) simulations revealed that in both copolymers, there was minimal interaction between the gases (CO₂ and N₂) and the hydrophobic PTFEMA segments, while CO₂ showed strong affinity for the hydrophilic POEM segments. The block and random copolymers demonstrated similar CO₂ permeance, which can be attributed to their comparable CO₂ diffusivity and solubility. However, the block copolymer exhibited significantly lower N₂ permeance than the random copolymer, resulting in nearly quadruple the CO₂/N₂ selectivity. This increase in selectivity was supported by the lower N₂ mean squared displacement (indicating reduced diffusivity) observed in the block copolymer. The PTF block copolymer outperformed the commercial Pebax block copolymer, achieving CO₂ capture efficiencies that surpass industrial standards for CO₂ separation and capture. This positions the single-matrix PTF block copolymer as a promising alternative to mixed-matrix membranes for practical applications in gas separation technologies.

Promoted lignocellulose fractionation and improved enzymatic hydrolysis of corn stalks through cationic surfactant combined with deep eutectic solvent pretreatment

The efficient conversion of lignocellulose relies on the implementation of an effective pretreatment strategy. Cationic surfactants combined with deep eutectic solvent ([Betaine][LA] was employed as a novel pretreatment strategy for treating corn stalks. Valuable insights were provided on the impact of the surfactant hydrophobic segment length on pretreatment efficacy. The specific pretreatment conditions were optimized by single factor and orthogonal experiment. Octadecyl trimethyl ammonium bromide (OTAB, 1.5 wt%) with the longest hydrophobic part combined with [Betaine][LA] (Betaine-to-LA molar ratio 1:4) achieved the best pretreatment effect (delignification 92.8 %, xylan elimination 91.1 %) when severity factor reached 4.26, meanwhile, 1.7 g/L xylo-oligosaccharides and 4.4 g/L furfural were detected in pretreatment liquid due to the hydrolysis of hemicellulose in corn stalks with acidic deep eutectic solvent [Betaine][LA]. The relative saccharification activity reached 2.7 times of raw material, while the lignin surface area significantly decreased, leading to enhanced cellulose accessibility. Additionally, molecular perspective provided by molecular dynamics showed the elimination of lignin and xylan was facilitated by strong interaction of hydrogen-bond and van der Waals force between lignin and hemicellulose with [Betaine][LA] + OTAB. Overall, the effectiveness and potential of cationic surfactant combined deep eutectic solvent pretreatment strategy for lignocellulose pretreatment was revealed.

Controlled Distribution of MXene on the Pore Walls of Polyarylene Ether Nitrile Porous Films for Absorption-Dominated Electromagnetic Interference Shielding Materials.

With the increasing application of electronic devices, absorption-dominated electromagnetic interference shielding materials (EMISM) have garnered significant attention for preventing secondary electromagnetic pollution. In this study, polyethyleneimine (PEI)-modified MXene (PEI@MXene) is fabricated and achieved its controlled distribution on the pore walls of polyarylene ether nitrile (PEN) porous films via the phase inversion method (PIM) to obtain a closed porous skeleton of MXene on the pore walls (CPS-MPW). The resulting PEI@MXene/PEN composite film (CFx) exhibited absorption-dominated EMIS efficiency (EMISE). Attributing to the strong interaction between PEI and the hydrophilic segment of amphiphilic Pluronic F127, with its hydrophobic segment anchored by the PEN matrix, PEI@MXene is directionally distributed on the pore walls of CFx. In addition, resulting from the cladding of MXene with PEI and isolating it with closed honeycomb pores, the obtained CFx are insulators without forming aconductive network. As a result, these CFx demonstrate absorption-dominated EMISE with the highest SET of 41.2 dB and coefficient A higher than 0.51. Further continuous hot pressing of CFx results in thinner and denser films with an impressive specific EMISE up to 750 dBcm-1. The successful fabrication of these CPS-MPW-type CFx with absorption-dominated EMISE provides a reference for developing and preparing novel EMISM.

Underwater Structurally‐Colored Adhesives for Visualized Adhesion Monitoring in Aqueous Media

AbstractAssessment of the local strain/stress changes of adhesives is highly desirable for their service to avoid premature failure. However, monitoring local strain/stress variations in adhesives in practical settings remains challenging, especially in aqueous media. Here, an underwater structurally‐colored adhesive for visualized local strain/stress monitoring in aqueous media is reported. The structurally‐colored adhesive is obtained by shearing composites of poly(butyl acrylate‐co‐acrylic acid) copolymer and carboxylated polystyrene colloidal particles. The resultant structurally‐colored adhesive exhibits underwater adhesive strength (i.e., 238 kPa for stainless steel substrates) to various substrates (e.g., metals and plastics) thanks to hydrophobic segments and carboxyl groups. Notably, they can shift color in response to external force, enabling real‐time visual monitoring of localized strain/stress changes. As a proof of concept, the structurally‐colored adhesive can be used to seal a leaking hole on a bottle or tube, and it can precisely visualize the localized pressure distribution, providing critical information on the adhesion performance and the local pressure. These distinctive properties make the structurally‐colored adhesive suitable for application in wet environments as a real‐time visual pressure tracking device.

Waterborne Polyurethane Micelles Reinforce PEO-Based Electrolytes for Lithium Metal Batteries.

Although solid polymer electrolytes have been developed for several decades, poly(ethylene oxide) (PEO) or polymers with ethoxy (EO) segments are still one of the most promising candidates for advanced batteries. The low ionic conductivity and lithium-iontransference number as well as the deterioration of mechanical properties after coupling with lithium salts restrict its further adoption. Herein, a serial of PEO-based composite electrolytes optimized by waterborne polyurethane are prepared via blend method. With the assistance of H2O, ionic type waterborne polyurethane assembles into flexible micelles, in which hydrophobic segments as the core and hydrophilic groups as the shell. Utilizing this feature of waterborne polyurethane, PEO and Li salt (LiTFSI) aqueous solution is slowly added to the organic solution of waterborne polyurethane to compoundin situ, and polymer composite electrolytes are fabricated. The multilevel (hydrogen bonds with different binding energy) and multiscale (deformation of flexible micelles) dynamic interaction endows the composite electrolyte with attractive mechanical properties. The assembled Li|Li symmetric battery with the molar ratio of EO to Li salts of 8:1 exhibits excellent cycling stability up to 800 h at 0.1 mA cm-2, and the assembled Li|LiFePO4battery can be stably cycled at 1C for >400 cycles.

Stabilized Cell Membrane-Derived Vesicles by Lipid Anchoring for Enhanced Drug Delivery.

A cell membrane-derived vesicle (MV) that has cell-mimicking features with characteristic functionalities holds vast appeal for biomimetic nanomedicine and drug delivery but suffers from a major limitation of innate fragility and poor stability. Herein, we report a lipid-anchoring strategy for stabilizing MV for enhanced drug delivery. An array of amphiphilic mono-acyl phosphatidylcholines (MPCs) with specific hydrophobic moieties are synthesized and readily engineered on MV based on their commendable aqueous solubility and efficient membrane insertability. Incorporation of MPCs containing rigid ring structures in the hydrophobic segment demonstrates the potency of stabilizing MV by the combined ordering and condensing effects. The optimized MPC-stabilized MV exhibits prolonged circulation in the bloodstream, elevated accumulation within a tumor, and enhanced therapeutic effects of chemotherapeutic and photothermal drugs. Moreover, doxorubicin-loaded MV, engineered with mono-all-trans retinoyl phosphatidylcholine as an MV stabilizer and a therapeutic prodrug, potently suppresses growth and metastasis of high-stemness tumors.

Synergizing autophagic cell death and oxaliplatin-induced immunogenic death by a self-delivery micelle for enhanced tumor immunotherapy

Chemotherapy has become an emerging strategy to activate cytotoxic T cell responses by inducing immunogenic cell death (ICD), but the level of antitumor immunity induced by chemotherapeutic agents, such as oxaliplatin (OXA), is limited due to inadequate tumor antigen presentation and T cell activation. Inducing autophagic cell death (ACD) promotes the release of tumor antigen and the recruitment of dendritic cells, therefore strengthening antitumor immune responses. Here we simultaneously activate ICD and ACD with tumor targeting micelle to achieve enhanced antitumor chemo-immunotherapy. A self-delivery micelle is formulated by conjugating OXA prodrug with tocopherol succinate (TOS) as a hydrophobic segment and further encapsulates autophagy activator SMER28 to afford TOPR/SMER28, which specifically targets αvβ3 on tumor cells with c(RGDfK). Upon cellular internalization, OXA is released from the prodrug in response to the high concentration of reduced glutathione (GSH) in tumor cells, triggering ICD and releasing associated molecular patterns (DAMPs) signaling molecules to stimulate immunity. Meanwhile, SMER28 over-activates autophagy to induce autophagic cell death, which further leads to the maturation of dendritic cells and ultimately activates anti-tumor immune response. In the 4T1 tumor-bearing mice, the combination of OXA and SMER28 effectively inhibits tumor growth and activates antitumor immune responses. The tumor targeted micelle releases OXA and SMER28 in an on-demand profile and strengthens tumor chemo-immunotherapy by synergizing ICD and ACD, providing an alternative for antitumor immunotherapy. Statement of significanceChemotherapy induces immunogenic cell death (ICD) to activate anti-tumor immunity. However, the efficacy is limited by low levels of antigen presentation and T cell activation. To strengthen the antitumor immune responses induced by ICD, we first combine autophagic cell death (ACD) with ICD by formulating a glutathione-responsive oxaliplatin prodrug micelle co-encapsulating the autophagy activator SMER28. The activated autophagic level by SMER28 enhances the release of antigen and the recruitment of APCs, and ultimately bolsters T cell-mediated antitumor immune responses. We provide a potential strategy to amplify antitumor immune effects by combining autophagy activation with chemotherapy.

Inertial migration of cylindrical micelles formed by comb-like copolymer in Poiseuille flow

By combining the lattice Boltzmann model of fluid flow with the molecular dynamics model of copolymers, we investigate the inertial migration of cylindrical micelles, which is obtained by controlling the length ratios of hydrophilic and hydrophobic segments in a comb-like copolymer. Our results demonstrate that cylindrical micelles gradually deviate from the center of the nanochannel with increasing Reynolds number (Re). For the same Re, the larger the cylindrical micelle is, the closer it is to the center of the nanochannel. Importantly, we find that the change in the equilibrium position is particularly pronounced at Re less than 0.1, while the trend becomes smoother at Re greater than 0.1, which is because of the transition of micelles from cylindrical to disk-like shapes when Re is smaller than 0.1, and does not change as Re further increases. This work provides an understanding of cylindrical micelles' inertial migration, particularly in identifying the effect of morphological changes on the equilibrium position, which could lead to significant advancements in the inertial migration of polymer micelles.

Self-healing Hydrophobic Antifouling Polymers with Fe3+-Catechol Coordination Interaction.

Hydrophobic antifouling polymers capable of self-healing performance are highly desirable for industrial applications. However, the construction of self-healing, hydrophobic antifouling polymers is challenging considering their complex fouling environments, which are humid in aqueous environment. In this work, a self-healing hydrophobic polymer containing Fe3+-catechol coordination applicable to antifouling is synthesized. The hydrophobic fluoroalkyl segments in the polymers formed unique domains dispersed in a polydimethylsiloxane matrix. The as-synthesized polymers can completely restore their tensile strength, and their self-healing efficiency is above 90% in both artificial seawater and pure water because of the dynamic Fe3+-catechol coordination interactions. The as-synthesized polymer exhibited self-healing and antifouling properties against common marine bacteria. The colony adhesion and self-healing processes of the damaged coating in artificial seawater containing marine bacteria are characterized by laser confocal microscopy. This strategy may be useful for the development of future polymeric antifouling materials.

Amphiphilic diblock copolymers of polyisobutylene-b-poly(2-ethyl-2-oxazoline) via cationic polymerization

A series of amphiphilic polyisobutylene-b-poly (2-ethyl-2-oxazoline) (PIB-b-PEOX) diblock copolymer/Ag nanoparticle composites were successfully in-situ synthesized via cationic ring-opening polymerization of 2-ethyl-2-oxazoline (EOX) with high initiation efficiency by using allyl bromide end functionalized polyisobutylene (PIB-allylBr) as a macroinitiator and AgClO4 as a coinitiator. The microphase separation formed in the resulting PIB-b-PEOX diblock copolymers due to the thermodynamic imcompability of hydrophilic PEOX segments and hydrophobic PIB segments. The micromorphology of phase separation is dependent on the copolymer composition, in which sea-island micromorphology formed for PIB118-b-PEOX80 and bicontinuous phase micromorphology formed for PIB118-b-PEOX97. The micelles with nano-scale size in the range of 15–80 nm and having high drug loading rate of ca. 48.9 % can be formed by self-assembly of the amphiphilic diblock copolymers in n-hexane. The drug cumulative release rate can be increased with an increase in the proportion of PEOX segments, due to the strong interaction between ibuprofen and the PEOX segments. The hydrophilicity of the PIB-b-PEOX diblock copolymer surfaces can be improved after ethanol vapor induction. The PIB-b-PEOX diblock copolymers behave biocompatibility and good anti-protein adsorption property. The amphiphilic PIB-b-PEOX diblock copolymer/Ag nanoparticle composites exhibit high antibacterial efficiency for Gram-negative bacterium (E. coli) and Gram-positive bacterium (S. aureus). To the best of our knowledge, this is the first example of PIB-b-PEOX diblock copolymer/Ag nanoparticle (6.4 ± 2.6 nm) composites synthesized in-situ with good biocompatibility, anti-protein adsorption, and antibacterial properties, which would have potential applications for drug delivery and anti-protein coating in biomedical areas.

Assembly Regulates Gamma Radiation Polymerization of Polytelluoxane.

Regulating chemical drug's responsiveness to gamma radiation is crucial for achieving better therapeutic effects in cancer treatment. Most research focused on thermodynamic chemical structure design, while little attention was paid to kinetic regulate strategy, which possesses greater universality and security. In this study, we achieved a kinetic-based regulate strategy of gamma radiation reaction, through the construction of microphase environment during polymerization of polytelluoxane (PTeO). We designed hydrophobic segments forming large compound micelles (LCMs) assembly to create kinetically favorable higher concentration for radiation-induced reaction. It exhibited a > ten times higher responsiveness and, as far as we know, merely required a minimum dosage of 5 Gy for polymerization to occur. What's more, by taking advantages of the assembly change with Te-O hydrophilic segments and gamma radiation, polymerization became milder with lower polydispersity than previous methods. Such kinetic-based regulate strategy could offer a novel perspective on the design of radiation-responsive chemoradiotherapy and other radiation-induced chemical process.

Assembly Regulates Gamma Radiation Polymerization of Polytelluoxane

Regulating chemical drug's responsiveness to gamma radiation is crucial for achieving better therapeutic effects in cancer treatment. Most research focused on thermodynamic chemical structure design, while little attention was paid to kinetic regulate strategy, which possesses greater universality and security. In this study, we achieved a kinetic‐based regulate strategy of gamma radiation reaction, through the construction of microphase environment during polymerization of polytelluoxane (PTeO). We designed hydrophobic segments forming large compound micelles (LCMs) assembly to create kinetically favorable higher concentration for radiation‐induced reaction. It exhibited a > ten times higher responsiveness and, as far as we know, merely required a minimum dosage of 5 Gy for polymerization to occur. What’s more, by taking advantages of the assembly change with Te‐O hydrophilic segments and gamma radiation, polymerization became milder with lower polydispersity than previous methods. Such kinetic‐based regulate strategy could offer a novel perspective on the design of radiation‐responsive chemoradiotherapy and other radiation‐induced chemical process.

PH-Induced color changeable AIE-featured polymeric micelles for self-indicating anticancer drug delivery

Multifunctional polymeric micelles, which possess capabilities for tracking, bioimaging, stimuli-responsive drug release and tumor targeting, are essential in facilitating the effective delivery of anticancer drugs. Hence, a novel copolymer (CD-CS-Bio-TPAA, CCBT) was synthesized with biotin and hydroxypropyl-β-cyclodextrin conjugated chitosan as the hydrophilic segment and aggregation-induced emission (AIE) featured tetraphenylethene derivative (TPAA) as the hydrophobic segment. Interestingly, under acidic conditions, CCBT exhibited color-tunable AIE behavior as a result of the cleavage of benzoic imine bonds in TPAA molecules, transitioning from red to yellow. Furthermore, CCBT could also self-assemble into polymeric micelles and be used as drug carriers to encapsulate paclitaxel (PTX) (PTX/CCBT PMs) for self-indicating cancer therapy. In vitro release experiments demonstrated that PTX/CCBT PMs could release drugs specifically under acidic conditions. Fluorescence imaging experiments demonstrated that CCBT PMs exhibited excellent cell imaging capabilities and could be tracked due to their unique color-changing behavior. Moreover, PTX/CCBT PMs exhibited notable cytotoxic effects on MCF-7 cells and showed selective internalization by MCF-7 cells through biotin receptor-mediated active targeting. In vivo antitumor experiments confirmed that PTX/CCBT PMs possessed remarkable tumor-inhibiting effects and low systemic toxicity. This work suggested that PTX/CCBT PMs provided new ideas for self-indicating breast cancer treatment.

Waste heat recovery in carbon capture process using a novel amphipathic inorganic membrane

To reduce the CO2 regeneration heat requirement in the CO2 chemical absorption process, a novel amphipathic ceramic membrane-based transport membrane condenser was developed in this study to act as a heat transfer medium in the rich solvent-split mechanism for enhancing the waste heat recovery performance from the stripped gas (i.e., mainly the gas mixture of CO2 and water vapor). Both hydrophobic and hydrophilic segments coexisted on one membrane surface of amphipathic ceramic membrane, while the other surface was totally hydrophilic. The surface characterization and waste heat recovery performance of the flat sheet amphipathic membrane were investigated, and the original hydrophilic ceramic membrane was adopted as the control. Results showed that the water contact angle with 108.9 ± 4° was screened for the hydrophobic surface of the ceramic membrane to achieve the best waste heat recovery performance. Additionally, the waste heat recovery performance of amphipathic membrane firstly increased and then dropped with an increase in the area ratio of hydrophobic surface to the total membrane surface. The maximum waste heat recovery of 13.39 MJ/(m2·h) was achieved at a hydrophobic area ratio of 37.5 % without segmenting by the hydrophilic surface, which was 5.6 % higher than that of the original hydrophilic ceramic membrane. Furthermore, the maximum water recovery of amphipathic membrane was 8.24 % higher than the original hydrophilic ceramic membrane. When the total area of hydrophobic surface was fixed, dividing the hydrophobic surface into two equally sized hydrophobic segments spaced by the hydrophilic segments could further improve the waste heat recovery performance of amphipathic membrane. This study might provide a new insight on improving the waste heat recovery performance of ceramic membrane.

Micelles of poly[oligo(ethylene glycol) methacrylate] as delivery vehicles for zinc phthalocyanine photosensitizers

Drug-loaded polymeric micelles have proven to be highly effective carrier systems for the efficient delivery of hydrophobic photosensitizers (PSs) in photodynamic therapy (PDT). This study introduces the micellization potential of poly(oligoethylene glycol methyl ether methacrylate) (pOEGMA) as a novel approach, utilizing the hydrophobic methacrylate segments of pOEGMA to interact with highly hydrophobic zinc phthalocyanine (ZnPc), thereby forming a potential micellar drug carrier system. The ZnPc molecule was synthesized from phthalonitrile derivatives and its fluorescence, photodegradation, and singlet oxygen quantum yields were determined in various solvents. In solvents such as tetrahydrofuran, dimethyl sulfoxide, and N,N-dimethylformamide, the ZnPc compound exhibited the requisite photophysical and photochemical properties for PDT applications. The pOEGMA homopolymer was synthesized via reversible addition-fragmentation chain-transfer polymerization, while ZnPc-loaded pOEGMA micelles were prepared using the nanoprecipitation method. Characterization of the pOEGMA, ZnPc, and micelles was conducted using FTIR,1H-NMR, dynamic light scattering, matrix-assisted laser desorption/ionization time-of-flight mass spectrometries, gel permeation chromatography, and transmission electron microscopy. The critical micelle concentration was determined to be 0.027 mg ml-1using fluorescence spectrometry. The drug loading and encapsulation efficiencies of the ZnPc-loaded micelles were calculated to be 0.67% and 0.47%, respectively. Additionally, the release performance of ZnPc from pOEGMA micelles was monitored over a period of nearly 10 d, while the lyophilized micelles exhibited stability for 3 months. Lastly, the ZnPc-loaded micelles were more biocompatible than ZnPc on L929 cell line. The results suggest that the pOEGMA homopolymer possesses the capability to micellize through its methacrylate segments when interacting with highly hydrophobic molecules, presenting a promising avenue for enhancing the delivery efficiency of hydrophobic PSs in PDT. Moreover, it was also deciphered that obtained formulations were highly biocompatible according to cytotoxicity results and could be safely employed as drug delivery systems in further applications.

Translation arrest cancellation of VemP, a secretion monitor in Vibrio, is regulated by multiple cis and trans factors, including SecY

VemP is a secretory protein in the Vibrio species that monitors cellular protein-transport activity through its translation arrest, allowing expression of the downstream secD2-secF2 genes in the same operon, which encode components of the protein translocation machinery. When cellular protein-transport function is fully active, secD2/F2 expression remains repressed as VemP translation arrest is canceled immediately. The VemP arrest-cancellation occurs on the SecY/E/G translocon in a late stage in the translocation process and requires both trans-factors, SecD/F and PpiD/YfgM, and a cis-element, Arg-85 in VemP; however, the detailed molecular mechanism remains elusive. This study aimed to elucidate how VemP passing through SecY specifically monitors SecD/F function. Genetic and biochemical studies showed that SecY is involved in the VemP arrest-cancellation and that the arrested VemP is stably associated with a specific site in the protein-conducting pore of SecY. VemP-Bla reporter analyses revealed that a short hydrophobic segment adjacent to Arg-85 plays a critical role in the regulated arrest-cancellation with its hydrophobicity correlating with the stability of the VemP arrest. We identified Gln-65 and Pro-67 in VemP as novel elements important for the regulation. We propose a model for the regulation of the VemP arrest cancellation by multiple cis-elements and trans-factors with different roles.

Ionic nanoporous membranes from self-assembled liquid crystalline brush-like imidazolium triblock copolymers.

There is a need to generate mechanically and thermally robust ionic nanoporous membranes for separation and fuel cell applications. Herein, we report a general approach to the preparation of ionic nanoporous membranes through custom synthesis, self-assembly, and subsequent chemical manipulations of ionic brush block copolymers. We synthesized polynorbornene-based triblock copolymers containing imidazolium cations balanced by counter anions in the central block, side-chain liquid crystalline units, and sidechain polylactide end blocks. This unique platform comprises: (1) imidazolium/bis(trifluoromethanesulfonyl)imide (TFSI) as the middle block, which has an excellent ion-exchange ability, (2) cyanobiphenyl liquid crystalline end block, a sterically hindered hydrophobic segment, which is chemically stable and immune to hydroxide attack, (3) polylactide brush-like units on the other end block that is easily etched under mild alkaline conditions and (4) a polynorbornene backbone, a lightly crosslinked system that offers mechanical robustness. These membranes retain their morphology before and after backbone crosslinking as well as etching of polylactide sidechains. The ion exchange performance and dimensional stability of these membranes were investigated by water uptake capability and swelling ratio. Moreover, the length of the carbon spacer in the imidazolium/TFSI central block moiety endowed the membrane with improved ionic conductivity. The ionic nanoporous materials are unusual due to their singular thermal, mechanical, alkaline stability and ion transport properties. Applications of these materials include electrochemical actuators, solid-state ionic nanochannel biosensors, and ion-conducting membranes.