The characterization of protein lactylation in relation to cardiac metabolic reprogramming in neonatal mouse hearts.

In mammals, the neonatal heart can regenerate upon injury within a short time after birth, while adults lose this ability. Metabolic reprogramming has been demonstrated to be critical for cardiomyocyte proliferation in the neonatal heart. Here, we reveal that cardiac metabolic reprogramming could be regulated by altering global protein lactylation. By performing 4D label-free proteomics and lysine lactylation (Kla) omics analyses in mouse hearts at postnatal days 1, 5, and 7, 2297 Kla sites from 980 proteins are identified, among which 1262 Kla sites from 409 proteins are quantified. Functional clustering analysis reveals that the proteins with altered Kla sites are mainly involved in metabolic processes. The expression and Kla levels of proteins in glycolysis show a positive correlation while a negative correlation in fatty acid oxidation. Furthermore, we verify the Kla levels of several differentially modified proteins, including ACAT1, ACADL, ACADVL, PFKM, PKM, and NPM1. Overall, our study reports a comprehensive Kla map in the neonatal mouse heart, which will help to understand the regulatory network of metabolic reprogramming and cardiac regeneration.

Ketone bodies promote epididymal white adipose expansion to alleviate liver steatosis in response to a ketogenic diet.

Liver can sense the nutrient status and send signals to other organs to regulate overall metabolic homoeostasis. Herein, we demonstrate that ketone bodies act as signals released from the liver that specifically determine the distribution of excess lipid in epididymal white adipose tissue (eWAT) when exposed to a ketogenic diet (KD). An acute KD can immediately result in excess lipid deposition in the liver. Subsequently, the liver sends the ketone body ß-hydroxybutyrate (BHB) to regulate white adipose expansion, including adipogenesis and lipogenesis, to alleviate hepatic lipid accumulation. When ketone bodies are depleted by deleting 3-hydroxy-3-methylglutaryl-CoA synthase 2 gene in the liver, the enhanced lipid deposition in eWAT but not in inguinal white adipose tissue is preferentially blocked, while lipid accumulation in liver is not alleviated. Mechanistically, ketone body BHB can significantly decrease lysine acetylation of peroxisome proliferator-activated receptor gamma in eWAT, causing enhanced activity of peroxisome proliferator-activated receptor gamma, the key adipogenic transcription factor. These observations suggest that the liver senses metabolic stress first and sends a corresponding signal, that is, ketone body BHB, to specifically promote eWAT expansion to adapt to metabolic challenges.

The BR-body proteome contains a complex network of protein-protein and protein-RNA interactions.

Bacterial ribonucleoprotein bodies (BR-bodies) are non-membrane-bound structures that facilitate mRNA decay by concentrating mRNA substrates with RNase E and the associated RNA degradosome machinery. However, the full complement of proteins enriched in BR-bodies has not been defined. Here, we define the protein components of BR-bodies through enrichment of the bodies followed by mass spectrometry-based proteomic analysis. We find 111 BR-body-enriched proteins showing that BR-bodies are more complex than previously assumed. We identify five BR-body-enriched proteins that undergo RNA-dependent phase separation in vitro with a complex network of condensate mixing. We observe that some RNP condensates co-assemble with preferred directionality, suggesting that RNA may be trafficked through RNP condensates in an ordered manner to facilitate mRNA processing/decay, and that some BR-body-associated proteins have the capacity to dissolve the condensate. Altogether, these results suggest that a complex network of protein-protein and protein-RNA interactions controls BR-body phase separation and RNA processing.

Mevalonate pathway and male reproductive aging.

Male fertility declines with age. The mevalonate pathway, through which cholesterol and nonsteroidal isoprenoids are synthesized, plays key role in metabolic processes and is an essential pathway for cholesterol production and protein prenylation. Male reproductive aging is accompanied by dramatic changes in the metabolic microenvironment of the testis. Since the mevalonate pathway has an important role in spermatogenesis, we attempted to explore the association between male reproductive aging and the mevalonate pathway to explain the mechanism of male reproductive aging. Alterations in the mevalonate pathway may affect male reproductive aging by decreasing cholesterol synthesis and altering testis protein prenylation. Decreased cholesterol levels affect cholesterol modification, testosterone production, and remodeling of germ cell membranes. Aging-related metabolic disorders also affect the metabolic coupling between somatic cells and spermatogenic cells, leading to male fertility decline. Therefore, we hypothesized that alterations in the mevalonate pathway represent one of the metabolic causes of reproductive aging.

pH-Dependent complexation and polyelectrolyte chain conformation of polyzwitterion-polycation coacervates in salted water.

The phase behavior and chain conformational structure of biphasic polyzwitterion-polyelectrolyte coacervates in salted aqueous solution are investigated with a model weak cationic polyelectrolyte, poly(2-vinylpyridine) (P2VP), whose charge fraction can be effectively tuned by pH. It is observed that increasing the pH leads to the increase of the yielding volume fraction and the water content of dense coacervates formed between net neutral polybetaine and cationic P2VP in contrast to the decrease of critical salt concentration for the onset of coacervation, where the P2VP charge fraction is reduced correspondingly. Surprisingly, a single-molecule fluorescence spectroscopic study suggests that P2VP chains upon coacervation seem to adopt a swollen or an even more expanded conformational structure at higher pH. As the hydrophobicity of P2VP chains is accompanied by a reduced charge fraction by increasing the pH, a strong pH-dependent phase and conformational behaviors suggest the shift of entropic and enthalpic contribution to the underlying thermodynamic energy landscape and chain structural dynamics of polyelectrolyte coacervation involving weak polyelectrolytes in aqueous solution.

Combining Hyperbranched and Linear Structures in Solid Polymer Electrolytes to Enhance Mechanical Properties and Room-Temperature Ion Transport.

Polyethylene oxide (PEO)-based polymers are commonly studied for use as a solid polymer electrolyte for rechargeable Li-ion batteries; however, simultaneously achieving sufficient mechanical integrity and ionic conductivity has been a challenge. To address this problem, a customized polymer architecture is demonstrated wherein PEO bottle-brush arms are hyperbranched into a star architecture and then functionalized with end-grafted, linear PEO chains. The hierarchical architecture is designed to minimize crystallinity and therefore enhance ion transport via hyperbranching, while simultaneously addressing the need for mechanical integrity via the grafting of long, PEO chains (M n = 10,000). The polymers are doped with lithium bis(trifluoromethane) sulfonimide (LiTFSI), creating hierarchically hyperbranched (HB) solid polymer electrolytes. Compared to electrolytes prepared with linear PEO of equivalent molecular weight, the HB PEO electrolytes increase the room temperature ionic conductivity from ∼2.5 × 10-6 to 2.5 × 10-5 S/cm. The conductivity increases by an additional 50% by increasing the block length of the linear PEO in the bottle brush arms from M n = 1,000 to 2,000. The mechanical properties are improved by end-grafting linear PEO (M n = 10,000) onto the terminal groups of the HB PEO bottle-brush. Specifically, the Young's modulus increases by two orders of magnitude to a level comparable to commercial PEO films, while only reducing the conductivity by 50% below the HB electrolyte without grafted PEO. This study addresses the trade-off between ion conductivity and mechanical properties, and shows that while significant improvements can be made to the mechanical properties with hierarchical grafting of long, linear chains, only modest gains are made in the room temperature conductivity.

Dynamics of Confined Microgel Liquids: Weakened Spatial Confinement Effect by Microgel Particle Compliance.

Spatial confinement has a great impact on the structures and dynamics of interfacial molecular and polymer liquid films. Most prior research has focused on confined liquids of fixed material compliance and often treated them in approximation to the "hard-sphere" interaction model. In this study, we microscopically investigate the structural dynamics of highly deformable poly(N-isopropylacrylamide) (PNIPAM) microgels confined between two solid surfaces in comparison to that of nearly nondeformable microgels of the same chemistry. We observe that the mobility and structural relaxation of highly deformable PNIPAM microgels at an apparent volume fraction, ϕ = 0.49-0.70, show little change with the reduction of gap spacing, in stark contrast to confinement-induced dynamic retardation of "hard-sphere"-like stiff PNIPAM microgels. The critical gap spacing, defined as the onset of confinement effect to deviate from the bulk behavior, is found to be approximately 17-22 particle layers for highly deformable microgels of ϕ = 0.56-0.70, much smaller than that of approximately 40 particle layers or larger for stiff microgels or model "hard-sphere" colloidal liquids of similar ϕ. Additionally, we observe no evident confinement-enhanced structural reorganization of deformable microgels near the confining surfaces when gap spacing approaches the critical gap spacing. Microgel deformation upon strong confinement is attributed to the disrupted confinement-induced ordering of confined microgels. Hence, it is clearly indicated that spatial confinement exhibits a much weaker effect on highly compliant microgel particles than stiff ones, resulting in a significantly less reduction in microgel interfacial dynamics. It therefore gives insights into the molecular design of polymeric thin films of variable compliance to control friction and lubrication.

Effect of polyampholyte net charge on complex coacervation between polyampholytes and inorganic polyoxometalate giant anions.

The effect of net charge of zwitterionic polymers on the phase behavior and viscoelastic properties of hybrid polyampholyte-polyoxometalate (POM) complexes in salted aqueous solutions is investigated with polyampholyte copolymers consisting of both positively and negatively charged monomers. Zwitterionic polyampholytes of varied net charge, abbreviated as PAxMy, are synthesized by varying the feeding molar ratio of negatively charged 2-acrylamido-2-methyl-1-propanesulfonic acid (AMPS) to positively charged [3-(methacryloylamino)propyl]trimethylammonium chloride (MAPTAC) monomers in aqueous solution. The coacervate formation between PAxMy and inorganic anionic metatungstate POM ({W12}) in LiCl added aqueous solutions can be enhanced by increasing the molar fraction of positively charged MAPTAC monomer and LiCl concentration. The salt-broadened coacervation, clearly distinct from the salt-suppressed one between oppositely charged polyelectrolytes, suggests the account of zwitterion-anion pairing for PAxMy-{W12} coacervate formation due to stronger binding of multivalent {W12} giant ions with PAxMy than simple ions. Importantly, as AMPS or MAPTAC monomer fraction in polyampholytes is varied by merely ±5% from the effective net neutral case, the viscoelasticity of PAxMy-{W12} coacervates can be modified by 4-5 folds, suggesting a new tuning parameter to fine control the macroionic interactions and material properties of biomimetic complex coacervates.

Rapid and Efficient Coacervate Extraction of Cationic Industrial Dyes from Wastewater.

Effluent wastewater containing dyes from textile, paint, and various other industrial wastes have long posed environmental damage. Functional nanomaterials offer new opportunities to treat these effluent wastes in an unprecedentedly rapid and efficient fashion due to their large surface area-to-volume ratio. In this work, we explore a new approach of wastewater treatment using macroionic coacervate complexes formed with zwitterionic polyampholytes and anionic inorganic polyoxometalate (POM) nanoclusters to extract methylene blue (MB) dye as well as other cationic industrial dyes from model wastewater. Biphasic organic-inorganic macroion complexes are designed to produce a small volume of coacervate adsorbents of high density and viscoelasticity, in contrast to a large volume of supernatant solution for rapid and efficient dye removal. The efficiency of coacervate extraction is characterized by the adsorption isotherm and maximum MB uptake capacity against the concentrations of polyampholyte, POM, and LiCl salt using UV-vis spectrophotometry to optimize the coacervate formation conditions. Our macroionic coacervate complexes could reach nearly 99% removal efficiency for the model wastewater samples of varied MB concentration in <1 min. The extraction capacity up to ∼400 mg/g far surpasses the dye extraction efficiency of widely used activated carbon adsorbents. We also explore the regeneration of coacervate complexes containing high concentration of extracted MB by a simple Fenton oxidation process to bleach coacervate complexes for repeated POM usage, which shows similar MB extraction efficiency after regeneration. Hence, coacervate extraction based upon spontaneous liquid-liquid separating complexation between polyzwitterions and POMs is demonstrated as a rapid, efficient, and sustainable method for industrial dye wastewater treatment. In perspective, coacervate extraction could advantageously possess dual processing options in separation industry through either membrane fabrication or use directly in mixer-settlers.

Long-Circulating Amphiphilic Doxorubicin for Tumor Mitochondria-Specific Targeting.

The mitochondria have emerged as a novel target for cancer chemotherapy primarily due to their central roles in energy metabolism and apoptosis regulation. Here, we report a new molecular approach to achieve high levels of tumor- and mitochondria-selective deliveries of the anticancer drug doxorubicin. This is achieved by molecular engineering, which functionalizes doxorubicin with a hydrophobic lipid tail conjugated by a solubility-promoting poly(ethylene glycol) polymer (amphiphilic doxorubicin or amph-DOX). In vivo, the amphiphile conjugated to doxorubicin exhibits a dual function: (i) it binds avidly to serum albumin and hijacks albumin's circulating and transporting pathways, resulting in prolonged circulation in blood, increased accumulation in tumor, and reduced exposure to the heart; (ii) it also redirects doxorubicin to mitochondria by altering the drug molecule's intracellular sorting and transportation routes. Efficient mitochondrial targeting with amph-DOX causes a significant increase of reactive oxygen species levels in tumor cells, resulting in markedly improved antitumor efficacy than the unmodified doxorubicin. Amphiphilic modification provides a simple strategy to simultaneously increase the efficacy and safety of doxorubicin in cancer chemotherapy.

Highly Proton Conducting Polyelectrolyte Membranes with Unusual Water Swelling Behavior Based on Triptycene-containing Poly(arylene ether sulfone) Multiblock Copolymers.

Multiblock poly(arylene ether sulfone) copolymers are attractive for polyelectrolyte membrane fuel cell applications due to their reportedly improved proton conductivity under partially hydrated conditions and better mechanical/thermal stability compared to Nafion. However, the long hydrophilic sequences required to achieve high conductivity usually lead to excessive water uptake and swelling, which degrade membrane dimensional stability. Herein, we report a fundamentally new approach to address this grand challenge by introducing shape-persistent triptycene units into the hydrophobic sequences of multiblock copolymers, which induce strong supramolecular chain-threading and interlocking interactions that effectively suppress water swelling. Consequently, unlike previously reported multiblock copolymer systems, the water swelling of the triptycene-containing multiblock copolymers did not increase proportionally with water uptake. This combination of high water uptake and low swelling behavior of these copolymers resulted in excellent proton conductivity and membrane dimensional stability under fully hydrated conditions. In particular, the triptycene-containing multiblock copolymer film with the longest hydrophilic block length (i.e., BPSH100-TRP0-15k-15k) had a water uptake of 105%, an excellent proton conductivity of 0.150 S/cm, and a volume swelling ratio of just 29% (more than 42% reduction compared to Nafion 212).

Distinct Effects of Multivalent Macroion and Simple Ion on the Structure and Local Electric Environment of a Weak Polyelectrolyte in Aqueous Solution.

Adding ionic species can critically affect the structure of weak polyelectrolyte (PE) chains, whose charge density in aqueous solution can be greatly regulated by bathing solution conditions such as pH and added ions. Distinct from simple ions that can be treated as point charges, multivalent macroions of finite size, including many charged nanoparticles and biopolymers, could show strong electrostatic coupling with PEs and effectively modify the conformation and assembly of PEs in aqueous solution. In this work, we have compared the effects of hydrophilic multivalent macroion of finite size and simple divalent ion on the conformational transition of a model weak polybase, poly(2-vinylpyridine) (P2VP), in dilute aqueous solution. By using fluorescence correlation spectroscopy combined with photon counting histogram analysis, we have examined the swollen-to-collapsed conformational transition and local electric potential of a P2VP chain in ionic aqueous solution at a single-molecule level. Adding inorganic polytungstate ([W12]) macroion bearing eight negative charges per [W12] of ∼0.8 nm in diameter at increased concentration from 10-9 to 10-5 mM can lead to a shift of the critical conformational transition pH, pHcr, of P2VP to lower pH values, in an opposite trend to the previously reported effect of adding simple monovalent anion. Conversely, adding simple divalent sulfate anion can lead to a nonmonotonic change of pHcr when increasing its concentration from 0.03 to 15 mM. Additionally, at pH < pHcr where P2VP is highly protonated and adopts a swollen conformation, a monotonic decrease of P2VP size is observed with increased sulfate ionic concentration, exhibiting the typical ionic screening effect. In contrast, the size of the P2VP chain shows little change with increasing [W12] concentration before the precipitation of P2VP from water. To investigate the distinct effects of multivalent ion and macroion on the conformational transition of P2VP in aqueous solution, we have also measured the local proton concentration in the vicinity to a P2VP chain by an attached pH-sensitive fluorescence probe. In both cases, we have observed the monotonic reduction of the local electric potential of a swollen P2VP chain with increased ionic concentration, despite the increased protonation degree of P2VP. The results suggest that counterion condensation of multivalent ion and macroion can modify the effective net charge density of P2VP chains in dilute aqueous solution. However, possibly due to its high multivalency and finite size, multivalent [W12] macroion is much more effective in modifying the local electric environment and structure of P2VP chains at 3-7 orders of magnitude lower concentrations than simple sulfate counterion.

Organic-inorganic macroion coacervate complexation.

Coacervate complexes that are liquid-liquid separated complex materials are often formed by stoichiometrically mixing oppositely charged polyelectrolytes in salted aqueous solution. Entropy-driven ion pairing, resulting from the release of counterions near polyelectrolytes, has been identified as the primary driving force for coacervate formation between oppositely charged polyelectrolytes, including proteins and DNA, in aqueous solution. In this work we have examined the complexation between net neutral zwitterionic poly(sulfobetaine methacrylate) (PSBMA) and inorganic polyoxometalate (POM) polyanions in LiCl aqueous solutions. Biphasic liquid-like coacervate complexes can be formed over a much broader range of POM-to-PSBMA molar ratio and LiCl concentration than that for conventional polyelectrolyte coacervate complexation. Composition analysis of the dried supernatant and dense coacervate has confirmed that both PSBMA and POM macroions are primarily present in the dense coacervate as the macroion-rich phase in contrast to the presence of LiCl solely in the supernatant as the macroion-poor phase. The increase of net charge negativity of PSBMA and supernatant conductivity suggests stronger binding of PSBMA with POM anions than monovalent Cl-, resulting in the release of bound Cl- anions to the aqueous solution for the formation of PSBMA-POM coacervates in LiCl solution. All experimental evidence has demonstrated the generality of ion-pairing induced coacervate complexation with net neutral zwitterionic polymers and multivalent inorganic nanomaterials. The complexation between organic and inorganic macroions could give insights into many supramolecular assembly processes in nature and also lead to a new paradigm in developing hybrid macroionic materials for emerging applications from green catalysis to nanomedicine.

Shape and Mechanical Control of Poly(ethylene oxide) Based Polymersome with Polyoxometalates via Hydrogen Bond.

Polymersomes are self-assembled vesicles of amphiphilic block copolymers and have been explored for wide applications from drug delivery to micro/nanoreactors. As polymersomes are soft and highly deformable, their shape instability due to osmolarity difference across polymer membranes and low elasticity could conversely limit their practical use. Instead of selecting particular polymer chemical reactions to enhance the mechanical properties, we have employed inorganic polyoxometalate (POM) clusters as simple physical cross-linkers to control the shape and mechanical stability of polymersomes in aqueous suspensions. Robust spherical shape with enhanced elastic and bending moduli of POM-dressed poly(ethylene oxide) (PEO) based polymersomes is achieved. We have accounted for the hydrogen bonding between POM and PEO blocks for the adsorption and stabilization of POMS on polymersomes, whose interaction strength could also be tuned by mixing solvents of hydrogen bond donors or receptors with water. The stimuli-responsive properties of POMs are introduced in POM-dressed polymersomes upon the interaction of POMs with PEO blocks in aqueous media. As POM can be used as nanomedicines, catalysts, and other functional nanomaterials, POM-dressed polymersomes with significant shape and mechanical reinforcement could broaden the applications of PEO-based polymersomes and other PEO-tethered nanocolloids.

Molecular Mechanism of Ionic-Liquid-Induced Membrane Disruption: Morphological Changes to Bilayers, Multilayers, and Vesicles.

The application of ionic liquids (ILs) in many industrially relevant processes provides an urgent need to better understand their molecular interactions with biological systems. A detailed understanding of the cytotoxicity mechanism of ILs can be helpful in facilitating the molecular design of nontoxic ILs. Using coarse-grained molecular dynamics (MD) simulations, we investigate the effects of imidazolium-based ILs on several lipid bilayer morphologies. Our results demonstrate that the asymmetric insertion of IL cations into one side of a lipid bilayer leaflet enhances the leaflet strain, which upon reaching a critical value triggers a morphological disruption in the bilayer. Consistently, the bending modulus of the bilayer is reduced by 1 to 2 orders of magnitude relative to that of an IL-free planar bilayer prior to the disruption event. Our results suggest that ILs that can easily insert into the lipid bilayer without diffusing across or inducing lipid flip-flop can be more disruptive to a lipid biomembrane.

Molecular mechanisms of ionic liquid cytotoxicity probed by an integrated experimental and computational approach.

Ionic liquids (ILs) are salts that remain liquid down to low temperatures, and sometimes well below room temperature. ILs have been called "green solvents" because of their extraordinarily low vapor pressure and excellent solvation power, but ecotoxicology studies have shown that some ILs exhibit greater toxicity than traditional solvents. A fundamental understanding of the molecular mechanisms responsible for IL toxicity remains elusive. Here we show that one mode of IL toxicity on unicellular organisms is driven by swelling of the cell membrane. Cytotoxicity assays, confocal laser scanning microscopy, and molecular simulations reveal that IL cations nucleate morphological defects in the microbial cell membrane at concentrations near the half maximal effective concentration (EC50) of several microorganisms. Cytotoxicity increases with increasing alkyl chain length of the cation due to the ability of the longer alkyl chain to more easily embed in, and ultimately disrupt, the cell membrane.

Interaction of Ionic Liquids with a Lipid Bilayer: A Biophysical Study of Ionic Liquid Cytotoxicity.

Ionic liquids (ILs) have been widely considered and used as "green solvents" for more than two decades. However, their ecotoxicity results have contradicted this view, as ILs, particularly hydrophobic ones, are reported to exhibit high toxicity. Yet the origin of their toxicology remains unclear. In this work, we have investigated the interaction of amphiphilic ILs with a lipid bilayer as a model cell membrane to understand their cytotoxicity at a molecular level. By employing fluorescence imaging and light and X-ray scattering techniques, we have found that amphiphilic ILs could disrupt the lipid bilayer by IL insertion, end-capping the hydrophobic edge of the lipid bilayer, and eventually disintegrating the lipid bilayer at high IL concentration. The insertion of ILs to cause the swelling of the lipid bilayer shows strong dependence on the hydrophobicity of IL cationic alky chain and anions and is strongly correlated with the reported IL cytotoxicity.

Probing the Inhomogeneous Charge Distribution on Annealed Polyelectrolyte Star Polymers in Dilute Aqueous Solutions.

The conformational structure of a polyelectrolyte chain in dilute aqueous solution is strongly coupled with its surrounding electrostatic environment. With the introduction of branched topology, the distribution of counterions in the vicinity of a polyelectrolyte chain becomes highly inhomogeneous, giving rise to complex structures of branched polyelectrolytes in dilute aqueous solution. To directly probe the local electrostatic conditions near a branched polyelectrolyte in aqueous solutions, star-shaped poly(2-vinylpyridine) (P2VP) polymers with precise labeling of one single fluorophore at different locations, for example, the star center or the terminal group of one arm, were synthesized using reversible addition-fragmentation chain transfer (RAFT) polymerization of vinyl-terminated P2VP macromonomers. Using fluorescence correlation spectroscopy (FCS) combined with photon counting histogram (PCH) analysis, the conformational structures and local electric potential of P2VP star polyelectrolytes were investigated in dilute aqueous solutions of varied pH at a single molecule level. Despite the same hydrodynamic radius of P2VP stars, pH-sensitive fluorophores labeled at different locations sensitively differentiated the higher electric potential at the star center from the lower electric potential at the periphery in dilute aqueous solutions.

Effects of Nanoparticle Morphology and Acyl Chain Length on Spontaneous Lipid Transfer Rates.

We report on studies of lipid transfer rates between different morphology nanoparticles and lipids with different length acyl chains. The lipid transfer rate of dimyristoylphosphatidylcholine (di-C14, DMPC) in discoidal "bicelles" (0.156 h(-1)) is 2 orders of magnitude greater than that of DMPC vesicles (ULVs) (1.1 × 10(-3) h(-1)). For both bicellar and ULV morphologies, increasing the acyl chain length by two carbons [going from di-C14 DMPC to di-C16, dipalmitoylphosphatidylcholine (DPPC)] causes lipid transfer rates to decrease by more than 2 orders of magnitude. Results from small angle neutron scattering (SANS), differential scanning calorimetry (DSC), and fluorescence correlation spectroscopy (FCS) are in good agreement. The present studies highlight the importance of lipid dynamic processes taking place in different morphology biomimetic membranes.

Accelerated insulin aggregation under alternating current electric fields: Relevance to amyloid kinetics.

The time-dependent nucleation phase is critical to amyloid fibrillation and related to many pathologies, in which the conversion from natively folded amyloidogenic proteins to oligomers via nucleation is often hypothesized as a possible underlying mechanism. In this work, non-uniform AC-electric fields across two asymmetric electrodes were explored to control and examine the aggregation of insulin, a model amyloid protein, in aqueous buffer solution at constant temperature (20 °C) by fluorescence correlation spectroscopy and fluorescence microscopy. Insulin was rapidly concentrated in a strong AC-field by imposed AC-electroosmosis flow over an optimal frequency range of 0.5-2 kHz. In the presence of an AC-field, direct fibrillation from insulin monomers without the formation of oligomer precursors was observed. Once the insulin concentration had nearly doubled its initial concentration, insulin aggregates were observed in solution. The measured lag time for the onset of insulin aggregation, determined from the abrupt reduction in insulin concentration in solution, was significantly shortened from months or years in the absence of AC-fields to 1 min-3 h under AC-fields. The ability of external fields to alter amyloid nucleation kinetics provides insights into the onset of amyloid fibrillation.