Covalent Attachment of Cyclic TAT Peptides to GFP Results in Protein Delivery into Live Cells with Immediate Bioavailability

The delivery of free molecules into the cytoplasm and nucleus by using arginine‐rich cell‐penetrating peptides (CPPs) has been limited to small cargoes, while large cargoes such as proteins are taken up and trapped in endocytic vesicles. Based on recent work, in which we showed that the transduction efficiency of arginine‐rich CPPs can be greatly enhanced by cyclization, the aim was to use cyclic CPPs to transport full‐length proteins, in this study green fluorescent protein (GFP), into the cytosol of living cells. Cyclic and linear CPP–GFP conjugates were obtained by using azido‐functionalized CPPs and an alkyne‐functionalized GFP. Our findings reveal that the cyclic‐CPP–GFP conjugates are internalized into live cells with immediate bioavailability in the cytosol and the nucleus, whereas linear CPP analogues do not confer GFP transduction. This technology expands the application of cyclic CPPs to the efficient transport of functional full‐length proteins into live cells.     

The Photolytic Activity of Poly‐Arginine Cell Penetrating Peptides Conjugated to Carboxy‐tetramethylrhodamine is Modulated by Arginine Residue Content and Fluorophore Conjugation Site

Upon light irradiation, Fluorophore–cell‐penetrating peptide (Fl‐CPP) conjugates can disrupt the integrity of biological membranes. This activity can in turn be used to photoinduce the disruption of endocytic organelles and promote the delivery of entrapped macromolecules such as proteins or RNAs into live cells. Recent mechanistic studies have shown that ROS production by the fluorophore and a latent lytic ability of CPPs act in synergy to elicit photolysis. However, how the structure of fluorophore‐CPP conjugates impacts this synergistic activity remains unclear. Herein, using red blood cells (RBCs) as a model of biological membranes, we show that the number of arginine residues in a CPP as well as the position of fluorophore with respect to the CPP dramatically affect the photolytic activity of a fluorophore‐CPP conjugate. These factors should therefore be considered for the development of effective photoinducible delivery agents.     

Design of peptide–dendrimer conjugates with tumor homing and antitumor effects

Development of drug delivery systems for cancer therapy is a crucial issue. Previously, some peptides were designed as tumor homing cell-penetrating peptides with antitumor activities. In this study, dual function dendrimers with tumor targeting activities and antitumor effects were designed using the tumor targeting CPP44 peptide for acute myelogenous leukemia (AML) and the antitumor p16^INK4a peptide. Two types of peptide–dendrimer conjugates were synthesized. One was a CPP44-linked p16^INK4a peptide-conjugated dendrimer (tandem linked dendrimer) and the other was a dendrimer conjugated with separate CPP44 and p16^INK4a peptides (parallel linked dendrimer). In addition, a peptide cathepsin B substrate was linked to the antitumor p16^INK4a peptide to release it from the carriers. These peptide–dendrimer conjugates produced more effective antitumor effects than a CPP44-linked p16^INK4a peptide. The parallel linked dendrimer showed less association with AML cells than the tandem linked dendrimer, but had greater antitumor effects. This suggested that both cellular uptake and antitumor peptide cleavage affected the antitumor activities of dual functional peptide-conjugated dendrimers.     

Photoinduced Endosomal Escape Mechanism: A View from Photochemical Internalization Mediated by CPP-Photosensitizer Conjugates

Endosomal escape in cell-penetrating peptide (CPP)-based drug/macromolecule delivery systems is frequently insufficient. The CPP-fused molecules tend to remain trapped inside endosomes and end up being degraded rather than delivered into the cytosol. One of the methods for endosomal escape of CPP-fused molecules is photochemical internalization (PCI), which is based on the use of light and a photosensitizer and relies on photoinduced endosomal membrane destabilization to release the cargo molecule. Currently, it remains unclear how this delivery strategy behaves after photostimulation. Recent findings, including our studies using CPP-cargo-photosensitizer conjugates, have shed light on the photoinduced endosomal escape mechanism. In this review, we discuss the structural design of CPP-photosensitizer and CPP-cargo-photosensitizer conjugates, and the PCI mechanism underlying their application.     

Recent Advances and Trends in Chemical CPP–Drug Conjugation Techniques

This review summarizes recent developments in conjugation techniques for the synthesis of cell-penetrating peptide (CPP)–drug conjugates targeting cancer cells. We will focus on small organic molecules as well as metal complexes that were used as cytostatic payloads. Moreover, two principle ways of coupling chemistry will be discussed direct conjugation as well as the use of bifunctional linkers. While direct conjugation of the drug to the CPP is still popular, the use of bifunctional linkers seems to gain increasing attention as it offers more advantages related to the linker chemistry. Thus, three main categories of linkers will be highlighted, forming either disulfide acid-sensitive or stimuli-sensitive bonds. All techniques will be thoroughly discussed by their pros and cons with the aim to help the reader in the choice of the optimal conjugation technique that might be used for the synthesis of a given CPP–drug conjugate     

Relation of Photochemical Internalization to Heat,pH and Ca2+ Ions

The inefficient endosomal escape of drugs or macromolecules is a major obstacle to achieving successful delivery to therapeutic targets. An efficient approach to circumvent this barrier is photochemical internalization (PCI), which uses light and photosensitizers for endosomal escape of the delivered macromolecules. The PCI mechanism is related to photogenerated singlet oxygen, but the mechanism is still unclear. In this study, we examined the relation of PCI to heat, pH and Ca²⁺ ions using cell penetrating peptide (CPP)‐cargo‐photosensitizer (Alexa546 or Alexa633) conjugates. A cell temperature changing experiment demonstrated that heat (thermal mechanism) does not significantly contribute to the photoinduced endosomal escape. Inhibition of V‐ATPase proton pump activity and endosomal pH upregulation indicated that PCI‐mediated endosomal escape needs endosomal acidification prior to photoirradiation. Imaging of the CPP‐cargo‐photosensitizer and Ca²⁺ ions during photostimulation showed that intracellular calcium increase is not the cause of the endosomal escape of the complex. The increment is mainly due to Ca²⁺ influx. These findings show the importance of extra‐ and intracellular milieu conditions in the PCI mechanism and enrich our understanding of PCI‐related changes in cell.     

Single-molecule motions of oligoarginine transporter conjugates on the plasma membrane of Chinese hamster ovary cells

To explore the real-time dynamic behavior of molecular transporters of the cell-penetrating-peptide (CPP) type on a biological membrane, single fluorescently labeled oligoarginine conjugates were imaged interacting with the plasma membrane of Chinese hamster ovary (CHO) cells. The diffusional motion on the membrane, characterized by single-molecule diffusion coefficient and residence time (tau R), defined as the time from the initial appearance of a single-molecule spot on the membrane (from the solution) to the time the single molecule disappears from the imaging focal plane, was observed for a fluorophore-labeled octaarginine (a model guanidinium-rich CPP) and compared with the corresponding values observed for a tetraarginine conjugate (negative control), a lipid analogue, and a fluorescently labeled protein conjugate (transferrin-Alexa594) known to enter the cell through endocytosis. Imaging of the oligoarginine conjugates was enabled by the use of a new high-contrast fluorophore in the dicyanomethylenedihydrofuran family, which brightens upon interaction with the membrane at normal oxygen concentrations. Taken as a whole, the motions of the octaarginine conjugate single molecules are highly heterogeneous and cannot be described as Brownian motion with a single diffusion coefficient. The observed behavior is also different from that of lipids, known to penetrate cellular membranes through passive diffusion, conventionally involving lateral diffusion followed by membrane bilayer flip-flop. Furthermore, while the octaarginine conjugate behavior shares some common features with transferrin uptake (endocytotic) processes, the two systems also exhibit dissimilar traits when diffusional motions and residence times of single constructs are compared. Additionally, pretreatment of cells with cytochalasin D, a known actin filament disruptor, produces no significant effect, which further rules out unimodal endocytosis as the mechanism of uptake. Also, the involvement of membrane potential in octaarginine-membrane interaction is supported by significant changes in the motion with high [K(+)] treatment. In sum, this first study of single transporter motion on the membrane of a living cell indicates that the mode by which the octaarginine transporter penetrates the cell membrane appears to either be a multimechanism uptake process or a mechanism different from unimodal passive diffusion or endocytosis.     

Bioreducible crosslinked low molecular weight branched PEI-PBLG as an efficient gene carrier

Low molecular weight polyethylenimine-poly(gamma-benzyl L-glutamate) (PEI-PBLG) was crosslinked by N,N′-cystamine-bisacrylamide (CBA) to get the polymer named as CBA-PEI-PBLG (CPP). CPP not only inherits PEI-PBLG’s amphiphilic advantages, but also possesses reducible properties. CPP can complex with DNA to form nanoparticles. CPP/DNA complex particles were characterized by particle size and zeta potential analysis. The result showed that the complex particles have suitable size and surface charges for gene delivery. And gel retardation assay also prove CBA-PEI-PBLG has proper condensing ability for DNA. CPP has good reducible property, and also has good biocompatibility because of introducing PBLG segment. The cytotoxicity of CPP was evaluated using MTT assay, and the results showed CPP has lower cytotoxicity compared with PEI 25 K. The transfection properties were characterized in different cells by using plasmid DNA as a reporter. CPP showed higher transfection efficiencies and lower cytotoxicity in HeLa cells. This was attributed to bioreducible and biocompatibility properties of the CPP. These results suggested that CPP is a promising low-toxic, highly effective non-viral gene carrier.     

Influence of phosphorylation on the foamability and stability of bovine serum albumin and citrus peel pectin mixed foams

We study the influence of phosphorylation on the foamability and stability of bovine serum albumin (BSA), phosphorylated BSA (pBSA), and citrus peel pectin (CPP) mixed foams as a function of BSA–CPP, pBSA–CPP mixing ratios, at a fixed solution pH of 4.5. Our results show that pBSA solutions result in more stable foams as compared with their BSA counterparts. We further show that the addition of CPP leads to BSA–CPP and pBSA–CPP complexation which increases the foamability and stability of foams as compared with protein-only foams. Also, foam stability is highest for pBSA–CPP mixed foams with mixing ratio pBSA:CPP?=?1:1 due to the combined effect of pBSA–pBSA and pBSA–CPP interactions.     

Electrocatalytic Behavior of Manganese and Cobalt Porphyrins Attached to Graphene Quantum Dots: Applied in the Oxidation of Hydrazine

Manganese and cobalt metalated 5, 10, 15-tris(aminophenyl)-20-(4-carboxyphenyl) porphyrins (ClMnTA₃CPP and CoTA₃CPP) were synthesized and attached to graphene quantum dots (GQDs) via π-π interaction and electrostatic interaction. The electrochemical oxidation of hydrazine was performed via cyclic voltammetry and chronoamperometry. The CoTA₃CPP showed good electrocatalytic activity towards the oxidation of hydrazine in terms of catalytic rate constants and limits of detection (LoD). ClMnTA₃CPP showed lower overpotential 0.60 V. The introduction of GQDs improved the electrocatalytic ability when combined with CoTA₃CPP and ClMnTA₃CPP with the lowest LoD (0.0025 mM CoTA₃CPP–GQDs) followed by ClMnTA₃CPP–GQDs with 0.0033 mM.     

粘度法研究氯化聚丙烯和涂料树脂间的相容性

用稀溶液粘度法研究了氯化聚丙烯与石油树脂、丙烯酸树脂和醇酸树脂间的相容性,并用α判据对相容性结果进行判别。结果显示,石油树脂/氯化聚丙烯的共混体系是相容的;丙烯酸树脂/氯化聚丙烯的共混体系是不相容的。而醇酸树脂与氯化聚丙烯的相容性情况复杂,由二者的组成决定。当m(醇酸树脂)∶m(氯化聚丙烯)1∶1时,体系是相容的;当m(醇酸树脂)∶m(氯化聚丙烯)1∶1时,体系是不相容的。通过共溶剂法和涂膜宏观特性对上述体系的相容性进行测定,所得结果与α判据的结果相符合,印证了稀溶液粘度法研究溶液中高分子间的相互作用来预测涂料树脂的相容性具有一定可行性。     

Electronic Communication between two [10]cycloparaphenylenes and Bis(azafullerene) (C59N)2 Induced by Cooperative Complexation

The complex of [10]cycloparaphenylene ([10]CPP) with bis(azafullerene) (C₅₉N)₂ is investigated experimentally and computationally. Two [10]CPP rings are bound to the dimeric azafullerene giving [10]CPP?(C₅₉N)₂?[10]CPP. Photophysical and redox properties support an electronic interaction between the components especially when the second [10]CPP is bound. Unlike [10]CPP?C₆₀, in which there is negligible electronic communication between the two species, upon photoexcitation a partial charge transfer phenomenon is revealed between [10]CPP and (C₅₉N)₂ reminiscent of CPP‐encapsulated metallofullerenes. Such an alternative electron‐rich fullerene species demonstrates C₆₀‐like ground‐state properties and metallofullerene‐like excited‐state properties opening new avenues for construction of functional supramolecular architectures with organic materials.     

Anti-Hyperglycemic Effects of Refined Fractions from Cyclocarya paliurus Leaves on Streptozotocin-Induced Diabetic Mice

To identify the chemical components responsible for the anti-hyperglycemic effect of Cyclocarya paliurus (Batal.) Iljinsk (Juglandaceae) leaves, an ethanol extract (CPE) and a water extract (CPW) of C. paliurus leaves, as well as their total flavonoids (CPF), triterpenoids (CPT) and crude polysaccharides (CPP), were prepared and assessed on streptozotocin (STZ)-induced diabetic mice. After being orally administrated once a day for 24 days, CPF (300 mg/kg), CPP (180 mg/kg), or CPF+CPP (300 mg/kg CPF + 180 mg/kg CPP) treatment reversed STZ-induced body weight and muscle mass losses. The glucose tolerance tests and insulin tolerance tests suggested that CPF, CPP, and CPF+CPP showed anti-hyperglycemic effect in STZ-induced diabetic mice. Furthermore, CPF enhances glucose-stimulated insulin secretion in MIN6 cells and insulin-stimulated glucose uptake in C2C12 myotubes. CPF and CPP suppressed inflammatory cytokine levels in STZ-induced diabetic mice. Additionally, CPF and CPP improved STZ-induced diabetic nephropathy assessed by H&E staining, blood urea nitrogen content, and urine creatinine level. The molecular networking and Emperor analysis results indicated that CPF showed potential anti-hyperglycemic effects, and HPLC–MS/MS analysis indicated that CPF contains 3 phenolic acids and 9 flavonoids. In contrast, CPT (650 mg/kg) and CPC (300 mg/kg CPF + 180 mg/kg CPP + 650 mg/kg CPT) did not show anti-hyperglycemic effect. Taken together, polysaccharides and flavonoids are responsible for the anti-hyperglycemic effect of C. paliurus leaves, and the clinical application of C. paliurus need to be refined.     

Solution properties of chlorinated polypropylene and maleic anhydride grafted chlorinated polypropylene

The solution behaviors of the chlorinated polypropylene (CPP) and its grafted polymers (CPP-g-MAH) were systematically studied to characterize their polar change with grafting maleic anhydride (MAH) onto the chain of CPP. The molecular weights of the polymers were determined with light scattering measurements, and the Mark–Houwink equation of CPP in toluene was also obtained. The result showed that the Mark–Houwink equation of CPP was suitable for estimating the molecular weight of the polydisperse samples of CPP and not suitable to CPP-g-MAH because the molecular polarity of the graft polymers had changed with grafting MAH onto CPP. The solubility result of CPP and CPP-g-MAH in various solvents indicated that the polarity of CPP gradually increased with grafting MAH onto its chain, which would cause the solubility of poorly hydrogen bonded solvents for CPP-g-MAH to gradually become poor, whereas that of moderately hydrogen bonded solvents for the polymers becomes better with an increase of the MAH graft content. This is consistent with the results of their dilution ratio and solubility parameter. Stabilities of the 344^# resin–CPP-g-MAH–toluene solutions showed that the miscibility of CPP-g-MAH and 344^# resin was improved with increase of the MAH grafted content.     

Cycloparaphenylene and their radicals anchored to a metal−organic framework

Cycloparaphenylene (CPP) shows modulated photophysical and electronic properties due to its strained structure and radially oriented π-electron system. Incorporation of CPP into metal-organic frameworks (MOFs) could transfer its extensive properties in solution to porous solids. Moreover, with the unique arrangement of the macrocycles and their interactions with the framework, emerging characteristics are anticipated. As an example of “robust dynamics”, we synthesized the first MOF structure (FDM-1001) with CPP precisely anchored to the ordered framework by employing a [8]CPP-containing linear dicarboxylate linker. Metric relationship between the dynamic macrocycles and the robust backbone creates ideal π-π interactions between them, which leads to an essentially directional arrangement of [8]CPP in the three-dimensional space. Furthermore, the MOF with [8]CPP could be successfully oxidized to generate an infinite array of radicals that show enhanced air stability compared to its molecular analogue.     

Cell-Penetrating Peptides: Correlation between Peptide-Lipid Interaction and Penetration Efficiency

Cell-penetrating peptides are used in the delivery of peptides and biologics, with some cell-penetrating peptides found to be more efficient than others. The exact mechanism of how they interact with the cell membrane and penetrate it, however, remains unclear. This study attempts to investigate the difference in free energy profiles of three cell-penetrating peptides (TAT, CPP1 and CPP9) with a model lipid bilayer (DOPC) using molecular dynamics pulling simulations with umbrella sampling. Potential mean force (PMF) and free energy barrier between the peptides and DOPC are determined using WHAM analysis and MM-PBSA analysis, respectively. CPP9 is found to have the smallest PMF value, followed by CPP1 and TAT, consistent with the experimental data. YDEGE peptide, however, does not give the highest PMF value, although it is a non-cell-permeable peptide. YDEGE is also found to form water pores, alongside with TAT and CPP9, suggesting that it is difficult to distinguish true water pore formation from artefacts arising from pulling simulations. On the contrary, free energy analysis of the peptide-DOPC complex at the lipid-water interface with MM-PBSA provides results consistent with experimental data with CPP9 having the least interaction with DOPC and lowest free energy barrier, followed by CPP1, TAT and YDEGE. These findings suggest that peptide-lipid interaction at the lipid-water interface has a direct correlation with the penetration efficiency of peptides across the lipid bilayer.     

Determination of three-dimensional solubility parameters of chlorinated polypropylene by ultrasonic degradation

The degradation reactions of chlorinated polypropylene (CPP) in toluene under ultrasonic irradiation were studied. The Mark–Houwink equation acquired from fractional precipitations was also suitable for estimating the molecular weight of degraded CPP. An objective standard was proposed for judging the solution behaviour of CPP in solvents by the study on the relative solubility of CPP before and after degradation. Then Hansen three-dimensional solubility parameters and the total parameter of CPP were obtained by optimization calculation in terms of the criterion proposed here. It was proved that the total parameter of CPP is creditable by the turbidity method. Compared to other standards, the result obtained from the proposed standard accorded well with the standard of complete miscibility suggested by Flory–Huggins for polymers and solvents as well as the objective reality. This standard may provide a reference for other polymers.     

Lactosylated casein phosphopeptides as specific indicators of heated milks

Casein phosphopeptides (CPP) were identified in small amounts in milks heated at various intensities by using matrix-assisted laser desorption/ionization (MALDI) time-of-flight mass spectrometry. CPP selectively concentrated on hydroxyapatite (HA) were regenerated using phosphoric acid mixed in the matrix. Unphosphorylated peptides not retained by HA were removed by buffer washing. This procedure enhanced the MALDI signals of CPP that are ordinarily suppressed by the co-occurrence of unphosphorylated peptides. CPP, belonging to the β-casein (CN) family, i.e., (f1-29) 4P, (f1-28) 4P, and (f1-27) 4P, and the α_s2-CN family, i.e., (f1-21) 4P and (f1-24) 4P, were observed in liquid and powder milk. The lactosylated counterparts were specific to intensely heated milks, but absent in raw and thermized/pasteurized milk. Most CPP with C-terminal lysines probably arose from the activity of plasmin; an enzyme most active in casein hydrolysis. A CPP analogue was used as the internal standard. The raw milk signature peptide β-CN (f1-28) 4P constituted ~4.3% of the total β-CN. Small amounts of lactosylated peptides, which varied with heat treatment intensity, were detected in the milk samples. The limit of detection of ultra-high-temperature milk adjunction in raw or pasteurized milk was ~10%.     

二步法聚丙烯/丙烯酸表面接枝聚合研究

研究了二步法聚丙烯膜表面的丙烯酸接枝反应 .实验发现 ,以醋酐为溶剂的反应体系所得接枝率明显好于以水为溶剂的体系 ;接枝率随光敏剂浓度、单体浓度增大而增加 ;提高反应温度 ,可使接枝率明显增大 ;接枝后的聚丙烯膜表面亲水性可明显改善 .并用红外光谱证实了丙烯酸在聚丙烯膜表面的接枝 .     

Partial Charge Transfer in the Shortest Possible Metallofullerene Peapod,La@C82⊂[11]Cycloparaphenylene

[11]Cycloparaphenylene ([11]CPP) selectively encapsulates La@C₈₂ to form the shortest possible metallofullerene–carbon nanotube (CNT) peapod, La@C₈₂?[11]CPP, in solution and in the solid state. Complexation in solution was affected by the polarity of the solvent and was 16 times stronger in the polar solvent nitrobenzene than in the nonpolar solvent 1,2‐dichlorobenzene. Electrochemical analysis revealed that the redox potentials of La@C₈₂ were negatively shifted upon complexation from free La@C₈₂. Furthermore, the shifts in the redox potentials increased with polarity of the solvent. These results are consistent with formation of a polar complex, (La@C₈₂)^δ??[11]CPP^δ+, by partial electron transfer from [11]CPP to La@C₈₂. This is the first observation of such an electronic interaction between a fullerene pea and CPP pod. Theoretical calculations also supported partial charge transfer (0.07) from [11]CPP to La@C₈₂. The structure of the complex was unambiguously determined by X‐ray crystallographic analysis, which showed the La atom inside the C₈₂ near the periphery of the [11]CPP. The dipole moment of La@C₈₂ was projected toward the CPP pea, nearly perpendicular to the CPP axis. The position of the La atom and the direction of the dipole moment in La@C₈₂?[11]CPP were significantly different from those observed in La@C₈₂?CNT, thus indicating a difference in orientation of the fullerene peas between fullerene–CPP and fullerene–CNT peapods. These results highlight the importance of pea–pea interactions in determining the orientation of the metallofullerene in metallofullerene–CNT peapods.