Combined site-specific release retardant mini-matrix tablets (C-SSRRMT) for extended oral delivery of dexketoprofen trometamol: in vitro evaluation and single versus multiple doses pharmacokinetic study in human volunteers

Abstract

Development of extended release oral formulations of dexketoprofen trometamol (DT), a rapidly eliminated drug with high solubility, poses a great challenge especially when a portion of the dose is to be absorbed from the colon. In this study, site-specific release-retardant mini-matrix tablets (SSRRMTs) were developed and functionally coated with pH-responsive materials to achieve a site-specific delivery of DT at the duodenojejunal (DSRRMT) and ileocecal (ISRRMT) regions. Stomach-specific coated mini-tablets (SSCMTs) were manufactured for immediate release of about 16% of the daily dose of DT in the stomach. The SSCMT, DSRRMT, and ISRRMT were combined into a solid dosage form (C-SSRRMT tablets or capsules) to achieve the required linear release profile for once daily administration of DT. The SSRRMT and C-SSRRMT formulations were evaluated for the physical properties, in vitro-disintegration and in vitro dissolution and proved to be consistent with the pharmacopeial specifications. The in vitro release profiles of both C-SSRRMT tablets and capsules showed a constant release rate of about 6?mg/h and were similar to that of the theoretical target linear release profile. The pharmacokinetic study using human volunteers showed the bioequivalence of a single oral dose of C-SSRRMT capsules compared to three-successive oral doses of the immediate release market tablets with less ups and downs in the drug levels. The C-SSRRMT capsules formulation, may therefore, constitute an advance in the extended oral delivery of DT without the lack of efficacy and the adverse events frequently encountered in multiple daily dosing of the immediate release tablets.     

A smart hydrogel-based time bomb triggers drug release mediated by pH-jump reaction

Abstract

We demonstrate a timed explosive drug release from smart pH-responsive hydrogels by utilizing a phototriggered spatial pH-jump reaction. A photoinitiated proton-releasing reaction of o-nitrobenzaldehyde (o-NBA) was integrated into poly(N-isopropylacrylamide-co-2-carboxyisopropylacrylamide) (P(NIPAAm-co-CIPAAm)) hydrogels. o-NBA-hydrogels demonstrated the rapid release of protons upon UV irradiation, allowing the pH inside the gel to decrease to below the pK_a value of P(NIPAAm-co-CIPAAm). The generated protons diffused gradually toward the non-illuminated area, and the diffusion kinetics could be controlled by adjusting the UV irradiation time and intensity. After irradiation, we observed the enhanced release of entrapped L-3,4-dihydroxyphenylalanine (DOPA) from the gels, which was driven by the dissociation of DOPA from CIPAAm. Local UV irradiation also triggered the release of DOPA from the non-illuminated area in the gel via the diffusion of protons. Conventional systems can activate only the illuminated region, and their response is discontinuous when the light is turned off. The ability of the proposed pH-jump system to permit gradual activation via proton diffusion may be beneficial for the design of predictive and programmable devices for drug delivery.     

Enzyme-directed pH-responsive exfoliation and dispersion of graphene and its decoration by gold nanoparticles for use as a hybrid catalyst

A non-destructive, safe and practical strategy to produce high quality graphene in high yield is urgently required, since this would pave the way for a wide range of applications of graphene in the future. Here we present a pH-responsive water-dispersible method for the exfoliation and functionalization of graphene by using lysozyme. The pH-responsive dispersion of graphene may be useful for the reversible assembly of multicomponent/multifunctional nanohybrid materials and nanoscale electronic devices. More importantly, composites can be easily constructed through the interactions between disulphide groups in lysozyme and gold nanoparticles （AuNPs）. The resulting graphene-AuNPs composites show excellent catalytic activity towards reduction of o-nitroaniline by NaBH4. Since lysozyme is low cost and has antibacterial properties, and has been widely used in food preservation, medicine and the pharmaceutical industry, our approach may open a new scalable route for the manufacture of high-quality, nondestructive graphene for practical applications.     

磷酸化改性纤维素纳米纤丝复合聚氨酯制备pH响应性形状记忆材料

本研究通过在纤维素大分子中引入磷酸基团获得具有pH敏感性的磷酸化纤维素纳米纤丝(Phosphorylation Cellulose Nanofibril,PCNF),然后采用溶剂共混复合聚氨酯(PU)成功制备了具有pH响应能力的形状记忆材料。探究了不同PCNF接枝已内酯材料(PCNF-CL)添加量下PCNF/PU复合材料(SMPU)在酸碱条件下的形状记忆性能。结果表明,在酸碱条件下PCNF-CL与PU分子间能可逆地产生一种氢键缔合,这种作用产生不同的效果可使材料固定和回复形状;当PCNF-CL添加量为10%时,在pH值=1的条件下,该材料可以加工成临时形状,固定率为99.8%,pH值=13时又回复到初始形状,回复率达到99.5%;力学拉伸结果表明,在添加PCNF-CL后SMPU复合材料的力学强度显著提升,且在添加量为1%时拉伸强度达到最大。     

Chimeric Stimuli-Responsive Liposomes as Nanocarriers for the Delivery of the Anti-Glioma Agent TRAM-34

Nanocarriers are delivery platforms of drugs, peptides, nucleic acids and other therapeutic molecules that are indicated for severe human diseases. Gliomas are the most frequent type of brain tumor, with glioblastoma being the most common and malignant type. The current state of glioma treatment requires innovative approaches that will lead to efficient and safe therapies. Advanced nanosystems and stimuli-responsive materials are available and well-studied technologies that may contribute to this effort. The present study deals with the development of functional chimeric nanocarriers composed of a phospholipid and a diblock copolymer, for the incorporation, delivery and pH-responsive release of the antiglioma agent TRAM-34 inside glioblastoma cells. Nanocarrier analysis included light scattering, protein incubation and electron microscopy, and fluorescence anisotropy and thermal analysis techniques were also applied. Biological assays were carried out in order to evaluate the nanocarrier nanotoxicity in vitro and in vivo, as well as to evaluate antiglioma activity. The nanosystems were able to successfully manifest functional properties under pH conditions, and their biocompatibility and cellular internalization were also evident. The chimeric nanoplatforms presented herein have shown promise for biomedical applications so far and should be further studied in terms of their ability to deliver TRAM-34 and other therapeutic molecules to glioblastoma cells.     

pH-responsive micelles based on (PCL)2(PDEA-b-PPEGMA)2 miktoarm polymer: controlled synthesis,characterization, and application as anticancer drug carrier

Amphiphilic A₂(BC)₂ miktoarm star polymers [poly(ϵ-caprolactone)]₂-[poly(2-(diethylamino)ethyl methacrylate)-b- poly(poly(ethylene glycol) methyl ether methacrylate)]₂ [(PCL)₂(PDEA-b-PPEGMA)₂] were developed by a combination of ring opening polymerization (ROP) and continuous activators regenerated by electron transfer atom transfer radical polymerization (ARGET ATRP). The critical micelle concentration (CMC) values were extremely low (0.0024 to 0.0043 mg/mL), depending on the architecture of the polymers. The self-assembled empty and doxorubicin (DOX)-loaded micelles were spherical in morphologies, and the average sizes were about 63 and 110 nm. The release of DOX at pH 5.0 was much faster than that at pH 6.5 and pH 7.4. Moreover, DOX-loaded micelles could effectively inhibit the growth of cancer cells HepG2 with IC₅₀ of 2.0 μg/mL. Intracellular uptake demonstrated that DOX was delivered into the cells effectively after the cells were incubated with DOX-loaded micelles. Therefore, the pH-sensitive (PCL)₂(PDEA-b-PPEGMA)₂ micelles could be a prospective candidate as anticancer drug carrier for hydrophobic drugs with sustained release behavior.     

pH-triggered conduction of amine-functionalized single ZnO wire integrated on a customized nanogap electronic platform

The electrical conductance response of single ZnO microwire functionalized with amine-groups was tested upon an acid pH variation of a solution environment after integration on a customized gold electrode array chip. ZnO microwires were easily synthesized by hydrothermal route and chemically functionalized with aminopropyl groups. Single wires were deposited from the solution and then oriented through dielectrophoresis across eight nanogap gold electrodes on a platform single chip. Therefore, eight functionalized ZnO microwire-gold junctions were formed at the same time, and being integrated on an ad hoc electronic platform, they were ready for testing without any further treatment. Experimental and simulation studies confirmed the high pH-responsive behavior of the amine-modified ZnO-gold junctions, obtaining in a simple and reproducible way a ready-to-use device for pH detection in the acidic range. We also compared this performance to bare ZnO wires on the same electronic platform, showing the superiority in pH response of the amine-functionalized material.     

pH-responsive molecularly imprinted polymer for sorption and rapid desorption of dibutyl phthalate

The pH-responsive molecularly imprinted polymers (SR-MIPs) for the removal of dibutyl phthalate (DBP) were obtained. The polymers were synthesized using methyl methacrylate, methacrylic acid, divinylbenzene, and a template mixed at different ratios allowing to optimize the process. The so-prepared SR-MIPs were evaluated at various pH values in processes of DBP sorption. The studies covered evaluation of uptake capacity, sorption kinetics, selectivity, and elution. The imprinted samples are characterized by improved factors comparing to their non-imprinted analogues, revealing also pH-sensitivity. The highest removal of DBP (130 mg g^?1) was achieved at pH = 6, while pH-driven desorption (90%) was the most efficient at pH = 8.     

SCL@SiO2纳米颗粒制备及其稳定Pickering乳液的研究

用共轭亚油酸钠（SCL）在SiO2纳米颗粒表面吸附,得到表面改性的SiO2纳米颗粒,然后在80 oC条件下通过热聚合引发SCL分子自交联,从而稳定SCL@SiO2纳米颗粒的SCL层并改善表面润湿性。通过Zeta电位表征手段证实SCL吸附在SiO2纳米颗粒表面。以SCL@SiO2纳米颗粒作为单一乳化剂制备液体石蜡的Pickering乳液,结果表明该Pickering乳液比传统乳液更稳定。由于SCL@SiO2纳米颗粒的SCL层比简单吸附脂肪酸的SiO2改性颗粒更稳定,且粒径会随着pH的变化而发生变化,因此由其稳定的Pickering乳液具有一定的pH响应性。     

A glutamic acid-based polymer keeping intact the integrity of all the three original functionalities of the amino acid

Dimethyl glutamate, on treatment with allyl bromide, afforded dimethyl N,N-diallylglutamate which upon alkaline ester hydrolysis followed by acidification with aqueous HCl gave N,N-diallylglutamic acid hydrochloride [(CH₂=CH–CH₂)₂NH⁺CH(CO₂H)(CH₂)₂CO₂H Cl^?] I. Using Butler’s cyclopolymerization protocol, new monomer I underwent ammonium persulfate-initiated polymerization to give pyrrolidine ring-embedded linear cyclopolymer II i.e. ?[?CH₂(C₄H₆)NH⁺{CH(CO₂H)(CH₂)₂CO₂H Cl^?}CH₂?]?_n retaining the integrity of all the three functionalities of glutamic acid. Under the influence of pH, the repeating units of triprotic acid (+) in II were equilibrated to those of water-insoluble diprotic polyzwitterionic acid (±) III, water-soluble monoprotic poly(zwitterion-anion) (±?) IV, and its conjugate base polydianion (=) V. The critical salt concentration required to promote water solubility of (±) III has been determined to be 0.548 M NaCl, 0.271 M NaBr, 0.133 M NaI. The basicity constants of the carboxyl groups and trivalent nitrogen in (=) V have been determined. A 5 ppm and 20 ppm concentrations of III are effective in inhibiting the precipitation of CaSO₄ from its supersaturated solution with a ≈100% scale inhibition efficiency at 40 °C for a duration of over 3 and 16 h, respectively.