ABSTRACT
The aerosol inhalation delivery of composite particles consisting of Ag nanoparticles enveloped by polyvinylpyrrolidone was investigated in experiments with mice. An ultrasonic nebulizing system was created for the generation of aerosols with a mean diameter and mass concentration of 700 ± 50 nm and 65 ± 5 mg/m3, respectively. The mass fraction of Ag in the composite particles was α = 0.061. The aerosol delivery was performed in a whole-body chamber with an exposition time of 20 min. Pharmacokinetic measurements were taken and the silver concentrations in the blood and lungs of the mice were measured as a function of time after exposition by means of electrothermal (graphite furnace) atomic absorption spectrometry. The inhalation dose and other pharmacokinetic parameters were determined. The antibacterial effect of aerosolized silver was assessed for mice infected with Klebsiella pneumoniae 82 and Staphylococcus aureus ATCC 25953. The survival rate of the infected mice after the aerosol exposure demonstrated the high antibacterial efficiency of Ag nanoparticles after inhalation delivery.
ABSTRACT
Aerosol inhalation delivery of ceftriaxone in mice was investigated. An ultrasonic nebulizer within the ranges of mean particle diameter 0.5-1.5 µm and mass concentration 0.01-0.6 µg/cm3 was used in inhalation experiments. Pharmacokinetic measurements were carried out using a nose-only chamber. Ceftriaxone concentration in blood serum and its mass in the lungs of mice were measured as a function of time using high-performance liquid chromatography. The body-delivered dose was within the range 3-5 mg/kg. The antibacterial effect of aerosolized ceftriaxone was investigated for mice infected with Klebsiella pneumoniae 82 and Staphylococcus aureus ATCC 25 953. The survival rate for infected mice after the treatment with ceftriaxone aerosol revealed the high antibacterial efficiency of this kind of treatment.
ABSTRACT
In the framework of classical fluctuation theory an analytical formula is derived for the reversible work of formation of just detached carbon cap on the surface of catalyst nanoparticle (NP). This cap is considered as single walled carbon nanotube (SWCNT) formation center. The work of cap formation depends on the source carbon chemical potential µC. Using the derived formula for this work an expression for the rate of SWCNT formation is determined. From this expression the SWCNT diameter distributions can be obtained. The obtained distributions have sharp maxima. It is found that the modal SWCNT diameter d(m) increases weakly with µC being in the narrow window of 1.0 < d(m) < 1.8 nm when changing the source carbon chemical potential in a wide range. The determined diameter distributions proved to be in a good agreement with the typical values of the SWCNT diameters as experimentally measured in the chemical vapor deposition process. The increase of d(m) is accompanied by the increase of the distribution width Δd. The selectivity d(m)/Δd is a function of µC, the higher values of µC the worse selectivity is observed. Although the value of the SWCNT formation rate I cannot be calculated precisely the relationship between I and the system parameters, such as the NP radius R(S), can be obtained. This relationship is derived for the solid-liquid-solid system. To determine the function I(R(S)) for nanotubes of a certain diameter d, formulas for catalyst∕amorphous carbon mutual solubilities as functions of NP radius are derived in the framework of the rigorous Gibbs theory of interface. Using the derived formulas an expression giving the dependence I(R(S)) is obtained. The expression predicts an increase of I with the radius R(S). The estimations carried out for the metal/carbon interface surface tension of 1000 mN/m show that the SWCNT formation rate increases by a few orders of magnitude with the radius increase from 1 to 10 nm.
ABSTRACT
BACKGROUND: Aerosol lung administration is a convenient way to deliver water-insoluble or poorly soluble drugs, provided that small-sized particles are generated. Here, for the outbred male mice, we show that the pulmonary administration of ibuprofen nanoparticles requires a dose that is three to five orders of magnitude less than that for the orally delivered particles at the same analgesic effect. METHOD: The aerosol evaporation-condensation generator consisted of a horizontal cylindrical quartz tube with an outer heater. Argon flow was supplied to the inlet and aerosol was formed at the outlet. The particle mean diameter and number concentration varied from 10 to 100 nm and 10(3)-10(7) cm(-)3, respectively. The analgesic action and side pulmonary effects caused by the inhalation of ibuprofen nanoparticles were investigated. RESULTS: The chemical composition of aerosol particles was shown to be identical with the maternal drug. Using the nose-only exposure chambers, the mice lung deposition efficiency was evaluated as a function of the particle diameter. CONCLUSIONS: The dose-dependent analgesic effect of aerosolized ibuprofen was studied in comparison with the oral treatment. It was found that the dose for aerosol treatment is three to five orders of magnitude less than that required for oral treatment at the same analgesic effect. Accompanying effects were moderate venous hyperemia and some emphysematous signs.
Subject(s)
Analgesics, Non-Narcotic/pharmacology , Ibuprofen/pharmacology , Nanoparticles/administration & dosage , Administration, Inhalation , Animals , Dose-Response Relationship, Drug , Ibuprofen/administration & dosage , Lung/drug effects , Lung/metabolism , Lung/pathology , Male , Mice , Particle SizeABSTRACT
The respiratory system provides entry for drug nanoparticles to cure systemic diseases. The modern devices that are available on the market of therapeutic aerosol delivery systems have a number of disadvantages. There remains a need for an alternative means that is low cost, convenient, and capable of producing small-sized particles. On the other hand, one-third of the modern drugs are poorly water soluble. Many currently available injectable formulations of such drugs can cause side effects that originate from detergents and other agents used for their solubilization. The aerosol lung administration may by a good way for delivery of the water-insoluble drugs. We present here a new way for the generation of drug nanoparticles suitable for many water insoluble substances based on the evaporation-condensation route. In this paper the indomethacin nanoaerosol formation was studied and its anti-inflammatory effect to the outbred male mice was examined. The evaporation-condensation aerosol generator consisted of a horizontal cylindrical quartz tube with an outer heater. Argon flow was supplied to the inlet and the aerosol was formed at the outlet. The particle mean diameter and number concentration were varied in the ranges 3 to 200 nm and 10(3) to 10(7) cm(-3), respectively. The liquid chromatography and X-ray diffraction methods have shown the nanoparticles consist of the amorphous phase indomethacin. The aerosol lung administration experiments were carried out in the whole-body exposure chamber. Both the lung deposited dose and the particle deposition efficiency were determined as a function of the mean particle diameter for mice being housed into the nose-only exposure chambers. The anti-inflammatory action and side pulmonary effects caused by the inhalation of indomethacin nanoparticles were investigated. It was found that the aerosol administration was much more effective than the peroral treatment. The aerosol route required a therapeutic dose six orders of magnitude less than that for peroral administration.
