Production of pharmacologic monodisperse aerosols

G. C. Smaldone; H. Itoh; D. L. Swift; J. Kaplan; R. Florek; W. Wells; H. N. Wagner

doi:10.1152/jappl.1983.54.2.393

Production of pharmacologic monodisperse aerosols

G. C. Smaldone
, H. Itoh
, D. L. Swift
, J. Kaplan
, R. Florek
, W. Wells
, H. N. Wagner

Pulmonary and Critical Care

Johns Hopkins University

Research output: Contribution to journal › Article › peer-review

22 Scopus citations

Abstract

Monodisperse aerosols containing a range of chemical material, including pharmacologically active substances, were produced by using a modified Sinclair-LaMer condensation generator. Instead of the usual hot-wire technique, an ultrasonic nebulizer was used to suspend nuclei in the gas phase as an aqueous polydisperse aerosol. This technique allowed the generation of monodisperse oil (sebacate) aerosols containing nuclei of sodium chloride, histamine, methacholine, antigen, iron oxide, methylene blue, uranine, radioactive technetium pertechnetate, and technetium-labeled human serum albumin. Quantitative agonist activity was demonstrated for each active nucleus. Particle sizes ranged from 0.65 to 3 μm, with a geometric standard deviation of 1.1-1.2. This system can produce a stable, monodisperse, biologically active radiolabeled aerosol for a period of several hours.

Original language	English
Pages (from-to)	393-399
Number of pages	7
Journal	Unknown Journal
Volume	54
Issue number	2
DOIs	https://doi.org/10.1152/jappl.1983.54.2.393
State	Published - 1983

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10.1152/jappl.1983.54.2.393

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title = "Production of pharmacologic monodisperse aerosols",

abstract = "Monodisperse aerosols containing a range of chemical material, including pharmacologically active substances, were produced by using a modified Sinclair-LaMer condensation generator. Instead of the usual hot-wire technique, an ultrasonic nebulizer was used to suspend nuclei in the gas phase as an aqueous polydisperse aerosol. This technique allowed the generation of monodisperse oil (sebacate) aerosols containing nuclei of sodium chloride, histamine, methacholine, antigen, iron oxide, methylene blue, uranine, radioactive technetium pertechnetate, and technetium-labeled human serum albumin. Quantitative agonist activity was demonstrated for each active nucleus. Particle sizes ranged from 0.65 to 3 μm, with a geometric standard deviation of 1.1-1.2. This system can produce a stable, monodisperse, biologically active radiolabeled aerosol for a period of several hours.",

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T1 - Production of pharmacologic monodisperse aerosols

AU - Smaldone, G. C.

AU - Itoh, H.

AU - Swift, D. L.

AU - Kaplan, J.

AU - Florek, R.

AU - Wells, W.

AU - Wagner, H. N.

PY - 1983

Y1 - 1983

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AB - Monodisperse aerosols containing a range of chemical material, including pharmacologically active substances, were produced by using a modified Sinclair-LaMer condensation generator. Instead of the usual hot-wire technique, an ultrasonic nebulizer was used to suspend nuclei in the gas phase as an aqueous polydisperse aerosol. This technique allowed the generation of monodisperse oil (sebacate) aerosols containing nuclei of sodium chloride, histamine, methacholine, antigen, iron oxide, methylene blue, uranine, radioactive technetium pertechnetate, and technetium-labeled human serum albumin. Quantitative agonist activity was demonstrated for each active nucleus. Particle sizes ranged from 0.65 to 3 μm, with a geometric standard deviation of 1.1-1.2. This system can produce a stable, monodisperse, biologically active radiolabeled aerosol for a period of several hours.

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DO - 10.1152/jappl.1983.54.2.393

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AN - SCOPUS:0020679392

VL - 54

SP - 393

EP - 399

JO - Unknown Journal

JF - Unknown Journal

IS - 2

ER -

Production of pharmacologic monodisperse aerosols

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