OZONE DOSIMETRY USING RADIOACTIVE AND STABLE ISOTOPES
Project Number5R01ES006554-02
Contact PI/Project LeaderRUSSELL, MICHAEL L
Awardee OrganizationDUKE UNIVERSITY
Description
Abstract Text
Ozone induces toxic damage to the lung at a small but specific site, the
alveolar region most proximal to the terminal bronchiole. Distal alveoli
are spared, thus suggesting the presence of either a decreasing O3 dose
gradient within the alveolar region or a difference in cellular
susceptibility. Because of resolution limitations no experimental studies
have ever demonstrated the alveolar region dose gradient. The final dose
that reaches this proximal alveolar region is regulated by 03 uptake
within the nasopharynx and tracheobronchial tree. Using radioactive and
stable oxygen isotopes as 03 dosimetry tracers we will test the hypothesis
that a significant alveolar region dose gradient exists causing the
proximal region to absorb substantially more 03 than the distal region,
and that the nasopharynx acts as a major determinate of alveolar 03
uptake. Oxygen-l5 labeled 03 (15-OOO) will be generated using a cyclotron,
and laboratory animals will be given an acute exposure. The radioactivity
of major tissues such as the nasopharynx, trachea, individual lung lobes,
and extra-pulmonary tissues will be measured using a gamma-ray counter.
Intraspecies comparisons in rats and interspecies comparisons between
mice, hamsters, rats, and guinea pigs will be examined for 03 deposition
differences. Mechanical ventilation will be used to investigate the effect
of ventilatory parameter alteration on dosimetry. The elution profile of
15-OOO reaction products from the trachea will be assessed for those
products which stay within the airway because they are unable to diffuse
in aqueous media. The lipid vs. non-lipid components of 15-OOO reaction
products in bronchoalveolar lavage fluid will be measured. The major
functional compartments containing 03 reaction products such as lipid vs.
non-lipid and aqueous soluble vs. non-soluble whole lung will be analyzed
using 18-O3. The 18-O3 will be analyzed using Charged Particle Activation
Analysis (CPAA) where the oxygen-18 is converted to fluorine-18, a
radioisotope which decays by positron release. CPAA followed by positron -
track autoradiography will be used to demonstrate and quantify 18-O3
gradients within the alveolar region of lung sections. This proposed
investigation will provide an experimentally-based analysis of 03
dosimetry throughout the respiratory tract.
National Institute of Environmental Health Sciences
CFDA Code
DUNS Number
044387793
UEI
TP7EK8DZV6N5
Project Start Date
01-August-1993
Project End Date
31-July-1998
Budget Start Date
01-August-1994
Budget End Date
31-July-1995
Project Funding Information for 1994
Total Funding
$170,259
Direct Costs
$112,904
Indirect Costs
$57,355
Year
Funding IC
FY Total Cost by IC
1994
National Institute of Environmental Health Sciences
$170,259
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 5R01ES006554-02
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