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Scientists at The Scripps Research Institute Make Strides in Addressing
Mysteries of Ozone in the Human Body
La Jolla, CA. February 27, 2003 - In what is a first for biology, a team
of investigators at The Scripps Research Institute (TSRI) is reporting that the
human body makes ozone.
Led by TSRI President Richard Lerner, M.D. and Associate Professor in the
Department of Chemistry Paul Wentworth, Jr, Ph.D., who made the original discovery,
the team has been slowly gathering evidence over the last few years that the
human body produces the reactive gas - most famous as the ultraviolet ray-absorbing
component of the ozone layer - as part of a mechanism to protect it from bacteria
and fungi.
"Ozone was a big surprise," says TSRI Professor Bernard Babior, M.D., Ph.D. "But
it seems that biological systems manufacture ozone, and that ozone has an effect
on those biological systems."
Now, in an important development in this unfolding story, Babior, Wentworth,
and their TSRI colleagues report in an upcoming issue of the journal Proceedings
of the National Academy of Sciences that the ozone appears to be produced
in a process involving human immune cells known as neutrophils and human immune
proteins known as antibodies.
"It is a tremendously efficient chemical and biological process," says Wentworth,
who adds that the presence of ozone in the human body may be linked to inflammation,
and therefore this work may have tremendous ramifications for treating inflammatory
diseases.
The Ozone Hole in Each One of Us
Ozone is a reactive form of oxygen that exists naturally as a trace gas in
the atmosphere. It is perhaps best known for its crucial role absorbing ultraviolet
radiation in the stratosphere, where it is concentrated in a so-called ozone
layer, protecting life on earth from solar radiation. Ozone is also a familiar
component of air in industrial and urban settings where the gas is a hazardous
component of smog. However, ozone has never before been detected in biology.
Two years ago, Lerner and Wentworth demonstrated that antibodies are able
to produce ozone and other chemical oxidants when they are fed a reactive form
of oxygen called singlet oxygen. And late last year, Lerner, Wentworth, and Babior
demonstrated that the oxidants produced by antibodies can destroy bacteria by
poking holes in their cell walls.
This was a completely unexpected development, since for the last 100 years,
immunologists believed that antibodies - proteins secreted into the blood
by the immune system - acted only to recognize foreign pathogens and attract
lethal "effector" immune cells to the site of infection.
Questions, Answers, and More Questions
The question still remained, however, as to how the antibodies were making
the ozone. The TSRI team knew that in order to make the ozone and other highly
reactive oxidants, the antibodies had to use a starting material known as singlet
oxygen, a rare, excited form of oxygen.
Now Babior and Wentworth believe they have found where the singlet oxygen
comes from - one of the effector immune cells called neutrophils which are
little cellular factories that produce singlet oxygen and other oxidants. During
an immune response, the neutrophils engulf and destroy bacteria and fungi by
blasting them with these oxidants.
The work of the TSRI scientists suggests that the antibacterial effect of
neutrophils is enhanced by antibodies. In addition to killing the bacteria themselves,
the neutrophils feed singlet oxygen to the antibodies, which convert it into
ozone, adding weapons to the assault.
"This is really something new, and there are a million questions [that follow]," says
Babior. "What does the ozone do to the body's proteins and nucleic acids? Can
neutrophils make ozone without the antibodies? Is ozone made by other cells?
How long does ozone last in the body? And, most importantly, how will these discoveries
help to cure disease?"
The research team continues to investigate.
The article, "Investigating antibody-catalyzed ozone generation by human
neutrophils," is authored by Bernard M. Babior, Cindy Takeuchi, Julie Ruedi,
Abel Gutierrez, and Paul Wentworth, Jr. The article will be available online
this week at: http://www.pnas.org/cgi/doi/1
0.1073/pnas.0530 251100, and it will be published in an upcoming issue of
the journal Proceedings of the National Academy of Sciences .
The research was funded by the National Institutes of Health (NIH), through
research grants and through a training grant; and by The Skaggs Institute for
Research.
For more information contact:
Jason Bardi
10550 North Torrey Pines Road
La Jolla, California 92037
Tel: 858.784.9254
Fax: 858.784.8118
jasonb@scripps.edu
Copyright © 2003 TSRI.
All rights reserved. Reproduction in whole or in part in any form or medium without express written permission of TSRI is prohibited.
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