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Document Description
Title
The
antibacterial
activity
of
trimethoprim-sulfamethoxazole
in
urine
Author
March
,
Sandra
B.
,
1939-
Description
Thesis
(M.
Sc.)--Memorial
University
of
Newfoundland
,
1983.
Medicine
Date
1982
Pagination
xiii, 161 leaves : ill.
Subject
Urine;
Co-trifamole
Degree
M.
Sc.
Degree Grantor
Memorial University of Newfoundland. Faculty of Medicine
Discipline
Medicine
Language
Eng
Notes
Bibliography:
leaves
148-157.
Abstract
Cotrimoxazole
(TMP-SMX)
is
a
premixed
combination
of-the
antimicrobial
agents
,
trimethoprim
(TMP)
and
sulfamethoxazole
(SMX)
, in a
fixed
ratio.
The
drug
has been
used
for the
treatment
of
urinary
tract
and
other
infections
for
more
than
10
years
but its
efficacy
and the
nature
of its
antibacterial
activity
have
remained
controversial.
The
present
work
was
undertaken
in an
effort
to
clarify
some
of the
issues
which
have been
raised.
-
The
antibacterial
properties
of the
drug
and its
components
were
assessed
in
several
in
vitro
systems.
Synergy
between
TMP
and
SMX
,
one
of the
main
arguments
supporting
the
use
of the
fixed
combination
, was
examined
by
drug
diffusion
in
agar
,
checkerboard
titration
, and
time-kill
curves
against
a
standard
Escherichia
coli
strain
(ATCC
25922)
and
against
a
variety
of
bacterial
pathogens
isolated
from
patients
with
urinary
tract
infection.
Minimal
inhibitory
concentrations
for
100
clinical
isolates
were
established
by
agar
dilution
and the
parameters
by
which
synergy
is
defined
were
evaluated.
Time-kill
curves
,
constructed
from
growth
in
drug-supplemented
broth
and
urine
, and in
urine
from
cotrimoxazole-treated
patients
, were
used
to
assess
the
kinetics
of
antibacterial
activity
of
TMP-SMX
and its
components
against
pathogens
commonly
associated
with
urinary
tract
infections.
--
The
results
reported
here
indicate
that
TMP
is
the
more
active
agent
in the
mixture
and in
many
instances
inhibition
is
afforded
by the
TMP
component
alone.
In
vitro
synergy
could
be
demonstrated
when
the
test
organism
was
sensitive
to
each
of the
components
but the
synergistic
effect
was
clear
only
at
drug
levels
significantly
lower
than those
achievable
in
urine
following
usual
drug
dosage.
Time-kill
curves
demonstrate
the
bactericidal
nature
of
TMP-SMX
activity
but
results
with
TMP
alone
were not
markedly
different.
Bactericidal
effects
could
not be
detected
for
SMX.
--
Bioassay
of
urine
samples
from
cotrimoxazole-treated
patients
showed
that
TMP
was the
major
active
constituent.
Only
low
levels
of
biologically
active
SMX
were
detected
by
assay
against
a
TMP-resistant
strain
of
Proteus
mirabilis.
The
minor
contribution
of
SMX
to
total
antibacterial
activity
in
urine
specimens
from these
patients
was
confirmed
by the
addition
of
para-aminobenzoic
acid
(PABA)
, a
known
antagonist
of
sulfonamides.
-
The
data
presented
do
not
support
the
efficacy
of the
fixed
ratio
combination
in
management
of
urinary
tract
infections.
Type
Text
Resource Type
Electronic
thesis
or
dissertation
Format
Image/jpeg;
Application/pdf
Source
Paper copy kept in the Centre for Newfoundland Studies, Memorial University Libraries
Local Identifier
75251332
Rights
The author retains copyright ownership and moral rights in this thesis. Neither the thesis nor substantial extracts from it may be printed or otherwise reproduced without the author's permission.
Collection
Electronic
Theses
and
Dissertations
Scanning Status
Completed
PDF File
(43.43
MB)
--
http://collections.mun.ca/PDFs/theses/March_SandraB.pdf
CONTENTdm file name
41316.cpd