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A New Piperazinobiguanide Series Effective Against Syphacia Obvelata in Mice
A
NEW
PIPERAZINOBIGUANIDE
AGAINST
SERIES
SYPHACIA
OBVELATA
EFFECTIVE IN
MICE
K.C. SINGHAL Department of Pharniwology,
J.N. Medical College, Aligarh, India
Acccpted February
Brown derivatives
et al (1) and Harfenist against
study by screening by Chan
Syphacia
et al (2) have evaluated
obeeelata in mice.
more of these derivatives.
(3) was used to obtain
relatively
water
together
500 mg/kg
weight.
with gum acacia
on the day of treatment day following
body
It was thought
uniform
Each
infection Drugs
the treatment.
and administered
Contents
worthwhile exposure in mice.
orally.
of caecum
of piperazine to extend
method
in 0.5 ml of distilled
Autopsy
and rectum
mice
in doses of
The mice were allowed was carried
were brushed
water and worm count was done against
this
described
The infected
were administered
dose was suspended
and were fasted again the next day.
into a petri dish containing
a large number
The laboratory
were fasted for one day prior to drug treatment. 100, 200 and
21, 1975
food on the
out gently
a black background.
SHORT
COMMUNICATIONS
Japan. J. Pharmacol. 25, 353 (1975)
TABLE1.
The dose response was estimated according to the proportion of mice cleared of infection and compared with piperazine citrate which served as the standard.
The approximate
LD50 of active compounds was determined on albino mice weighing between 20-25 G. Table I summarizes the results. at 200 mg/kg dose.
PPb (N-phenyl) cleared all the mice of S. obvelata
The lower dose of 100 mg/kg did not show any effect.
PPb (N-ac'
pip), in which phenyl ring is substituted for the acetyl group, was found ineffective up to a dose of 500 mg/kg. PPb (N-0-tolyl), with methyl group at ortho position, exhibited a dose dependent response. kg.
It cleared 82.5 % of the mice of their infection at a dose of 100 mg/
This effect was equal to that observed with 200 mg/kg of piperazine citrate.
PPb
(N-p-tolyl) in which the methyl group is substituted in the para position cleared 100% mice of their infection at 500 mg/kg dose. The lower dose of 200 mg/kg was found to be in effective. None of the seven quinazolone derivatives tested for anthelmintic
activity against
S. ohvelata, was found to be active up to a dose of 500 mg/kg orally (Table 1). The presence of a phenyl substitution in the biguanide derivative of piperazine ap pears essential for anthelmintic activity.
This is evident from the observation that its
SHORT replacement
COMMUNICATIONS
by the acetyl group
sent findings are not in parallel
results
Japan. J. Pharmacol. 25, 354 (1975)
in abolition
with the conclusions
of the activity,
base and its simple salts are more effective against S. obrelata stituted position vity.
compounds. enhances However,
Further, the activity,
substitution
of a methyl group
while substitution
1).
The pre
than are more complex
activity
as is evident from the column
sub
in the phenyl ring at ortho
at the para position,
with the increase in the anthelmintic
toxicity of the compounds
(Table
of Brown et al (1) that the piperazine
decreases
the acti
there is also an increase in
3 of Table 1.
REFERENCES 1) BROWN,H.W., CHAN, K.F. AND 1-IussAY,K.L.: Ain. J. Trop. Med. Hvg., 3, 504-510, 1954; 2) HARFENIST,M., FANELLI,R.V., BALTZLY,R., BROWN,H.W., HUSSAY,K.L. AND CHAN, K.F.: J. Pharmacol. exp. Ther., 121, 347-353, 1957; 3) CHAN, K.F.: Am. J. Hyg., 56, 22-30, 1952
NEW
PIPERAZINOBIGUANIDE
AGAINST
SERIES
SYPHACIA
OBVELATA
EFFECTIVE IN
MICE
K.C. SINGHAL Department of Pharniwology,
J.N. Medical College, Aligarh, India
Acccpted February
Brown derivatives
et al (1) and Harfenist against
study by screening by Chan
Syphacia
et al (2) have evaluated
obeeelata in mice.
more of these derivatives.
(3) was used to obtain
relatively
water
together
500 mg/kg
weight.
with gum acacia
on the day of treatment day following
body
It was thought
uniform
Each
infection Drugs
the treatment.
and administered
Contents
worthwhile exposure in mice.
orally.
of caecum
of piperazine to extend
method
in 0.5 ml of distilled
Autopsy
and rectum
mice
in doses of
The mice were allowed was carried
were brushed
water and worm count was done against
this
described
The infected
were administered
dose was suspended
and were fasted again the next day.
into a petri dish containing
a large number
The laboratory
were fasted for one day prior to drug treatment. 100, 200 and
21, 1975
food on the
out gently
a black background.
SHORT
COMMUNICATIONS
Japan. J. Pharmacol. 25, 353 (1975)
TABLE1.
The dose response was estimated according to the proportion of mice cleared of infection and compared with piperazine citrate which served as the standard.
The approximate
LD50 of active compounds was determined on albino mice weighing between 20-25 G. Table I summarizes the results. at 200 mg/kg dose.
PPb (N-phenyl) cleared all the mice of S. obvelata
The lower dose of 100 mg/kg did not show any effect.
PPb (N-ac'
pip), in which phenyl ring is substituted for the acetyl group, was found ineffective up to a dose of 500 mg/kg. PPb (N-0-tolyl), with methyl group at ortho position, exhibited a dose dependent response. kg.
It cleared 82.5 % of the mice of their infection at a dose of 100 mg/
This effect was equal to that observed with 200 mg/kg of piperazine citrate.
PPb
(N-p-tolyl) in which the methyl group is substituted in the para position cleared 100% mice of their infection at 500 mg/kg dose. The lower dose of 200 mg/kg was found to be in effective. None of the seven quinazolone derivatives tested for anthelmintic
activity against
S. ohvelata, was found to be active up to a dose of 500 mg/kg orally (Table 1). The presence of a phenyl substitution in the biguanide derivative of piperazine ap pears essential for anthelmintic activity.
This is evident from the observation that its
SHORT replacement
COMMUNICATIONS
by the acetyl group
sent findings are not in parallel
results
Japan. J. Pharmacol. 25, 354 (1975)
in abolition
with the conclusions
of the activity,
base and its simple salts are more effective against S. obrelata stituted position vity.
compounds. enhances However,
Further, the activity,
substitution
of a methyl group
while substitution
1).
The pre
than are more complex
activity
as is evident from the column
sub
in the phenyl ring at ortho
at the para position,
with the increase in the anthelmintic
toxicity of the compounds
(Table
of Brown et al (1) that the piperazine
decreases
the acti
there is also an increase in
3 of Table 1.
REFERENCES 1) BROWN,H.W., CHAN, K.F. AND 1-IussAY,K.L.: Ain. J. Trop. Med. Hvg., 3, 504-510, 1954; 2) HARFENIST,M., FANELLI,R.V., BALTZLY,R., BROWN,H.W., HUSSAY,K.L. AND CHAN, K.F.: J. Pharmacol. exp. Ther., 121, 347-353, 1957; 3) CHAN, K.F.: Am. J. Hyg., 56, 22-30, 1952