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Title: Prezentace aplikace PowerPoint

1
ANXIOLYTIC
and SEDATIVE- HYPNOTIC DRUGS
Prof. Martínková 2006
2
Anxiolytic and sedative-hypnotic drugs
A sedative-hypnotic drug (terminology) Sedation
can be defined as a supression of
responsiveness to a constant level of
stimulation, with decreased spontaneous
activity and ideation.
3
Anxiolytic and hypnotic drugs
A h y p n o t i c drug should produce
drowsiness and encourage the onset and
maintenance of a state of sleep that as far as
possible resembles the natural state of sleep.
H y p n o t i c effects involve more
pronounced depression of the CNS than s e d a t
i o n, and this can be achieved with most
sedative drugs simply by
increasing the dose.
4
Anxiolytic and hypnotic drugs
A n x i e t y In anxiety states the fear
response to threatening stimuli occur in an
anticipatory manner independently of external
events. Among other the fear response includes
defensive behaviours, autonomic reflexes, arousal
and alertness, corticoid secretion and negative
emotions. An effective anxiolytic agent
should reduce anxiety and
exert a calming effect - sedation - with
little or no effect on motor and menthal
function.
5
Anxiolytic and hypnotic drugs (Fig 1)
Graded dose-dependent depression of the CNS
function is a characteristic of
sedative-hypnotics. However, individual drugs
differ in the relationship between the dose and
the degree of CNS depression (see Fig 1). The
linear slope for drug A is typical of many of the
older sedative-hypnotics. With such drugs, an
increarse in dose above that needed for hypnosis
may lead to a state of general anesthesia. At
still high doses, sedative-hypnotics may depress
respiratory and vasomotor centres in the medulla,
leading to coma and death.
6
Anxiolytic and hypnotic drugs (Fig 1)
Deviation from a linear dose-response
relationship, as shown for drug B, will require
proportionately greater dosage increments in
order to achive CNS depression more profound
than hypnosis. This appears to be the case for
most drugs of the benzodiazepine class, and the
greater margin of safety is an important reason
for their clinical use to treat anxiety states
and sleep disorders.
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8
Anxiolytic and hypnotic drugs
Anxiety disorders include - generalised
anxiety disorder (an ongoing state of excessive
anxiety lacking any clear reason ) - panic
disorder (attacks of overwhelming fear
occuring in association with somatic symptoms
(sweating, tachycardia, chest pain) - phobias
(strong fears of specific things or situation
(snakes, flying) - postraumatic stress disorder
(anxiety triggered by insistent recall of
past stressful experiences
9
Anxiolytic and hypnotic drugs

In most developed countries anxiolytic drugs are
among the most frequently prescribed drugs
Classes
benzodiazepines
newer drugs
5 -HT1A -receptor agonists (buspiron)
zolpidem, zaleplon
miscellaneous other drugs
older sedative-hypnotics
barbiturates (obsolete)

10
Anxiolytic and hypnotic drugs

benzodiazepines
Pharmacodynamics(BZ) act selectively
on gamma-aminobutyric acid A (GABAA) receptors,
which mediate fast inhibitory synaptic
transmission through the CNS. They bind
specifically to a regulatory site of the
receptor, distinct from the GABA binding site and
act allosterically to increase the affinity of
GABA for the receptors.
By facilitating the opening of GABA
activated chloride-channels BZ enhance the
response to GABA.
The antagonist f l u m a z e n i l

11
Anxiolytic and hypnotic drugs
Fig 2 A model of the GABAA receptor-chloride ion
channel macromolecular complex. The complex
consists of five or more membrane-spanning
subunits. GABA appears to interact with alpha or
beta subunits triggering chloride channel opening
with resultant membrane hyperpolarization. Binding
of BZs to gamma subunits facilitates the process
of channel opening.
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Anxiolytic and hypnotic drugs - benzodiazepines
(BZ)

Pharmacokinetics
absorption well absorbed if given orally , Cmax
reached in about 1 h
binding strongly bound to plasma proteins
distribution large Vd accumulation in body
fat (high
lipid solubility)
metabolism (Fig 2)
hydroxylation
conjugation with glucuronic acid
short-, medium- and long-acting BZ
the role of N-desmethyldiazepam

14
Anxiolytic and hypnotic drugs - benzodiazepines
(BZ)
Fig. 3
15
Anxiolytic and hypnotic drugs benzodiazepines
(BZ)

Fig. 3 demonstrates
the short-acting drugs are those that are
metabolised directly by conjugation with
glucuronide.
gradual bild-up and slow disappearance of
nordazepam from the plasma gives long-acting
drugs.
Remember AGE advancing age affects the rate of
oxidative reactions more than that of
conjugation.
the effect of long-acting BZs tends to
increase with age (drowsiness and confusion)

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17
Anxiolytic and hypnotic drugs benzodiazepines
(BZ)

Pharmacological effects and uses
The main effects
reduction of anxiety and agression
sedation and induction of sleep
reduction of muscle tone and coordination
anticonvulsant effects
anterograde amnesia

18
Anxiolytic and hypnotic drugs benzodiazepine
(BZ)

reduction of anxiety and agression
Note BZ may paradoxically produce an increase
in irritability and aggression in some
individuals
(particularly if short- acting drugs are given
(triazolam)
sedation and induction of sleep
BZs decrease the time taken to get to sleep
increase the total duration of sleep
(only in subjects who normally sleep for less
than about 6 hours each night)

19
Anxiolytic and hypnotic drugs benzodiazepines
(BZ)
REM sleep ( rapid eye movement) is less affected
if compared with the same effect of other
hypnotics. Is that important? Yes, artificial
interruption of REM sleep causes irritability and
anxiety even if the total amount of sleep is not
reduced).
20
Anxiolytic and hypnotic drugs benzodiazepines
(BZ)

reduction of muscle tone and coordination
may be clinically useful increased muscle tone
is a common feature of anxiety states and may
contribute to pains (headache). Influence of
manual skills (!)
anticonvulsant effects (GABAA receptors)
clonazepam to treat epilepsy
diazepam (i.v.) status epilepticus to control
life-threatening seizures
anterograde amnesia
BZs obliterate memory of events experienced while
under their influence

21
Anxiolytic and hypnotic drugs benzodiazepines
(BZ)

Unwanted effects
acute overdosage
effects occuring during normal therapeutic use
tolerance and dependence
acute overdosage (BZs are relatively safe in
overdose)
BZs produce prolonged sleep, without serious
depression of respiration or cardiovascular
function
Severe even life-threatening respiratory
depression may appear in BZ combination with
other CNS depressants, particularly alcohol.
Acute overdosage can be counteracted with
flumazenil

22
Anxiolytic and hypnotic drugs benzodiazepines
(BZ)

unwanted effects occuring during therapeutic use
---Influence of manual skills (such as driving
performance) due to drowsiness, confusion,
amnesia and impaired coordination
--- enhance of depressant action of other drugs
(in a more than additive way)
tolerance , dependence
Tolerance (gradual escalation of dose needed to
produce the required effect) occurs with all BZs.
T.appears to represent a change at the receptor
level.
Dependence In human subjects and patients,
stopping BZ treatment after weeks and months
causes an increase in symptoms of anxiety,
together with tremor and dizziness.

23
Anxiolytic and hypnotic drugs benzodiazepines
(BZ)
The withdrawal syndrome short acting BZs cause
more abrupt withdrawal effects Addiction
(-craving -severe psychological dependence) is
not a major problem.
24
Anxiolytic and hypnotic drugs - 5 -HT1A -receptor
agonists

newer drugs
5 -HT1A -receptor agonists
Buspiron-anxiolytic effects take days or weeks to
develop.That is the most distinctive drug in
terms of antianxiety actions, since these are
achieved with minimal effects on psychomotor
functions.
Unwanted effects
appear to be less troublesome dizziness, nauzea,
headache,
not sedation or loss of coordination

25
Anxiolytic and hypnotic drugs zoplidem, zaleplon

Zolpidem pharmacodynamics
binds selectively to the BZ1 subtype of BZ
receptors and
facilitates GABA-mediated neuronal inhibition
like the BZs, the actions of zolpidem are
antagonised by
f l u m a z e n i l
minimal muscle relaxing and anticonvulsant
effects
the risk of development of tolerance and
dependence
with extended use is less than with the use
of
hypnotic BZs
pharmacokinetics
rapidly metabolized to inactive metabolites by
the liver, T1/2 1.5-3.5 h. Dosage reduction in
hepatic dysfuction, elderly.

26
Anxiolytic and hypnotic drugs zoplidem, zaleplon
Ind- short-term treatment of insomnia Zaleplon
resembles zolpidem, t1/2 1h Rapid onset and
short duration of action are favorable properties
for those patients who have difficulty falling
asleep.
27
Anxiolytic and hypnoptic drugs miscellaneous
other drugs
miscellaneous other drugs- older
sedative-hypnotics meprobamate,
glutethimide rarely used
28
Anxiolytic and hypnotic drugs barbiturates (BA)