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Presented by-
Sindhu K,
M. V. Sc. Scholar, Dept. of VPT, COVAS, Pookode.
Greek: an = without
aesthesia = sensation
Anesthesiology is defined as art & science of administration of
anesthesia.
Anesthesia term coined (1846) by an American physician Oliver
Wendell Holmes, Sr. (1809-1894)
In 1975, The American College of Veterinary Anesthesiologists
was officially recognized by the American Veterinary Medical
Association as the body to certify veterinarians as specialists in
veterinary anesthesia.
To apply methods to
minimize / eliminate pain,
relax muscles,
Facilitate patient restraint during surgical, obstetrical,
medical, diagnostic & therapeutic procedures.
To monitor & support
Life functions in patients during the operative as well as in
critically ill, injured, / seriously ill patients.
Elimination of sensibility to noxious stimuli.
Humane restraint (protect animal, facilitate
diagnostic/surgical procedure).
Technical efficiency (protect personnel, facilitate
diagnostic/surgical procedures).
Specific biomedical research tool (sleep time).
Control convulsions.
Euthanasia.
Prevention of the perception of noxious stimuli (pain) during
surgery is the primary justification for anesthesia.
A noxious stimulus = stimulus that potentially damages the
body tissue.
Nociception has no emotional/perceptional connotation.
Pain is an unpleasant sensory & emotional experience; it is a
perception, not a physical entity.
Perception of pain depends  functioning cerebral cortex.
• Sensory
• Discriminative
• Motivational
• Affective
Anesthesia is produced by
 Chemicals (drugs)
 Physical (sensory nerve destruction)
According to route of administration:
Topical.
Injection.
Gastrointestinal tact.
Respiratory system.
I. Cutaneous.
II. Mucous membrane.
I. Intravenous
II. Subcutaneous
III. Intramuscular
IV. Intraperitoneal
V. Intraosseous
Oral
Rectal
I. Inhalation
Based on extent of loss of sensation
1. Local/regional: drugs placed in close proximity to nerve
membranes, causing conduction block.
Eg: topical, area infiltration, perineural, peridural,
subarachnoid.
2. General anesthesia: state of controlled, reversible CNS
depression including unconsciousness produced by
one/multiple drugs.
Eg: injectable, inhalation, balanced.
Administered usually to
conscious or mildly sedated
animals, to desensitize a
localized or regional area of
the body.
It is deposited in close
proximity to nerve membrane
causing nerve conduction
blockade.
 GA is a condition induced by pharmacological or other means
that results in controlled, reversible CNS depression.
 Basic elements of GA:
I. Reversibility
II. Unconsciousness
III. Amnesia
IV. Analgesia
V. Muscle relaxation
VI. Immobility
A favorable anesthetic course begins with good plan – a
plan based on sound pharmacological & physiological
principles.
Anesthetic management = physiology of respiration +
circulatory + central + autonomic nervous system.
Pre-anesthetic period.
Anesthetic period/ peri-anesthetics period.
Post-anesthetic period.
Tranquilizer-sedative (Acepromazine, benzodiazepines).
Hypnotic sedatives (pentobarbital & chloral hydrate).
Opioid (agonist-morphine & meperidine, agonist-antagonist-
butorphanol).
Alpha-adrenergic agonist (xylazine, detomidine,
medetomidine).
Dissociative (ketamine)
Parasympatholytics (atropine & glycopyrrolate).
Sedative drugs (telozol = tiletamine + zolazepam).
 Administration of anesthesia requires a combination of
knowledge + skill+ ingenuity.
 Given by inhalation / injections.
 Classification
Hypnotic sedatives
Dissociative
Opioid
Tranquilizer-sedatives
Balanced anesthetics.
 Also known as anesthetic recovery period.
 Hazards of immediate postanesthetic period:
Circulatory system complication  arterial hypo- & hypertension,
cardiac dysrhythmias.
Respiratory system complications  hypoxemia, hypercapnia
Pain  nociception
Emergency excitement  physical trauma
Hyper-/hypothermia
Vomiting
Delayed awakening.
• Used clinically act by interfering with the effectiveness of the
endogenous neurotransmitter Ach to activate nicotinic
cholinergic receptors of skeletal muscle cells, thereby
inhibiting receptor-coupled transmembrane ion movements
necessary for muscle contraction. (Bouzat et al. 2004: Unwin
2005).
• End result = skeletal muscle paralysis + muscle relaxation.
• Most often used as adjuvants to anesthesia to facilitate
tracheal intubation, abdominal muscle relaxation, orthopedic
manipulations & as a part of balanced anesthesia procedure to
reduce the amount of GA required in high-risk patients.
A direct alteration of the effectiveness
of Ach to activate postjunctional
receptors.
According to the mechanisms of
postjunctional action, neuromuscular
blocking agents are classified as
I. competitive (nondepolarising)
agent.
II. depolarizing agent.
 Drugs compete with Ach for available cholinergic receptors at
postsynaptic membrane & by occupying these receptors, prevent the
transmitter function of Ach.
 Prototype: d-tubocurarine (Tubocurarine chloride, USP, Tubarine).
 Metocurine Iodide, USP (Metubine).
 Gallamine Triethiodide, USP, (Flaxedil) gallamine.
 Pancuronium Bromide, Pavulon, Pancuronium.
 Synthetic compound: alcuronium, atracurium.
 Vecuronium, a derivative of pancuronium.
Drugs exert their skeletal muscle paralyzing effects
by interfering with Ach-mediated depolarization of
the post synaptic membrane.
Prototype: Succinylcholine chloride USP (quelcin,
anectine, sucostrin, suxamethonium).
Decamethonium bromide, USP (syncurine, C-10)
Muscle paralysis head & neck muscles (head drop)  tail 
limb muscles deglutition & laryngeal muscles  abdominal
muscles  intercostal muscles  diaphragm.
Recovery usually proceeds in the reverse sequence (Hall, 1971).
Unique among anesthetic drugs
because of ease in administration & in large
part removed from the body, via the lungs.
Used widely for anesthetic management of
animals due to their pharmacokinetic
characteristics favors predictable & rapid
adjustment of anesthetic depth.
Specialized apparatus is used to deliver the
inhaled agents, helps minimize patient
morbidity/mortality  facilitates accurate &
controlled anesthetic delivery, lung
ventilation & improved arterial oxygenation.
 Group I : agents in current use for animals.
Volatile halothane, isoflurane, desflurane, sevoflurane.
Gas nitrous oxide (N2o)
 Group II : gaseous agent under investigation
Xenon
 Group III : volatile agents of immediate past use/ interest.
Enflurane
Methoxyflurane
Diethylether
 Provide rapid means of producing sedation/anesthesia in
veterinary patients.
 Advantage of injectable anesthetic over inhalation  the ability
to proceed more rapidly through stage II anesthesia (the
excitement stage).
 These agent allows a more rapid control of airway, smooth
induction of anesthesia, rapid control & reduction in CNS
activity, unobstructed visualization of URT for surgical
procedures.
 For large animal (horses), preventing the excitement stage is
paramount for the animal’s safety + medical personnel.
Physiological properties  unconsciousness, amnesia,
analgesia & skeletal muscle relaxant.
Pharmacological properties  margin of safety/
therapeutic index, short duration of action &
noncumulative, readily metabolized & excreted ideally by
> one route, a specific & complete reversal of anesthesia.
Ideal drug  chemically stable, long shelf life,
physiological pH, nontoxic vehicle & inexpensive.
I. Barbiturates.  (thiopental, pentobarbital, amobarbital &
phenobarbital.)
II. Non barbiturates – non dissociative anesthetics.
a. Phenol derivatives (propofol & fospropofol)
b. Imidazole derivatives (etomidate & metomidate)
c. Neurosteroids (alfaxalone-alfadolone & alfaxalone-CD)
d. Benzodiazepines (midazolam, diazepam & lorazepam)
e. Opiods, neuroleptanalgesics & neuroleptanalgesthics.
(fentanyl, fentanyl+droperidol, methadone+acepramazine+nitrous
oxide.)
f. Miscellaneous i/v anesthetics [chloralhydrate, Guaifenesin (triple
drip), chloralose, propranidid, tribromoethanol, urethane]
III. Dissociative anesthetics  (ketamine, phencyclidine &
tiletamine).
Classification Compounds Clinical
applications
Ultra short acting Thiopental, thiamylal,
thialbarbital, hexobarbital,
methohexital.
As general anesthetic
Short acting Pentobarbital, secobarbital. As hypnotic, pre-anesthetic &
emergency management of
seizures.
Intermediate acting Amobarbital, aprobarbital,
mephobarbital.
As hypnotic, pre-anesthetic &
emergency management of
seizures.
Long acting Barbital, phenobarbital. As anticonvulsant &
sedatives.
An anesthetic state caused from interruption of
ascending transmission from the unconscious to conscious part of
the brain.
Characterized by  catalepsy.
 somatic analgesia.
 intact ocular+laryngeal+pharengeal
reflexes.
 control of the airway may not be complete, intubation with a
cuffed endotracheal tube is recommended.
Commonly used  induction + maintenance of anesthesia in cats
& dogs.
 CNS acting drugs which decreases activity, moderate excitement,
produce drowsiness & calm the recipient.
 Drugs having capacity to decrease the CNS activity  calming &
drowsiness.
 Clinical indication  to produce restrain.
 to facilitate handling + transport.
 to modify behavior of animals.
 Sedative = non specific ~ general CNS depressants.
I. Hypnotic-sedatives/ Classical sedatives.
II. Tranquilliser-sedatives/Tranquillisers (ataractics, neuroleptics).
I. Benzodiazepines  diazepam, midazolam, lorazepam.
II. Alpha2 adrenoceptor agonists  xylazine, detomidine,
medetomidine, romifidine & clonidine.
III. Barbiturates  barbital, phenobarbital, amobarbital,
secobarbital, pentobarbital.
IV. Chloral derivatives  chloral hydrate.
V. Aldehydes  paraldehyde.
VI. Inorganic salts  sodium bromide, potassium bromide &
magnesium sulphate.
VII.Miscellaneous agents  ethyl alcohol, ethchlorvynol,
glutethimide, methyprylon, ethinamate & meprobamate.
I. Phenothiazines  chlorpromazine, acepromazine,
promazine, piperacetazine, triflupromazine.
II. Thioxanthenes  chlorprothixene, clopenthixol, thiothixene.
III. Butyrophenones  azaperone, droperidol, fluanisone.
Diverse group of drugs used primarily in the treatment of
epilepsy.
It is important to 1st approach epilepsy as a manifestation of an
underlying disease.
When the underlying cause of disease cannot be identified
(idiopathic epilepsy) or treated  management of epilepsy is
primarily based on control of seizures with anticonvulsant drugs.
Major molecular target of commercially available drugs
Voltage gated sodium channels.
GABA a receptors.
The GAT-1 GABA transporter.
GABA transaminase.
I. Barbiturates  phenobarbital, pentobarbital & mephobarbital.
II. Deoxybarbiturates  primidone
III. Hydantoins  phenytoin, mephenytoin, ethotoin, fosphenytion.
IV. Benzodiazepines  clonazepam, diazepam, lorazepam, oxazepam,
clorazepate.
V. Aliphatic carboxylic acids  valoproic acid & sodium valproate
VI. Bromides  potassium bromide & sodium bromide
VII.Succimides  ethosuximide, methsuximide, phensuximide &
mesuximide
VIII.GABA analogues  gabapentin, vigabatrin, pregabalin,
progabide
IX. Dicarbamates  felbamate & meprobamate
X. Sulphonamides  zonisamide, acetazolamide, methazolamide &
sultiame
XI. Pyrrolidines  levetiracetam, brivaracetam & seletracetam
XII. Carboxamides  carbamazepine, oxcarbazepine, eslicarbazepine
& rufinamide
XIII. Oxazolidinediones  trimethadione, paramethadione & etadione.
XIV. Miscellaneous agents  topiramate, lamotrigine, valpromide,
beclamide, lacosamide, paraldehyde, tiagabine, stiripentol &
valnoctamide.
Veterinary clinical ethology  A relatively new branch of vet. Medicine
dealing with study of customs & behaviour of animals in their natural
habitat.
Behaviour is a complex phenomenon.
It is not easy to define in terms of normal & abnormal behaviour.
Adverse behaviour in animals  disease condition (neural disorders).
 lack of socialization & training.
 genetically determined.
Classification of behaviour disorders on basis of their origin.
Genetic problems, developmental & age related problems, instinctive &
species related problems, socialization/ social behaviour related
problems, disease related problems & adaptation problems.
Sr. no. Behaviour disorder Etiology
1 Aggression Dominance, competition, fear, learned, idiopathic &
feeling of uncertainty.
2 Anxiety Separation, travelling, new place & unfriendly
environment.
3 Fear/phobia Thunderstorms, gunshots, fireworks, heavy vehicle’s
engine noise.
4 Destruction Fear anxiety, over activity & reaction to arousing
stimuli.
5 Excessive vocalization Frustrated social/sexual environment, aggression &
reaction to external stimuli.
6 Elimination behaviour
(urination/defecation)
Marking territory, urine spraying (cats), submission,
excitement, lack of training & separation.
7 Sexual behaviour Hyper-sexuality, lack of libido, false pregnancy.
8 Self mutilation Attention getting & stress response.
9 stereotypies Stress response & compulsive behaviour.
Abnormal behaviour in man/animal is closely related to
alterations in concentrations of various neurotransmitters
Biogenic amines
Acetylcholine
Excitatory AA
Inhibitory AA
A wide variety of drugs from different pharmacological classes
are employed to modify abnormal behaviour in animals 
Psychotropic drugs, anticonvulsants, hormonal preparations,
CNS stimulants, artificial pheromones & miscellaneous drugs.
Algesia = ill-defined, unpleasant sensation,
usually evoked by external / internal noxious stimulus.
Physiological pain  nociceptive pain.
Pathological pain  neurogenic & cancer pain.
Opioids  potent analgesic agents, which induces analgesia by
stimulation of central opioid receptors.
Classified into
I. Opioid agonists.
II. Opioid mixed agonist-antagonists & partial agonists.
I. Natural opium alkaloids  morphine & codeine.
II. Semi-synthetic opioids  diacetylmorphine, hydromorphine,
oxymorphone, hydrocodone, oxycodone, etorphine.
III. Synthetic opioids
1. Phenylpiperidines (pethidine, ketobemidone, prodine, allylprodine,
anileridine).
2. Anilidopiperidines (fentanyl, alfentanil, carfentanil, sufentanil).
3. Diphenylpropylamine derivatives (methadone, propoxyphene,
dextromoramide, dipipanone, loperamide & diphenoxylate).
4. Morphinans (levorphanol & levomethorphan).
5. Benzomorphans (phenazocine).
6. Miscellaneous drugs (tramadol, tapentadol & tilidine).
I. Semi-synthetic opioids (buprenorphine & nalbuphine).
II. Synthetic opioids
1. Morphinans (butorphanol).
2. Benzomorphans (pentazocine, dezocine & cyclazocine).
3. Miscellaneous agents (meptazinol).
Drugs which stimulate the CNS/improves specific brain
functions.
Classification  pyscostimulants / cerebral stimulants
 brain stem stimulants / analeptics
 convulsants
 psychotomimetics / hallucinogens
 Small animal clinical pharmacology: D. M. Boothe. (2nd ed.)
 Veterinary Pharmacology and Therapeutics: Jim E Riviere & Mark G Papich.
(9th ed.)
 Veterinary pharmacology and therapeutics: H. R. Adams. (8th ed.)
 Essentials of veterinary pharmacology & therapeutics: H. S. Sandhu. (2nd
ed.)
 Google images.

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Drugs acting on CNS (veterinary)

  • 1. Presented by- Sindhu K, M. V. Sc. Scholar, Dept. of VPT, COVAS, Pookode.
  • 2. Greek: an = without aesthesia = sensation Anesthesiology is defined as art & science of administration of anesthesia. Anesthesia term coined (1846) by an American physician Oliver Wendell Holmes, Sr. (1809-1894) In 1975, The American College of Veterinary Anesthesiologists was officially recognized by the American Veterinary Medical Association as the body to certify veterinarians as specialists in veterinary anesthesia.
  • 3. To apply methods to minimize / eliminate pain, relax muscles, Facilitate patient restraint during surgical, obstetrical, medical, diagnostic & therapeutic procedures. To monitor & support Life functions in patients during the operative as well as in critically ill, injured, / seriously ill patients.
  • 4. Elimination of sensibility to noxious stimuli. Humane restraint (protect animal, facilitate diagnostic/surgical procedure). Technical efficiency (protect personnel, facilitate diagnostic/surgical procedures). Specific biomedical research tool (sleep time). Control convulsions. Euthanasia.
  • 5. Prevention of the perception of noxious stimuli (pain) during surgery is the primary justification for anesthesia. A noxious stimulus = stimulus that potentially damages the body tissue. Nociception has no emotional/perceptional connotation. Pain is an unpleasant sensory & emotional experience; it is a perception, not a physical entity. Perception of pain depends  functioning cerebral cortex.
  • 6. • Sensory • Discriminative • Motivational • Affective
  • 7. Anesthesia is produced by  Chemicals (drugs)  Physical (sensory nerve destruction)
  • 8. According to route of administration: Topical. Injection. Gastrointestinal tact. Respiratory system.
  • 10. I. Intravenous II. Subcutaneous III. Intramuscular IV. Intraperitoneal V. Intraosseous
  • 13. Based on extent of loss of sensation 1. Local/regional: drugs placed in close proximity to nerve membranes, causing conduction block. Eg: topical, area infiltration, perineural, peridural, subarachnoid. 2. General anesthesia: state of controlled, reversible CNS depression including unconsciousness produced by one/multiple drugs. Eg: injectable, inhalation, balanced.
  • 14. Administered usually to conscious or mildly sedated animals, to desensitize a localized or regional area of the body. It is deposited in close proximity to nerve membrane causing nerve conduction blockade.
  • 15.  GA is a condition induced by pharmacological or other means that results in controlled, reversible CNS depression.  Basic elements of GA: I. Reversibility II. Unconsciousness III. Amnesia IV. Analgesia V. Muscle relaxation VI. Immobility
  • 16. A favorable anesthetic course begins with good plan – a plan based on sound pharmacological & physiological principles. Anesthetic management = physiology of respiration + circulatory + central + autonomic nervous system. Pre-anesthetic period. Anesthetic period/ peri-anesthetics period. Post-anesthetic period.
  • 17. Tranquilizer-sedative (Acepromazine, benzodiazepines). Hypnotic sedatives (pentobarbital & chloral hydrate). Opioid (agonist-morphine & meperidine, agonist-antagonist- butorphanol). Alpha-adrenergic agonist (xylazine, detomidine, medetomidine). Dissociative (ketamine) Parasympatholytics (atropine & glycopyrrolate). Sedative drugs (telozol = tiletamine + zolazepam).
  • 18.  Administration of anesthesia requires a combination of knowledge + skill+ ingenuity.  Given by inhalation / injections.  Classification Hypnotic sedatives Dissociative Opioid Tranquilizer-sedatives Balanced anesthetics.
  • 19.  Also known as anesthetic recovery period.  Hazards of immediate postanesthetic period: Circulatory system complication  arterial hypo- & hypertension, cardiac dysrhythmias. Respiratory system complications  hypoxemia, hypercapnia Pain  nociception Emergency excitement  physical trauma Hyper-/hypothermia Vomiting Delayed awakening.
  • 20. • Used clinically act by interfering with the effectiveness of the endogenous neurotransmitter Ach to activate nicotinic cholinergic receptors of skeletal muscle cells, thereby inhibiting receptor-coupled transmembrane ion movements necessary for muscle contraction. (Bouzat et al. 2004: Unwin 2005). • End result = skeletal muscle paralysis + muscle relaxation. • Most often used as adjuvants to anesthesia to facilitate tracheal intubation, abdominal muscle relaxation, orthopedic manipulations & as a part of balanced anesthesia procedure to reduce the amount of GA required in high-risk patients.
  • 21. A direct alteration of the effectiveness of Ach to activate postjunctional receptors. According to the mechanisms of postjunctional action, neuromuscular blocking agents are classified as I. competitive (nondepolarising) agent. II. depolarizing agent.
  • 22.  Drugs compete with Ach for available cholinergic receptors at postsynaptic membrane & by occupying these receptors, prevent the transmitter function of Ach.  Prototype: d-tubocurarine (Tubocurarine chloride, USP, Tubarine).  Metocurine Iodide, USP (Metubine).  Gallamine Triethiodide, USP, (Flaxedil) gallamine.  Pancuronium Bromide, Pavulon, Pancuronium.  Synthetic compound: alcuronium, atracurium.  Vecuronium, a derivative of pancuronium.
  • 23. Drugs exert their skeletal muscle paralyzing effects by interfering with Ach-mediated depolarization of the post synaptic membrane. Prototype: Succinylcholine chloride USP (quelcin, anectine, sucostrin, suxamethonium). Decamethonium bromide, USP (syncurine, C-10)
  • 24. Muscle paralysis head & neck muscles (head drop)  tail  limb muscles deglutition & laryngeal muscles  abdominal muscles  intercostal muscles  diaphragm. Recovery usually proceeds in the reverse sequence (Hall, 1971).
  • 25. Unique among anesthetic drugs because of ease in administration & in large part removed from the body, via the lungs. Used widely for anesthetic management of animals due to their pharmacokinetic characteristics favors predictable & rapid adjustment of anesthetic depth. Specialized apparatus is used to deliver the inhaled agents, helps minimize patient morbidity/mortality  facilitates accurate & controlled anesthetic delivery, lung ventilation & improved arterial oxygenation.
  • 26.  Group I : agents in current use for animals. Volatile halothane, isoflurane, desflurane, sevoflurane. Gas nitrous oxide (N2o)  Group II : gaseous agent under investigation Xenon  Group III : volatile agents of immediate past use/ interest. Enflurane Methoxyflurane Diethylether
  • 27.  Provide rapid means of producing sedation/anesthesia in veterinary patients.  Advantage of injectable anesthetic over inhalation  the ability to proceed more rapidly through stage II anesthesia (the excitement stage).  These agent allows a more rapid control of airway, smooth induction of anesthesia, rapid control & reduction in CNS activity, unobstructed visualization of URT for surgical procedures.  For large animal (horses), preventing the excitement stage is paramount for the animal’s safety + medical personnel.
  • 28. Physiological properties  unconsciousness, amnesia, analgesia & skeletal muscle relaxant. Pharmacological properties  margin of safety/ therapeutic index, short duration of action & noncumulative, readily metabolized & excreted ideally by > one route, a specific & complete reversal of anesthesia. Ideal drug  chemically stable, long shelf life, physiological pH, nontoxic vehicle & inexpensive.
  • 29. I. Barbiturates.  (thiopental, pentobarbital, amobarbital & phenobarbital.) II. Non barbiturates – non dissociative anesthetics. a. Phenol derivatives (propofol & fospropofol) b. Imidazole derivatives (etomidate & metomidate) c. Neurosteroids (alfaxalone-alfadolone & alfaxalone-CD) d. Benzodiazepines (midazolam, diazepam & lorazepam) e. Opiods, neuroleptanalgesics & neuroleptanalgesthics. (fentanyl, fentanyl+droperidol, methadone+acepramazine+nitrous oxide.) f. Miscellaneous i/v anesthetics [chloralhydrate, Guaifenesin (triple drip), chloralose, propranidid, tribromoethanol, urethane] III. Dissociative anesthetics  (ketamine, phencyclidine & tiletamine).
  • 30.
  • 31. Classification Compounds Clinical applications Ultra short acting Thiopental, thiamylal, thialbarbital, hexobarbital, methohexital. As general anesthetic Short acting Pentobarbital, secobarbital. As hypnotic, pre-anesthetic & emergency management of seizures. Intermediate acting Amobarbital, aprobarbital, mephobarbital. As hypnotic, pre-anesthetic & emergency management of seizures. Long acting Barbital, phenobarbital. As anticonvulsant & sedatives.
  • 32. An anesthetic state caused from interruption of ascending transmission from the unconscious to conscious part of the brain. Characterized by  catalepsy.  somatic analgesia.  intact ocular+laryngeal+pharengeal reflexes.  control of the airway may not be complete, intubation with a cuffed endotracheal tube is recommended. Commonly used  induction + maintenance of anesthesia in cats & dogs.
  • 33.  CNS acting drugs which decreases activity, moderate excitement, produce drowsiness & calm the recipient.  Drugs having capacity to decrease the CNS activity  calming & drowsiness.  Clinical indication  to produce restrain.  to facilitate handling + transport.  to modify behavior of animals.  Sedative = non specific ~ general CNS depressants. I. Hypnotic-sedatives/ Classical sedatives. II. Tranquilliser-sedatives/Tranquillisers (ataractics, neuroleptics).
  • 34. I. Benzodiazepines  diazepam, midazolam, lorazepam. II. Alpha2 adrenoceptor agonists  xylazine, detomidine, medetomidine, romifidine & clonidine. III. Barbiturates  barbital, phenobarbital, amobarbital, secobarbital, pentobarbital. IV. Chloral derivatives  chloral hydrate. V. Aldehydes  paraldehyde. VI. Inorganic salts  sodium bromide, potassium bromide & magnesium sulphate. VII.Miscellaneous agents  ethyl alcohol, ethchlorvynol, glutethimide, methyprylon, ethinamate & meprobamate.
  • 35. I. Phenothiazines  chlorpromazine, acepromazine, promazine, piperacetazine, triflupromazine. II. Thioxanthenes  chlorprothixene, clopenthixol, thiothixene. III. Butyrophenones  azaperone, droperidol, fluanisone.
  • 36. Diverse group of drugs used primarily in the treatment of epilepsy. It is important to 1st approach epilepsy as a manifestation of an underlying disease. When the underlying cause of disease cannot be identified (idiopathic epilepsy) or treated  management of epilepsy is primarily based on control of seizures with anticonvulsant drugs. Major molecular target of commercially available drugs Voltage gated sodium channels. GABA a receptors. The GAT-1 GABA transporter. GABA transaminase.
  • 37.
  • 38. I. Barbiturates  phenobarbital, pentobarbital & mephobarbital. II. Deoxybarbiturates  primidone III. Hydantoins  phenytoin, mephenytoin, ethotoin, fosphenytion. IV. Benzodiazepines  clonazepam, diazepam, lorazepam, oxazepam, clorazepate. V. Aliphatic carboxylic acids  valoproic acid & sodium valproate VI. Bromides  potassium bromide & sodium bromide VII.Succimides  ethosuximide, methsuximide, phensuximide & mesuximide VIII.GABA analogues  gabapentin, vigabatrin, pregabalin, progabide
  • 39. IX. Dicarbamates  felbamate & meprobamate X. Sulphonamides  zonisamide, acetazolamide, methazolamide & sultiame XI. Pyrrolidines  levetiracetam, brivaracetam & seletracetam XII. Carboxamides  carbamazepine, oxcarbazepine, eslicarbazepine & rufinamide XIII. Oxazolidinediones  trimethadione, paramethadione & etadione. XIV. Miscellaneous agents  topiramate, lamotrigine, valpromide, beclamide, lacosamide, paraldehyde, tiagabine, stiripentol & valnoctamide.
  • 40. Veterinary clinical ethology  A relatively new branch of vet. Medicine dealing with study of customs & behaviour of animals in their natural habitat. Behaviour is a complex phenomenon. It is not easy to define in terms of normal & abnormal behaviour. Adverse behaviour in animals  disease condition (neural disorders).  lack of socialization & training.  genetically determined. Classification of behaviour disorders on basis of their origin. Genetic problems, developmental & age related problems, instinctive & species related problems, socialization/ social behaviour related problems, disease related problems & adaptation problems.
  • 41. Sr. no. Behaviour disorder Etiology 1 Aggression Dominance, competition, fear, learned, idiopathic & feeling of uncertainty. 2 Anxiety Separation, travelling, new place & unfriendly environment. 3 Fear/phobia Thunderstorms, gunshots, fireworks, heavy vehicle’s engine noise. 4 Destruction Fear anxiety, over activity & reaction to arousing stimuli. 5 Excessive vocalization Frustrated social/sexual environment, aggression & reaction to external stimuli. 6 Elimination behaviour (urination/defecation) Marking territory, urine spraying (cats), submission, excitement, lack of training & separation. 7 Sexual behaviour Hyper-sexuality, lack of libido, false pregnancy. 8 Self mutilation Attention getting & stress response. 9 stereotypies Stress response & compulsive behaviour.
  • 42. Abnormal behaviour in man/animal is closely related to alterations in concentrations of various neurotransmitters Biogenic amines Acetylcholine Excitatory AA Inhibitory AA A wide variety of drugs from different pharmacological classes are employed to modify abnormal behaviour in animals  Psychotropic drugs, anticonvulsants, hormonal preparations, CNS stimulants, artificial pheromones & miscellaneous drugs.
  • 43. Algesia = ill-defined, unpleasant sensation, usually evoked by external / internal noxious stimulus. Physiological pain  nociceptive pain. Pathological pain  neurogenic & cancer pain. Opioids  potent analgesic agents, which induces analgesia by stimulation of central opioid receptors. Classified into I. Opioid agonists. II. Opioid mixed agonist-antagonists & partial agonists.
  • 44. I. Natural opium alkaloids  morphine & codeine. II. Semi-synthetic opioids  diacetylmorphine, hydromorphine, oxymorphone, hydrocodone, oxycodone, etorphine. III. Synthetic opioids 1. Phenylpiperidines (pethidine, ketobemidone, prodine, allylprodine, anileridine). 2. Anilidopiperidines (fentanyl, alfentanil, carfentanil, sufentanil). 3. Diphenylpropylamine derivatives (methadone, propoxyphene, dextromoramide, dipipanone, loperamide & diphenoxylate). 4. Morphinans (levorphanol & levomethorphan). 5. Benzomorphans (phenazocine). 6. Miscellaneous drugs (tramadol, tapentadol & tilidine).
  • 45. I. Semi-synthetic opioids (buprenorphine & nalbuphine). II. Synthetic opioids 1. Morphinans (butorphanol). 2. Benzomorphans (pentazocine, dezocine & cyclazocine). 3. Miscellaneous agents (meptazinol).
  • 46.
  • 47. Drugs which stimulate the CNS/improves specific brain functions. Classification  pyscostimulants / cerebral stimulants  brain stem stimulants / analeptics  convulsants  psychotomimetics / hallucinogens
  • 48.
  • 49.
  • 50.  Small animal clinical pharmacology: D. M. Boothe. (2nd ed.)  Veterinary Pharmacology and Therapeutics: Jim E Riviere & Mark G Papich. (9th ed.)  Veterinary pharmacology and therapeutics: H. R. Adams. (8th ed.)  Essentials of veterinary pharmacology & therapeutics: H. S. Sandhu. (2nd ed.)  Google images.