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Drugs and the
                         Brain
                         Psychotropic Medications -
                         Effects and Adverse Effects
                         Adonis Sfera, MD




Neurovascular coupling
Why Do We Get Side Effects From
Drugs?
             Any time you alter you body chemistry
             you will have some form of side effect.


             The benefits of the medication will
             often outweigh the cost of the side
             effects by improving heath or allowing
             people to function in daily life.

             It is up to us to decide.
Sometimes The Risks Do Not
Outweigh The Benefits
Current Psychotropic Drugs Are Not
“Smart” Drugs
   They travel to every area of the body including the
    brain
Let’s Follow the Drug




Brain Compartments
First Compartment: The Brain Vessels
Extracellular Space - Between
Capilaries and Cells
Second Compartment: The Space
Between The Cells
The Firewall (Blood Brain Barrier)
 The
    blood-brain barrier (BBB) is located
 between the blood vessels (capilaries)
 and the extracellular space of the brain.
Blood Brain Barrier (BBB)
 Endotelialcells
 Astrocyte endfeet

                        Trans-cellular
                        passage of drugs

                        Passage of drugs
                        from the
                        bloodstream to the
                        brain is dependent
                        on the ability of the
                        molecules to
                        penetrate through
                        cell membranes.
Crossing the Membranes
Penetration of a molecule from the bloodstream to the neurons
and glial cells is dependent on the compound's liposolubility.
Targets of psychotropic drugs

   30% of psychotropic drugs target transporter
    proteins
   30% of psychotropic drugs target G protein
    linked receptors
   20% of psychotropic drugs target ligand-
    gated ion channels
   10% of psychotropic drugs target voltage
    sensitive ion channels
   10% of psychotropic drugs target enzymes
Transporter Protein and G Protein
(60% of psychotropic drugs)




Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Ligand Gated Ion Channels, Voltage Sensitive
        Ion Channels and Enzymes
        (40% of psychotropic drugs)




Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Transporter Proteins
Transporters are receptors that bind neurotransmitters (they go in
and out of the neuronal membrane 12x)




 Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
All Antidepressants (except MAO inhibitors)
 Target and Block Transporter Proteins
Serotonin Transporter(SERT); Norepinephrine Transporter(NET);
Dopamine Transporter(DAT)
Antidepressants Bind to
        Transporters
1. When Na binds to the
transporter, serotonin also
binds and renders the
transporter ready.

2. When the antidepressant
binds to the transporter it
displaces serotonin and Na,
blocking the transporter




Stahl SM Stahl’s Essential Psychopharmacology;
The Prescriber’s Guide 4th ed 2011
G Protein Linked Receptors
G protein linked receptors (7 transmembrane regions, one intracellular
and one extracellular portion)
Ligand-Gated Ion Channels (20%
      of Psychotropic Drugs)




Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
N Methyl D Aspartate Receptors
GABA Receptors
VOLTAGE SENSITIVE CHANNELS

 Voltage -sensitive sodium channels
 Voltage-sensitive calcium channels
Voltage-Sensitive Sodium
          Channels




Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Some Mood Stabilizers’
Binding Sites




 Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Voltage-Sensitive Calcium
Channels
Alpha 2 Delta Ligands
Antihypertensive Calcium Channel
Blockers
Enzymes Directly Targeted by
          Psychotropic Drugs




   Some Enzymes Create New
   Molecules.
   Others Destroy Existing
   Molecules.



Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s
Guide 4th ed 2011
Enzymes as Targets of Psychotropic
   Drugs




Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Irreversible Enzyme Inhibitor

                                 An irreversible inhibitor of an enzyme binds
                                 to the enzyme in such a way that
                                 permanently prevents a substrate from
                                 binding.




 Stahl SM Stahl’s Essential Psychopharmacology; The
 Prescriber’s Guide 4th ed 2011
Reversible Enzyme Inhibitor
Dopamine Pathways
I wish I could inhibit only the mesolimbic pathway, but I cannot
because the drugs are not “smart”.
All antipsychotics (typical
and atypical) are
dopamine D2 blockers, but
unfortunately they affect
other receptors as well
-adverse effects




Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Tardive Dyskinesia (TD)
   Up regulation of the postsynaptic dopamine
    receptors.

   5% of patients maintained on typical
    antipsychotics will develop TD in 1 year (25%
    in 5 years).

    TD in elderly can be as high 25% in the first
    year of treatment

Kane JM in Bloom FE, Kupfer DJ, Psychopharmacology: The fourth generation of
progress. Philadelphia Raven 1996
National Alliance on Mental illness. Tardive dyskinesia Available at
www.nami.org/ContentGroups/Helpline1/Tardive_Dyskinesia.html
Question
Which of the following risk factors for the
development of TD is most important?
 Age
 Gender
 Mood disorders
 Substance abuse
Question
The estimated annual rate of TD in
olanzapine treated patients is:
 0.5%
 1.0%
 2.0%
 3%
 4%
What happens in the
Tuberoinfundibular pathway?
 With   D2 blockade

 With   5HT2A blockade
Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Cardiometabolic Syndrome
Weight gain is mediated by:
 5HT2C
 H1
 M3
Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011

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Drugs and the brain

  • 1. Drugs and the Brain Psychotropic Medications - Effects and Adverse Effects Adonis Sfera, MD Neurovascular coupling
  • 2. Why Do We Get Side Effects From Drugs? Any time you alter you body chemistry you will have some form of side effect. The benefits of the medication will often outweigh the cost of the side effects by improving heath or allowing people to function in daily life. It is up to us to decide.
  • 3. Sometimes The Risks Do Not Outweigh The Benefits
  • 4. Current Psychotropic Drugs Are Not “Smart” Drugs  They travel to every area of the body including the brain
  • 5. Let’s Follow the Drug Brain Compartments
  • 6. First Compartment: The Brain Vessels
  • 7. Extracellular Space - Between Capilaries and Cells
  • 8. Second Compartment: The Space Between The Cells
  • 9. The Firewall (Blood Brain Barrier)  The blood-brain barrier (BBB) is located between the blood vessels (capilaries) and the extracellular space of the brain.
  • 10. Blood Brain Barrier (BBB)  Endotelialcells  Astrocyte endfeet Trans-cellular passage of drugs Passage of drugs from the bloodstream to the brain is dependent on the ability of the molecules to penetrate through cell membranes.
  • 11. Crossing the Membranes Penetration of a molecule from the bloodstream to the neurons and glial cells is dependent on the compound's liposolubility.
  • 12. Targets of psychotropic drugs  30% of psychotropic drugs target transporter proteins  30% of psychotropic drugs target G protein linked receptors  20% of psychotropic drugs target ligand- gated ion channels  10% of psychotropic drugs target voltage sensitive ion channels  10% of psychotropic drugs target enzymes
  • 13. Transporter Protein and G Protein (60% of psychotropic drugs) Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 14. Ligand Gated Ion Channels, Voltage Sensitive Ion Channels and Enzymes (40% of psychotropic drugs) Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 15. Transporter Proteins Transporters are receptors that bind neurotransmitters (they go in and out of the neuronal membrane 12x) Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 16. All Antidepressants (except MAO inhibitors) Target and Block Transporter Proteins Serotonin Transporter(SERT); Norepinephrine Transporter(NET); Dopamine Transporter(DAT)
  • 17. Antidepressants Bind to Transporters 1. When Na binds to the transporter, serotonin also binds and renders the transporter ready. 2. When the antidepressant binds to the transporter it displaces serotonin and Na, blocking the transporter Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 18. G Protein Linked Receptors G protein linked receptors (7 transmembrane regions, one intracellular and one extracellular portion)
  • 19. Ligand-Gated Ion Channels (20% of Psychotropic Drugs) Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 20. N Methyl D Aspartate Receptors
  • 22. VOLTAGE SENSITIVE CHANNELS  Voltage -sensitive sodium channels  Voltage-sensitive calcium channels
  • 23. Voltage-Sensitive Sodium Channels Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 24. Some Mood Stabilizers’ Binding Sites Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 26. Alpha 2 Delta Ligands
  • 28. Enzymes Directly Targeted by Psychotropic Drugs Some Enzymes Create New Molecules. Others Destroy Existing Molecules. Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 29. Enzymes as Targets of Psychotropic Drugs Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 30. Irreversible Enzyme Inhibitor An irreversible inhibitor of an enzyme binds to the enzyme in such a way that permanently prevents a substrate from binding. Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 32. Dopamine Pathways I wish I could inhibit only the mesolimbic pathway, but I cannot because the drugs are not “smart”.
  • 33. All antipsychotics (typical and atypical) are dopamine D2 blockers, but unfortunately they affect other receptors as well -adverse effects Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 34. Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 35. Tardive Dyskinesia (TD)  Up regulation of the postsynaptic dopamine receptors.  5% of patients maintained on typical antipsychotics will develop TD in 1 year (25% in 5 years).  TD in elderly can be as high 25% in the first year of treatment Kane JM in Bloom FE, Kupfer DJ, Psychopharmacology: The fourth generation of progress. Philadelphia Raven 1996 National Alliance on Mental illness. Tardive dyskinesia Available at www.nami.org/ContentGroups/Helpline1/Tardive_Dyskinesia.html
  • 36. Question Which of the following risk factors for the development of TD is most important?  Age  Gender  Mood disorders  Substance abuse
  • 37. Question The estimated annual rate of TD in olanzapine treated patients is:  0.5%  1.0%  2.0%  3%  4%
  • 38.
  • 39. What happens in the Tuberoinfundibular pathway?  With D2 blockade  With 5HT2A blockade
  • 40. Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 41.
  • 42. Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 43. Cardiometabolic Syndrome Weight gain is mediated by:  5HT2C  H1  M3
  • 44. Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 45. Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011
  • 46.
  • 47. Stahl SM Stahl’s Essential Psychopharmacology; The Prescriber’s Guide 4th ed 2011