Catecholamines Flashcards

1
Q

Catecholamines

A
  • Molecules w/ benzene rings containing 2 adjacent hydroxyl residues and a side chain amine
  • Are synthesized from tyrosine
  • Liver controls availability of tyrosine and its precursor phenylalanine
  • Tyr can also be obtained from high-protein foods
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2
Q

Biosynthesis of tyrosine

A
  • Phe is converted to Tyr by phenylalanine hydroxylase
  • Mutations in this nz can lead to accumulation of neurotoxic phenylketones (phenylketonuria, or PKU)
  • Decarboxylation of phe leads to phenylethylamine, which is elevated in the crises of paranoid schizophrenics
  • Tyrosine decarboxylation leads to tyramine (sympathomimetic), which has actions similar to epinephrine (is also present in cheese, beer, wine, chocolate)
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3
Q

Biosynthesis of L-DOPA

A
  • Tyr hydroxylase (TH) converts tyr into L-DOPA, this is the rate-limiting step in catecholamine (CA) synthesis
  • TH is most important nz in CA synthesis
  • TH is in all cells capable of synthesizing CAs
  • TH inhibited by AA analogs (alpha-methyltyrosine), CA-derivatives, Fe chelators, and lead
  • Short-term regulation of TH activity occurs thru phosphorylation (increasing activity)
  • Long-term regulation of TH thru transcriptional regulation by NTs, hormones, caffeine, and nicotine
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4
Q

Biosynthesis of dopamine (DA)

A
  • Action of DOPA decarboxylase, aromatic acid or dihydroxyphenylalanine decarboxylase (AADC) converts L-DOPA into DA
  • Vit B6 is cofactor
  • Nzs are present in excess
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5
Q

Biosynthesis of dopamine (DA)

A
  • Action of DOPA decarboxylase, aromatic acid or dihydroxyphenylalanine decarboxylase (AADC) converts L-DOPA into DA
  • Vit B6 is cofactor
  • Nzs are present in excess
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6
Q

Biosynthesis of norepinephrine (NE)

A
  • Synthesized from dopamine beta-hydroxylase nz, requires vit C, Cu, O2
  • NE plays important role in sleep, arousal, attention, vigilance, learning, and memory
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7
Q

Catecholamine catabolism 1

A
  • Monoamine oxidases (MAO) convert the amino group to aldehyde (two types: A and B)
  • MAO is preceded by or followed by COMT, then followed by aldehyde reductase, to produce a hydroxyl group from the aldehyde, or by aldehyde dehydrogenase, to produce a carboxyl group
  • 1-deprenyl is a MAO-B inhibitor and can increase the T1/2 of DA
  • Smoking inhibits MAO-B activity, increasing the T1/2 of DA and could be relevant to addiction
  • Nicotine also stimulates the cholinergic receptors on DA neurons causing them to fire APs and release DA
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8
Q

MAO mutations

A
  • Abnormal and violent behavior in a family is associated w/ a point mutation in the MAO-A gene
  • Pts do not have detectable amounts of HVA (CA breakdown product) and low amounts of 5HIA (serotonin breakdown product)
  • MAO-B does not compensate for loss of MAO-A
  • MAO-B KO in mice lead to submissive behavior
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9
Q

MAO mutations

A
  • Abnormal and violent behavior in a family is associated w/ a point mutation in the MAO-A gene
  • Pts do not have detectable amounts of HVA (CA breakdown product) and low amounts of 5HIA (serotonin breakdown product)
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10
Q

DA and NE catabolism

A
  • Principle metabolite of DA after action of MAO + COMT followed by aldehyde dehydrogenase is homovanillic acid (HVA)
  • HVA is an indicator of DA activity in the CNS
  • Principle metabolite of NE after the action of MAO + COMT + aldehyde dehydrogenase is 3-methyle-4-hydroxyphenol-glycol (MHPG)
  • MHPG is an indicator of NE activity in the CNS
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11
Q

DA and NE catabolism

A

-Principle metabolite of DA after action of MAO + COMT followed by aldehyde dehydrogenase is homovanillic acid (HVA)

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12
Q

DA systems of the brain

A
  • DA neurons that originate in substantia nigra project to the striatum
  • Those that originate in VTA project to nucleus accumbens (NA), cerebral cortex, and hypothalamus
  • DA in NA is where the DA rush occurs, associated w/ drugs, sex, and risk-taking
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13
Q

DA storage and release

A
  • DA release requires an influx of Ca ions and the fusion of synaptic vessels
  • Membrane potentials and DA synthesis/release can be regulated by presynaptic receptors
  • DAT (dopamine transporter) reuptakes DA into presynaptic cells
  • DAT inhibited by cocaine
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14
Q

DA receptors

A
  • 5 major types and all are GPCRs
  • D1 and D5: stimulate cAMP synthesis by AC
  • D2-4: inhibit cAMP synthesis by AC
  • Present in presynaptic cells to regulate NT release
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15
Q

Other compounds affecting CA pathways

A
  • Alpha-methyltyrosine: inhibits TH and prevents CA production
  • Reserpine: blocks DA uptake (VMAT) and storage
  • Amphetamine: stimulates release of DA and blocks its uptake
  • Cocaine: inhibits DAT
  • Pargyline: inhibitor of MAO
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16
Q

Other compounds affecting CA pathways

A
  • Alpha-methyltyrosine: inhibits TH and prevents CA production
  • Reserpine: blocks DA uptake and storage
  • Amphetamine: stimulates release of DA and blocks its uptake
17
Q

DA receptor and schizophrenia

A

-D4 receptor bp repeats lead to increased susceptibility to delusional disorder