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The Adrenal Gland

  Atif Hassan Khirelsied, Ph.D
                        ,

   Department of Biochemistry
       Faculty of Medicine
International University of Africa
The Adrenal Glands

•   The two adrenal glands are 
                     g
    located on the anterior 
    surface above the kidneys.
                             y



•   Each gland weighs about 6 
    grams, the left adrenal is 
           th l ft d      li
    longer and thinner. 
The Adrenal Glands
The Adrenal Glands
The Adrenal Glands

The adrenal gland is compound gland, comprises 
The adrenal gland is compound gland comprises
two different endocrine tissues. 

Cross sectioning through the adrenal gland reveals 
a pale medulla in the centre  surrounded by a 
darker cortex.

Each of these two regions produces a distinctly 
Each of these two regions produces a distinctly
different group of hormones.
The cortex

• It is the outer part of the gland.

• It consists of three concentric 
  zones of cells, rich in cholesterol. 
  zones of cells rich in cholesterol




• Each zone has a characteristic arrangement of cells and 
  contains different set of enzymes, thus differ in their 
  major hormonal products.
The adrenal cortex

• Zona glomerulosa
       glomerulosa, 
  predominantly secretes 
  mineralocorticoids
  (aldosterone). 

• Zona fasiculata, the main 
  source of glucocorticoids
  source of glucocorticoids
  (cortisol) and androgens.

• Zona reticularis, produces 
  androgens
The Adrenal Gland

• The adrenal medulla (AM) is actually an extension of
  The adrenal medulla (AM) is actually an extension of 
  the sympathetic NS “special ganglion”.

   1. The splenic nerve terminates in the AM, innervates 
      the chromaffin cells.
      th h       ffi   ll

   2. Chromaffin cells produce the catecholamines.
The hormones of the adrenal medulla

• Chromaffin cells produce the catecholamines.
   1. Epinephrine
   2. Norepinepherine
   3. Dopamine.

• Th
  They are not essential for life.
                     i l f lif

• A
  Are required for adaptation to stress (acute , 
           i df     d     i             (
  chronic).

• Major element for severe stress.
The biosynthesis of catecholamines
The biosynthesis of catecholamines
Tyrosine hydroxylase
                   ,     y    yp     y        (  )
 1. Produces L‐3,4‐dihydroxyphenylalanine (L‐DOPA). 
 2. Is the rate limitting enzyme.
 3 Iron‐containing protein[ferric state(Fe2)]
 3. Iron‐containing protein[ferric state(Fe )].
 4. Exists in soluble and particle forms.
 5. Uses molecular oxygen.
 5 U          l l
 6. Requires tetrahydrobiopterin (BH4).
The biosynthesis of catecholamines
• Tyrosine hydroxylase inhibitors.
   1. Feedback inhibited by its products.
   1 Feedback inhibited by its products

   2. Can be competitively inhibited by tyrosine derivatives 
   2 Can be competiti el inhibited b t rosine deri ati es
      ( e.g., α‐methyltyrosine), used for treatment of 
      pheochromocytoma.
      pheochromocytoma

   3. Can also be inhibited by iron‐chelating agents (e.g., 
   3 C     l b i hibit d b i         h l ti       t (
      αα‐‐bipyridine).



                             22‐‐bipyridyl
The biosynthesis of catecholamines
• Aromatic L‐amino acid (Dopa) 
  decarboxylase

    Synonyms: 
  – tryptophan decarboxylase, 
  – 5‐hydroxytryptophan decarboxylase. 

      It catalyzes several different 
      decarboxylation reactions:
     • L‐DOPA to dopamine
     • 5‐HTP to serotonin
     • tryptophan to tryptamine
The biosynthesis of catecholamines
• Aromatic L‐amino acid (Dopa) decarboxylase

  1.   Soluble form.
  2.
  2    Requires pyridoxal phosphate.
       Req ires pyridoxal phosphate
  3.   Is competitively inhibited by α‐methyl dopa.
  4.   Can also be inhibited by halogenated compounds.
  5.   Anti‐hypertension drugs (methyl dopa, 3‐
       hydroxtyramine, α‐methyl tyrosine, metaraminol) 
       inhibits this enzyme .
The biosynthesis of catecholamines


• Dopamine‐β‐hydroxylase (DBH)
  1.   Converts dopamine to norepinephrine
                   p                p p
  2.   Requires ascorbic acid as e‐ donor.
  3.   Has Cu in active site. 
       Has Cu in active site.
  4.   Use fumarate as modulator
The biosynthesis of catecholamines

• Phenylethanolamine‐N‐methyl transferase (PNMT)
  Phenylethanolamine‐N‐methyl transferase
  1. Soluble in cytoplasm.
  2. Induced by glucocorticoids.
  2 I d db l             ti id
  3. Uses SAM, methyl donor.
The regulation of catecholamines synthesis

 1. Stimulated by splanchnic nerve.
 1 Stimulated by splanchnic nerve
 2. Increases after acute stress by activation of enzymes.
 3. Enzymes are induced by chronic stress (corticoids).
 3 En mes are ind ced b chronic stress (corticoids)
The storage, release and uptake of catecholamines
• Storage .
   1. Stored in the chromaffin granules
   2. Associated with ATP‐Mg2+ and Ca2+

• Release .
   1. By exocytosis (Ca2+‐dependent)
   2. Stimulated by cholinergic and β‐adrenergic
   3. Inhibited by α‐adrenergic

• Uptake.
   Neuronal uptake of the hormone is necessary for:
   1. Conservation of the hormone
   2. Termination of signal
The catecholamines receptors
• α1 .
   1. Acts via calcium.
   2. Increases glycogenolysis.
   3. Smooth muscle contraction (blood vessels, urinogenital
       tract).
       tract)

• α2.
   1.   Inhibits cAMP formation.
   2.   Smooth muscle relaxation (GIT)
   3.   Smooth muscle contraction (some vascular beds)
   4.   Inhibits:
        1.
        1    lipolysis
             li l i
        2.   Renine release
        3.   Platelets aggregation
        4.   Insulin secretion
The catecholamines receptors
• β1 .
   1. Stimulates cAMP formation
   2. Stimulates lipolysis
   3. Increases mycocardial contraction (rate and force)

• β2.
   1. Stimulates cAMP formation
   2. Increases smooth muscle contraction (bronchi, blood 
      vessels, GIT and GUT)
      vessels GIT and GUT)
   3. Increases:
         1.   Hepatic gluconeogenesis
                p     g         g
         2.   Hepatic glycogenolysis
         3.   Muscle  glycogenolysis
         4.   Release of insulin, glucagon and renin
Types of adrenergic receptors

Receptor     Effectively     Effect of Ligand          Physiologic
               Binds             Binding                 Effects

  α1       Norepinephrine,
           Norepinephrine    Increased free     ↑ vasoconstriction.
                                                  vasoconstriction
           Epinephrine.      calcium            ↑ smooth muscle
                                                contraction.
                                                ↑ skin and visceral
                                                   ki     d i      l
  α2       Norepinephrine,   Decreased cyclic   arterioles constriction.
           Epinephrine.      AMP                ↑ sphincters and pilomotor
                                                constriction.
                                                ↓ insulin secretion
Types of adrenergic receptors

Receptor     Effectively    Effect of Ligand             Physiologic
               Binds            Binding                    Effects


   β1      Epinephrine,
           E i hi         Increased cyclic
                          I       d    li      ↑ h t rate
                                                 heart t
           Norepinephrine AMP                  ↑ heart strength
                                               ↑ lipolysis.

  Β2       Epinephrine     Increased cyclic    ↑ vasodilatation.
                           AMP                 ↑ bronchodilatation.
                                               ↑ glycogenolysis.
                                                  l         l i
                                               ↑ glycolysis
                                               ↑ calorigenesis.
                                               ↑ relaxation of intestine, uterus
                                               and bladder wall.
The catecholamines mechanism of signaling

• Binding to β1 and β2
  Binding to β1 and β2 .
   1. Stimulates G‐proteins coupled to adenylate cyclase.


• Binding to α2.
  1. Inhibits adenylate cyclase.


• Binding to α1.
   1. Is coupled to phospholipase C, increases 
   1 Is coupled to phospholipase C increases
      phosphoinsitol, DAG and Ca2+.
The catabolism of catecholamines
1. Have very short t½ (10‐30 sec)

2. Less than 5% is excreted in urine

3. Catabolized by:
   1. Catechol‐o‐methyl transferase (
           h l      h l      f      (COMT) 
                                         )
   2. Monoamine oxidase
Catecholamine degradation




COMT = Catechol‐o‐methyl transferase, MAO = Monoamine oxidase, 
DOPAC = 3,4‐Dihydroxyphenylacetic acid,  MHPG = 3‐Methoxy‐4‐hydroxyphenylglycol , 
DOPAC = 3 4 Dihydroxyphenylacetic acid MHPG = 3 Methoxy 4 hydroxyphenylglycol
DHPG = 3,4 dihydroxyphenylglycol, 
VMA = Vanillylmandelic acid,  HVA = homovanillic acid (HVA,

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The adrenal gland, catecholamine synthesis