19. adrenal glands

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hysiology of the Adrenal Glan ysiology of the Adrenal Glan Adrenal cortex -Anatomy review -Synthesis of corticosteroids -Glucocorticoids -Mineralocorticoids -Controlling system -Renin-angiotensin system Adrenal medulla and its hormones -Synthesis and secretion -Adrenergic receptors -Physiologic effects

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Transcript of 19. adrenal glands

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Physiology of the Adrenal GlandPhysiology of the Adrenal GlandAdrenal cortex

-Anatomy review-Synthesis of corticosteroids

-Glucocorticoids-Mineralocorticoids-Controlling system

-Renin-angiotensin system

Adrenal medulla and its hormones-Synthesis and secretion-Adrenergic receptors-Physiologic effects

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The adrenal glands are situated at the upper poles of each kidneyand consist of an outer cortex surrounding a central medulla

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Adrenal cortex•Has three histological zones 1. Zona glomerulosa (produces aldosterone, mineralocorticoid) 2. Zona fasciculata and 3. Zona reticularis (both produce glucocorticoids, cortisol and corticosterone) + androgens (DHEA, DHEA sulfate)

•21 carbon atom compounds - mineralocorticoid (aldosterone) affects Na & K metabolism - glucocorticoids (cortisol & corticosterone) affect carbohydrate and protein metabolism

•19 carbon atoms - adrenal androgenes

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•Synthesis of corticosteroids

Zona glomeruloza

Pregnenolone

Progesterone

11-Deoxycorticosterone

Corticosterone

Aldosterone

Angiotensin II(18-OH Corticosterone)

(2)

(3)

(4)

(5)

Cholesterol

Pregnenolone

Progesterone

11-Deoxycorticosterone

Corticosterone

17-OHPregnenolone DHEA

Androstene-dione

(2)

(1)

17-OHProgesterone

(2)

11-Deoxy-cortisol

Cortisol

(3)

(4)

(2)

(3)

(4)

Zona fasciculata andzona reticularis

Hormone synthesis in the adrenal cortex. The zona glomerulosa can not convert corticosterone tocortisol. 1-5 indicate the enzymes responsible for hormone synthesis: 1) 17α-hydroxylase (lacking in

zona glomerulosa); 2) 3 β-dehydrogenase; 3) 21 β-hydroxylase; 4) 11 β-hydroxylase; 5) corticosteronemethyloxidase

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•Glucocorticoids - cortisol ~ 96% is bound to corticosteroid- binding globulin (CBG) or transcortin - a minor degree of binding to albumin - ~ 4% is free (biologically active) - corticosterone (secreted 1/10th amount of cortisol)

•Plasma level follows circadian rhythm: - highest between 4.00 – 8.00 am - levels secondary to variation in ACTH and circadian rhythm of CRF

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Effects of glucocorticoids

•Metabolic effects - anti-insulin - stimulate gluconeogenesis plasma glucose - plasma amino acid levels - lipolysis which causes truncal obesity

•Renal effect: - maintain GFR (glomerular filtration rate) and RPF (renal plasma flow)

•Gastric effects: - gastric flow and acid secretion - mucosal cell proliferation

•Vascular effect: - Cortisol catecholamine synthesis

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•Antigrowth effects: - growth hormone and its action on somatic growth - cause muscle atrophy and muscle weakness - Ca absorption from the gut - collagen formation osteoporosis and delayed wound healing

•Anti-inflammatory and anti-allergic effects: - capillary permeability - leucocyte migration - number of lymphocytes, monocytes, eosinophils, basophils and histamine release - number of neutrophils, erythrocytes and platelets

•Stress adaptation: - activates the hypothalamic-hypophyseal-adrenal axis - has some mineralocorticoid action – retain Na and water - exerts negative feedback effect at the level of CRF and ACTH secretion

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Effects of mineralocorticoidEffects of mineralocorticoid•Is essential for life

•Aldosterone exerts ~95% of mineralocorticoid effect

•The majority of aldosterone remains bound: - to albumin - the rest is bound to CBG

•Na retention by: - absorption of Na in distal and collecting tubules of nephrons - sweat glands - salivary glands and - GI mucosa

• K elimination

•Maintains ECF (extracellular fluid volume)

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Hypothalamic-hypophyseal-adrenal axis (control system)Hypothalamic-hypophyseal-adrenal axis (control system)

•CRF (hypothalamus) ACTH (adenohypophysis) adrenal cortex (ZG & ZF) Cortisol

• Cortisol CRF ACTH cortisol (negative feedback)•CRH-ACTH axis is activated by: - severe trauma - hemorrhage - burns - heavy exercise - pyrogens - infection and fever - hypoglycemia - chemical intoxication - histamine - pain - electrical shock - surgery - anxiety - cold exposure•Level of “free” cortisol acts on anterior pituitary and hypothalamus by negative feedback

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Higher brain centers

Hormonal Limbic system

Hypothalamus

Pituitary

CRF

Adrenal

ACTH

ACTH

Stress

Diurnal rhythm

Cortisol

-

- negativefeedback

Mineralocorticoids

Androgens/Estrogens

The hypothalamic-pituitary-adrenal axis

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Renin-angiotensin-aldosterone (control system)Renin-angiotensin-aldosterone (control system)•Renin, a proteolytic enzyme, secreted by juxtaglomerular cells (JG) of the juxtaglomerular apparatus (JGA)

•Baroreceptors and chemoreceptors of JGA are sensitive to: - hypovolemia renin - concentration of Na renin

•The renin-angiotensin system is also stimulated by: - sympathetic nervous system renin

•Hypotension renin

•Aldosterone secretion is controlled by: ECF volume BP or Na renin (JGA) angiotensin (plasma) angiotensin I angiotensin II aldosterone (zona glomerulosa) [“converting enzyme” converts ANG I to ANG II]

• K adrenal zona glomerulosa aldosterone

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Clinical

•Addison’s disease (due to destruction of adrenal gland – autoimmune disease/ tuberculosis) – primary hypoadrenalism

• ACTH melanocyte activity pigmentation of the skin + buccal mucosa

•Secondary hypoadrenalism is due to: ACTH (pituitary damage)

•Features: - weakness - anorexia - loss of weight - abdominal pain - loss of Na and water dehydration - hypercalcemia - hypotension - hyperkalemia metabolic acidosis - postural dizziness - anemia - hypoglycemia - lymphocytosis - vomiting - eosinophilia - diarrhea

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•Cushing’s syndrome – results from excess glucocorticoid activity/hypercortisolism•May be caused by - ACTH - glococorticoid secreting tumor and stunted growth•Features:•In children: arrested puberty and stunted growth•In adults: - truncal obesity - hirsutism ( androgens) - moon face - hypertension - think skin striae - altered mentation - acne - proximal muscle weakness - menstrual irregularity - osteoporosis - increased appetite - decreased libido - diabetes mellitus - poor wound healing

•Mineralocorticoid excess (primary hyperaldosteronism/Conn’s syndrom)•Features: - hypertension - headache - hypokalemia metabolic alkalosis - tateny - fatigue - polyuria and polydipsia - nocturia - escape phenomenon prevents edema - muscle weakness

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Adrenal Medullary HormonesAdrenal Medullary Hormones

•Cells in the adrenal medulla synthesize and secrete epinephrine and norepinephrine.

•The ratio of these two catecholamines differs considerably among species:

in humans, cats and chickens, roughly 80, 60 and 30% of thecatecholamine output is epinephrine.

•Following release into blood, these hormones bind adrenergicreceptors on target cells, where they induce essentially the same

effects as direct sympathetic nervous stimulation

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Synthesis and Secretion of Catecholamines

Synthesis of catecholamines begins with the amino acid tyrosine, which is taken up by chromaffin cells in the medulla and converted to norepinephrine and

epinephrine through the following steps:

Norepinephine and epinephrine are stored in electron-dense granules which alsocontain ATP and several neuropeptides.

Secretion of these hormones is stimulated by acetylcholine release from preganglionicsympathetic fibers innervating the medulla.

Many types of "stresses" stimulate such secretion, including exercise, hypoglycemiaand trauma. Following secretion into blood, the catecholamines bind loosely to and

are carried in the circulation by albumin and perhaps other serum proteins.

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Adrenergic Receptors and Mechanism of Action

•The physiologic effects of epinephrine and norepinephrine are initiated by their binding to adrenergic receptors on the surface of target cells.•These receptors are prototypical examples of seven-pass transmembrane proteins that are coupled to G proteins which stimulate or inhibit intracellular signalling pathways.

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Complex physiologic responses result from adrenal medullary stimulation becausethere are multiple receptor types which are differentially expressed in differenttissues and cells. The alpha and beta adrenergic receptors and their subtypes wereoriginally defined by differential binding of various agonists and antagnonists and,more recently, by analysis of molecular clones.

Receptor Effectively Binds Effect of Ligand Binding

Alpha1 Epinephrine, Norepinphrine Increased free calcium

Alpha2 Epinephrine, Norepinphrine Decreased cyclic AMP

Beta1 Epinephrine, Norepinphrine Increased cyclic AMP

Beta2 Epinephrine Increased cyclic AMP

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Physiologic Effects of Medullary HormonesIn general, circulating epinephrine and norepinephrine released from the

adrenal medulla have the same effects on target organs as direct stimulationby sympathetic nerves, although their effect is longer lasting.

•Increased rate and force of contraction of the heart muscle: this is predominantly an effect of epinephrine acting through beta receptors. •Constriction of blood vessels: norepinephrine, in particular, causes widespread vasoconstriction, resulting in increased resistance and hence arterial blood pressure. •Dilation of bronchioles: assists in pulmonary ventilation. •Stimulation of lipolysis in fat cells: this provides fatty acids for energy production in many tissues and aids in conservation of dwindling reserves of blood glucose. •Increased metabolic rate: oxygen consumption and heat production increase throughout the body in response to epinephrine. Medullary hormones also promote breakdown of glycogen in skeletal muscle to provide glucose for energy production. •Dilation of the pupils. •Inhibition of certain "non-essential" processes: an example is inhibition of gastrointestinal secretion and motor activity.

Common stimuli for secretion of adrenomedullary hormones include exercise,hypoglycemia, hemorrhage and emotional distress.

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