Gastric Function PDF

Summary

This document provides an overview of gastric function, including the arrangement of the gastric mucosa, its functions, the types of cells involved, and the mechanisms controlling secretion during various phases. It is a summary of gastric function, not an examination paper.

Full Transcript

GASTRIC SECRETION
 Gastric Mucosa
* Arranged in folds or rugae covered by simple
columnar epithelium.

* Opening onto the surface  gastric pits- 100 /cm2
lined by surface mucus cells.

* 3 – 7 tubular glands empty into each gastric pit.
 Functions of Stomach
1. Storage of ingested meal.
2. Regulate rate of emptying into small intestine.
3. Mix contents of stomach.

4. Dissolve meal  chemical action of HCL.
5. Inhibit bacterial growth  by acid.
6. Provide intrinsic factor for vitamin B12
absorption.
 Four cell types make up the gastric mucosa:
1. Parietal (Oxyntic) Cells:
- HCL secretion.
- Intrinsic Factor.

2. Chief (Zymogen) Cells:
- Pepsinogen secretion.

3. Mucus Neck Cells:
- Mucus secretion.
4. Argentaffin Cells:
? Uncertain function.
 Stomach is divided into Three Areas:

Cardia Fundic Pyloric

Mucus secreting All 4 cell types -Mucus mainly
Cells -Gastrin(G-cells)

- ↑↑HCL
- ↑↑Pepsinogen
- ↑↑Intrinsic Factor
 Gastric Juice:
* Normal secretion  1.5 – 2 L /day.
- Exact amount determined by quantity & quality
of ingested food.

* Isotonic.

* Rates:
- With a decreased rate  main cation is Na+.
- With an increased rate  Na+ replaced by H+.

* Ph may drop < Ph 1.
* Chief cells →→secrete    Pepsins (I,II,III)

secreted as

Cholinergic Gastrin Histamine Pepsinogens
Impulse (Inactive form)
HCL
Pepsins

* Lipase enzyme  Small amount for fat digestion.
(cellular origin is unknown!)
* Parietal cells secrete  Intrinsic Factor (macromolec.polyp.)

- I.F + Vit. B12 Cobalamine complex→absorbed in ileum

Deficiency of I.F

Pernicious Anaemia.
 CONTROL OF GASTRIC SECRETION
Stimulation of Gastric secretion
Gastric secretion is controlled through:
1. Neural Stimulation :    Extrinsic Nerves
   Intrinsic Nerves

2. Hormonal Stimulation :   G.I.T Hormones

* Both mechanisms(1&2) involved in the gastric
secretory response to a meal.
 NEURAL STIMULATION
CEPHALIC PHASE:
* Vagal impulses release acetylcholine from nerve
endings in the neighbourhood of the acid & pepsin
producing cells    Secrete.

* Tonic impulses in the vagus nerve →→ Basal or
continuous secretion of gastric juice.

* Eating   Immediate & profound stimulation.
* Impulses in the vagus N Aroused reflexly by the
Sight, Odour & Taste of Palatable Food.

* ↑↑ increase in acid secretion  Exposure to :
appetizing meal or (anticipation) + strong
response
to a meal of choice. (see fig.)

* No response to a meal dutifully eaten.

* Psychic Stimulation  Maximal Acid Secretion.
 GASTRIC PHASE:
1) Nervous Stimulation after Distension of Fundus:
* Distention of oxyntic gland area (by food) :
 Copious Acid & Pepsinogen secretion.

This response is partially suppressed

If oxyntic area is extrinsically denervate (Both Afferent
& Efferent are in the vagus nerve.)

↠Another reflex is local through intrinsic plexuses
2) The Pyloro-Oxyntic Reflex:
* Acid secretion in response to antral distension.

* This is a gastrin independent mechanism.

* The stimulus is mediated by a long reflex Vago-
Vagal & a short reflex  Local.

* This mechanism operates only in patients with
Duodenal Ulcer i.e not in normal humans.

* Marked Acid response in patients with active D.U
Regulation of
Gastric Activity
 HORMONAL STIMULATION
▪ In 1905, Edkins → Food stuffs released from the
pyloric area   a chemical substance which
stimulates oxyntic cells.

* I.V. injections of extracts of pyloric mucosa
result
in increased gastric secretion.
* Extracts of oxyntic gland area  No response.

*  The chemical substance is named GASTRIN
 Stimulation of Gastrin Release:
* Gastrin  released by the antrum (pyloric) by 3
mechanisms:
A- Mechanical
B- Chemical Stimulation
C- Vagal

A- Mechanical:
* Mechanical distension of the antrum
↑Gastrin.

* Exists in the absence of nervous pathways betw-
een the pyloric & the fundic gland.
B- Chemical:
* Various secretagogues(e.g. meat extracts) ↑Gastrin
+ some chemical compounds:

1) Small peptides & āā  Most important natural
stimulants.

2) Acetylcholine.

3) Adrenaline: thro. β-adrenergic receptors:
 Important in causing Stress Ulcer.
4) Elevation of serum ca++.

5) Bile Acids Importance in causing Gastric
ulcer
in pts. with significant duodeno-gastric reflux.

6) Coffee.
7) Alcohol.

C- Vagal:
* Gastrin  The only G.I. hormone released by
direct neural stimulation.
 Inhibition of Gastrin Release:
* Gastrin secretion in response to all stimuli is :
 inhibited at a pH < 3 in the antrum.

- This mechanism  main form of feedback auto-
regulation of gastric secretion. HOW?

- During interdigestive period → pH of antrum is
low & gastrin is inhibited:

- On eating  Vagus stimulates Acid secretion:.. Food buffers, neutralizes & dilutes gastric acid:
This removes inhibition of Gastrin release i.e.
Gastrin is released + Mechanical & chemical
stimuli effects:

∴Released Gastrin ↑Acid ↑Gastric Acidity i.e
pH < 3   Inhibiting Gastrin Release.
 Interaction of Vagal & Gastrin Stimulation:
* The Pavlov pouch is more sensitive to gastrin
stimulation & responds with a great output of
gastric juice than Heidenhain pouch.

i.e. Gastric glands become more sensitive when
under the influence of the Vagus nerve.

i.e. Synergism exists between gastrin & the physio-
logical vagal excitation of the acid-secreting
glands.
 Histamine & Gastric Secretion:
* Histamine is widely distributed in the body.

* Its actions divided into 2 groups according to
type of receptors:
a) H1 Receptor : contraction of gut & bronchial
smooth muscle  blocked by antihistamines.

b) H2 Receptor: e.g. gastric acid secretion blocked
by  e.g. Cimitidine (Tagamet).

* Histamine blockers on H2 receptor also inhibit
the response due to gastrin & vagal stimulation.
 Conclusion:

* For full response   Interaction of Histamine
with Acetylcholine & Gastrin would be needed.

* This explains why Vagotomy also decreases the
gastric acid response to Histamine.
 Vagus Gastrin Producing
producing
Vagus
cell
cells
Histamine
Histamineproducing
producing
Inhibited cell
Cell
by
Vagotomy inhibited by inhibited by
cimitidine secretin
Acetylcholine Histamine Gastrin

Inhibited by
Atropine Synergistic Effect

Oxyntic cell
HCL Full Response
 CONTROL OF GASTRIC SECRETION
Inhibition of Gastric secretion
* Chyme entering the duodenum  Stimulates the
release of 2 G.I. hormones:
1. Secretin 2. Cholecystokinin(CCK)

Inhibition by Secretin:
* Secretin released into blood when Acid is introd-
uced into the duodenum(S-cells)  stimulates
pancreatic secretion.
* I.V. injection of secretin  blocks completely the
stimulation of gastric secretion in the
Heidenhain
pouch in response to a meal.

* The major inhibitory effect of secretin on gastric
secretion is exerted on  gastrin-producing cells.

i.e Secretin is the nature’s Antiacid
 Inhibition by CCK:
* CCK is released by āā & fatty acids when they
reach duodenum(I-cells).

* CCK is chemically similar to Gastrin :

Competitive Inhibition of gastric secretion
 Inhibition by other Intestinal Polypeptides:
1. Somatostatin.

2. Bulbogastrone.

3. Gastric Inhibitory Polypeptide (GIP).

4. Vasoactive Intestinal Polypeptide (VIP).

5. Glucagon.
 Factors Increasing HCL Secretion in D.U. Pts:
1) More parietal cells i.e. ↑capacity to secrete Acid.

2) More secretion of Acid at rest & in response to
stimulants like histamine, a meal etc…

3) 2 or 3 times more gastrin activity per gram of
antral mucosa than normals.

4) Ulcer pts. release more gastrin than normals.

5) Gastrin release is not suppressed normally by
antral acidification.