the digestive system
TRANSCRIPT
The Digestive System
Human physiology
Functions of the GI Tract Motility:
▫Movement of of food through the GI tract. Ingestion:
Taking food into the mouth. Mastication:
Chewing the food and mixing it with saliva. Deglutition:
Swallowing the food. Peristalsis:
Rhythmic wave-like contractions that move food through GI tract.
Functions of the GI Tract (continued)
•Secretion:▫Includes both exocrine and endocrine
secretions. Exocrine:
HCl, H20, HC03-, bile, lipase, pepsin, amylase,
trypsin, elastase, and histamine are secreted into the lumen of the GI tract.
Endocrine: Stomach and small intestine secrete hormones to
help regulate the GI system.▫Gastrin, secretin, CCK, GIP, GLP-1, guanylin, VIP, and
somatostatin.
Functions of the GI Tract (continued)
•Digestion:▫Breakdown of food particles into
subunits (chemical structure change).•Absorption:
▫Process of the passage of digestion (chemical subunits) into the blood or lymph.
•Storage and elimination:▫Temporary storage and elimination of
indigestible food.
Digestive System (GI)
• GI tract divided into:▫ Alimentary
canal.▫ Accessory
digestive organs.
• GI tract is 30 ft long and extends from mouth to anus.
Insert fig. 18.2
Layers of GI Tract
•Composed of 4 tunics:▫Mucosa.▫Submucosa.
Muscularis.Serosa.
Mucosa•Lines the lumen of GI tract.
▫Consists of simple columnar epithelium.•Lamina propria:
▫Thin layer of connective tissue containing lymph nodules.
•Muscularis mucosae: ▫Thin layer of smooth muscle responsible for
the folds. Folds increase surface area for absorption.
•Goblet cells:▫Secrete mucus.
Submucosa•Thick, highly vascular layer of
connective tissue.•Absorbed molecules enter the blood and
lymphatic vessels.•Submucosal plexus (Meissner’s plexus):
▫Provide autonomic nerve supply to the muscularis mucosae.
Muscularis•Responsible for segmental contractions
and peristaltic movement through the GI tract.▫Inner circular layer of smooth muscle.▫Outer longitudinal layer of smooth muscle.
•Contractions of these layers move food through the tract; pulverize and mix the food.
•Myenteric plexus located between the 2 muscle layers.▫Major nerve supply to GI tract.
Fibers and ganglia from both sympathetic and parasympathetic nervous systems.
Serosa
•Binding and protective outer layer.•Consists of areolar connective tissue covered
with simple squamous epithelium.
Regulation of the GI Tract•Extrinsic innervation:
▫Parasympathetic nervous system: Vagus and spinal nerves:
Stimulate motility and GI secretions.▫Sympathetic nervous system:
Postganglionic sympathetic fibers that pass through submucosal and myenteric plexuses and innervate GI tract: Reduce peristalsis and secretory activity.
Regulation of the GI Tract (continued)
•Enteric nervous system:▫Sites where parasympathetic fibers synapse
with postganglionic neurons that innervate smooth muscle.
•Submucosal and myenteric plexuses:▫Local regulation of the GI tract.
•Paracrine secretion:▫Molecules acting locally.
•Hormonal secretion:▫Secreted by the mucosa.
From Mouth to Stomach•Mastication (chewing):
▫Mixes food with saliva which contains salivary amylase. Enzyme that can catalyze the partial digestion of starch.
•Deglutition (swallowing):▫Begins as a voluntary activity.▫Involves 3 phases:
Oral phase is voluntary. Pharyngeal and esophageal phases are involuntary.
Cannot be stopped.▫Larynx is raised.▫Epiglottis covers the entrance to respiratory
tract.
From Mouth to Stomach (continued)
•Involuntary muscular contractions and relaxations in the mouth, pharynx, larynx, and esophagus are coordinated by the swallowing center in the medulla.
•Esophagus:▫Connects pharynx to the stomach.
Upper third contains skeletal muscle. Middle third contains a mixture of skeletal and
smooth muscle. Terminal portion contains only smooth muscle.
Esophagus
• Peristalsis: ▫ Produced by a series of
localized reflexes in response to distention of wall by bolus.
• Wave-like muscular contractions:▫ Circular smooth muscle
contract behind, relaxes in front of the bolus.
▫ Followed by longitudinal contraction (shortening) of smooth muscle. Rate of 2-4 cm/sec.
▫ After food passes into stomach, LES constricts.
Insert 18.4a
Stomach•Most distensible part of GI tract.
▫Empties into the duodenum.•Functions of the stomach:
▫Stores food.▫Initiates digestion of proteins.▫Kills bacteria.▫Moves food (chyme) into intestine.
Stomach (continued)
• Contractions of the stomach churn chyme.▫ Mix chyme
with gastric secretions.
▫ Push food into intestine.
Insert fig. 18.5
Stomach (continued)
• Gastric mucosa has gastric pits in the folds.
• Cells that line the folds deeper in the mucosa, are gastric glands.
Insert fig. 18.7
Gastric Glands•Secrete gastric juice:
▫Goblet cells: mucus.▫Parietal cells: HCl and intrinsic factor.▫Chief cells: pepsinogen.▫Enterochromaffin-like cells (ECL):
histamine and serotonin.▫G cells: gastrin.▫D cells: somatostatin.▫Stomach: ghrelin.
HCl Production
• Parietal cells secrete H+ into gastric lumen by primary active transport, through H+/ K+
ATPase pump.• Parietal cell’s
basolateral membrane takes in Cl- against its electrochemical gradient, by coupling its transport with HC03
-.
Insert fig. 18.8
HCl Production (continued)
•HCl production is stimulated:▫Indirectly by gastrin.▫Indirectly by ACh.
•ACh and gastrin stimulate release of histamine.▫Histamine:
Stimulates parietal cells to secrete HCl.
HCl Functions
• Makes gastric juice very acidic.▫ Denatures
ingested proteins (alter tertiary structure) so become more digestible.
• Activates pepsinogen to pepsin.▫ Pepsin is more
active at pH of 2.0.
Insert fig. 18.9
Digestion and Absorption in the Stomach
•Proteins partially digested by pepsin.•Carbohydrate digestion by salivary
amylase is soon inactivated by acidity.•Alcohol and aspirin are the only
commonly ingested substances absorbed.
Gastric and Peptic Ulcers• Peptic ulcers:
▫ Erosions of the mucous membranes of the stomach or duodenum produced by action of HCl.
• Zollinger-Ellison syndrome:▫ Ulcers of the duodenum are produced by excessive
gastric acid secretions.• Helicobacter pylori:
▫ Bacterium that resides in GI tract that may produce ulcers.
• Acute gastritis:▫ Histamine released by tissue damage and
inflammation stimulate further acid secretion.
Protective Mechanisms of Stomach•Parietal and chief cells impermeable to
HCl.•Alkaline mucus contains HC03
-.•Tight junctions between adjacent
epithelial cells.•Rapid rate of cell division (entire
epithelium replaced in 3 days).•Prostaglandins inhibit gastric
secretions.
Small Intestine• Each villus is a fold in
the mucosa.• Covered with columnar
epithelial cells interspersed with goblet cells.
• Epithelial cells at the tips of villi are exfoliated and replaced by mitosis in crypt of Lieberkuhn.
• Lamina propria contain lymphocytes, capillaries, and central lacteal.
Insert fig. 18.12
Absorption in Small Intestine•Duodenum and jejunum:
▫Carbohydrates, amino acids, lipids, iron, and Ca2+.
•Ileum:▫Bile salts, vitamin B12, electrolytes, and
H20.
Intestinal Enzymes•Microvilli contain brush border
enzymes that are not secreted into the lumen.▫Brush border enzymes remain attached to
the cell membrane with their active sites exposed to the chyme.
•Absorption requires both brush border enzymes and pancreatic enzymes.
Intestinal Contractions and Motility
• 2 major types of contractions occur in the small intestine:▫Peristalsis:
Slow movement. Pressure at the pyloric
end of small intestine is greater than at the distal end.
▫Segmentation: Major contractile activity
of the small intestine. Contraction of circular
smooth muscle. Mix chyme.
Insert fig. 18.14
Contractions of Intestinal Smooth Muscles
• Occur automatically in response to endogenous pacemaker activity.
• Rhythm of contractions is paced by graded depolarizations called slow waves.▫ Slow waves produced by
interstitial cells of Cajal.▫ Slow waves spread from
1 smooth muscle cell to another through nexuses.
Insert fig. 18.15
Contractions of Intestinal Smooth Muscles
•When slow waves above threshold, it triggers APs by opening of VG Ca2+
channels.•Inward flow of Ca2+:
▫Produces the upward depolarization phase.▫Stimulates contraction of smooth muscle.
•Repolarization:▫VG K+ channels open.
Slow waves decrease in amplitude as they are conducted.
•May stimulate contraction in proportion to the magnitude of depolarization.
Cells and Electrical Events in the Muscularis
Insert fig. 18.16
Large Intestine• Outer surface bulges outward to form haustra.• Little absorptive function.
▫ Absorbs H20, electrolytes, several vitamin B complexes, vitamin K, and folic acid. Intestinal microbiota produce significant amounts of folic
acid and vitamin K. Bacteria ferment indigestible molecules to produce short-
chain fatty acids. Does not contain villi.
• Secretes H20, via active transport of NaCl into intestinal lumen.▫ Guanylin stimulates secretion of Cl- and H20, and
inhibits absorption of Na+ (minor pathway). Membrane contains Na+/K+ pumps.
▫ Minor pathway.
Fluid and Electrolyte Absorption in the Intestine
•Small intestine:▫Most of the fluid and electrolytes are
absorbed by small intestine. Absorbs about 90% of the remaining volume.
▫Absorption of H20 occurs passively as a result of the osmotic gradient created by active transport. Aldosterone stimulates NaCl and H20 absorption in
the ileum.•Large intestine:
▫Absorbs about 90% of the remaining volume. Absorption of H20 occurs passively as a result of the
osmotic gradient created by active transport of Na+ and Cl-.
Defecation•Waste material passes to the rectum.•Occurs when rectal pressure rises and
external anal sphincter relaxes. •Defecation reflex:
▫Longitudinal rectal muscles contract to increase rectal pressure. Relaxation of internal anal sphincter.
▫Excretion is aided by contractions of abdominal and pelvic skeletal muscles. Push feces from the rectum.
Structure of Liver
•Liver largest internal organ.▫Hepatocytes form hepatic plates that are 1–2
cells thick.▫Arranged into functional units called lobules.
•Plates separated by sinusoids.▫More permeable than other capillaries.
•Contains phagocytic Kupffer cells.•Secretes bile into bile canaliculi, which
are drained by bile ducts.
Structure of Liver (continued)
Insert fig. 18.20
Hepatic Portal System•Products of digestion that are absorbed
are delivered to the liver.•Capillaries drain into the hepatic portal
vein, which carries blood to liver.▫¾ blood is deoxygenated.▫Hepatic vein drains liver.
Enterohepatic Circulation
• Compounds that recirculate between liver and intestine.▫ Many compounds can
be absorbed through small intestine and enter hepatic portal blood.
▫ Variety of exogenous compounds are secreted by the liver into the bile ducts.
• Can excrete these compounds into the intestine with the bile.
Insert fig. 18.22
Major Categories of Liver Function
Bile Production and Secretion• The liver produces and secretes 250–1500 ml of
bile/day.• Bile pigment (bilirubin) is produced in spleen,
bone marrow, and liver.▫ Derivative of the heme groups (without iron) from
hemoglobin.• Free bilirubin combines with glucuronic acid and
forms conjugated bilirubin.▫ Secreted into bile.
• Converted by bacteria in intestine to urobilinogen.▫ Urobilogen is absorbed by intestine and enters the
hepatic vein. Recycled, or filtered by kidneys and excreted in urine.
Metabolism of Heme and Bilirubin
Insert fig. 18.23
Bile Production and Secretion (continued)
• Bile acids are derivatives of cholesterol.▫ Major pathway of
cholesterol breakdown in the body.
• Principal bile acids are:▫ Cholic acid.▫ Chenodeoxycholic acid.
Combine with glycine or taurine to form bile salts. Bile salts aggregate as
micelles.• 95% of bile acids are
absorbed by ileum.
Insert fig. 18.25
Detoxification of the Blood•Liver can remove hormones, drugs, and
other biologically active molecules from the blood by:▫Excretion into the bile.▫Phagocytosis by Kupffer cells.▫Chemical alteration of the molecules.
Ammonia is produced by deamination of amino acids in the liver.
Liver converts it into urea. Excreted in urine.
Detoxification of the Blood (continued)
•Inactivation of steroid hormones and drugs.▫Conjugation of steroid hormones and
xenobiotics make them anionic. Can be transported into bile by
multispecific organic anion transport carriers.
▫Steroid and xenobiotic receptors stimulate production of cytochrome P450 enzymes.
Secretion of Glucose, Triglycerides and Ketones•Liver helps regulate blood glucose
concentration by:▫Glycogenesis and lipogenesis.▫Glycogenolysis and gluconeogenesis.
•Contains enzymes required to convert free fatty acids into ketone bodies.
Production of Plasma Proteins•Albumin and most of the plasma
globulins (except immunoglobulins) are produced by the liver.
•Albumin:▫Constitutes 70% of the total plasma
protein. Contributes most to the colloid osmotic
pressure in the blood.•Globulins:
▫Transport cholesterol and hormones.▫Inhibit trypsin.▫Produce blood clotting factors I, II, III, V,
VII, IX, XI.
Gallbladder•Sac-like organ attached to the inferior
surface of the liver.•Stores and concentrates bile.•When gallbladder fills with bile, it expands.
▫Contraction of the muscularis layer of the gallbladder, ejects bile into the common bile duct into duodenum.
•When small intestine is empty, sphincter of Oddi closes.▫Bile is forced up to the cystic duct to gallbladder.
Pancreas
•Exocrine:▫Acini:
Secrete pancreatic juice.
•Endocrine:▫Islets of
Langerhans: Secrete
insulin and glucagon.
Insert fig. 18.26
Pancreatic Juice• Contains H20, HC03
- and digestive enzymes.
Pancreatic Juice
• Complete digestion of food requires action of both pancreatic and brush border enzymes.▫ Most pancreatic
enzymes are produced as zymogens.
▫ Trypsin (when activated by enterokinase) triggers the activation of other pancreatic enzymes.
• Pancreatic trypsin inhibitor attaches to trypsin.▫ Inhibits its activity in
the pancreas.
Fig. 18.29
Neural and Endocrine Regulation•Neural and endocrine mechanisms modify
the activity of the GI system.•GI tract is both an endocrine gland, and a
target for the action of hormones.
Regulation of Gastric Function•Gastric motility and secretion are
automatic.•Waves of contraction are initiated
spontaneously by pacesetter cells.•Extrinsic control of gastric function is
divided into 3 phases:▫Cephalic phase.▫Gastric phase.▫Intestinal phase.
Cephalic Phase•Stimulated by sight, smell, and taste of
food. •Activation of vagus:
▫Stimulates chief cells to secrete pepsinogen.
▫Directly stimulates G cells to secrete gastrin.
▫Directly stimulates ECL cells to secrete histamine.
▫Indirectly stimulates parietal cells to secrete HCl.
•Continues into the 1st 30 min. of a meal.
Gastric Phase• Arrival of food in stomach stimulates the
gastric phase.• Gastric secretion stimulated by:
▫ Distension.▫ Chemical nature of chyme (amino acids and short
polypeptides). Stimulates G cells to secrete gastrin. Stimulates chief cells to secrete pepsinogen. Stimulates ECL cells to secrete histamine.
Histamine stimulates secretin of HCl.▫ Positive feedback effect.
As more HCl and pepsinogen are secreted, more polypeptides and amino acids are released.
Gastric Phase (continued)
• Secretion of HCl is also regulated by a negative feedback effect:▫ HCl secretion
decreases if pH < 2.5.
▫ At pH of 1.0, gastrin secretion ceases. D cells stimulate
secretion of somatostatin. Paracrine
regulator to inhibit secretion of gastrin.
Insert. Fig. 18.30
Intestinal Phase•Inhibits gastric activity when chyme
enters the small intestine.•Arrival of chyme increases osmolality
and distension.▫Activates sensory neurons of vagus and
produces an inhibitory neural reflex: Inhibits gastric motility and secretion. In the presence of fat, enterogasterone inhibits
gastric motility and secretion.•Hormone secretion:
▫Inhibit gastric activity: Somatostatin, CCK, and GLP-1.
Enteric Nervous System•Submucosal and myenteric plexuses
contain 100 million neurons.•Include preganglionic parasympathetic
axons, ganglion cell bodies, postganglionic sympathetic axons; and afferent intrinsic and extrinsic sensory neurons.
Enteric Nervous System (continued)
• Peristalsis:• ACh and
substance P stimulate smooth muscle contraction above the bolus.
• NO, VIP, and ATP stimulate smooth muscle relaxation below the bolus.
Insert fig. 18.31
Paracrine Regulators of the Intestine• Serotonin (5-HT):
▫ Stimulates intrinsic afferents, which send impulses into intrinsic nervous system; and activates motor neurons.
• Motilin:▫ Stimulates contraction of the duodenum and stomach
antrum.• Guanylin:
▫ Activates guanylate cyclase, stimulating the production of cGMP. cGMP stimulates the intestinal cells to secrete Cl- and H20.
Inhibits the absorption of Na+.• Uroguanylin:
▫ May stimulate kidneys to secrete salt in urine.
Intestinal Reflexes•Intrinsic and extrinsic regulation controlled
by intrinsic and paracrine regulators.•Gastroileal reflex:
▫Increased gastric activity causes increased motility of ileum and movement of chyme through ileocecal sphincter.
•Ileogastric reflex:▫Distension of ileum, decreases gastric motility.
•Intestino-intestinal reflex:▫Overdistension in 1 segment, causes relaxation
throughout the rest of intestine.
Secretion of Pancreatic Juice• Secretion of pancreatic juice and bile is stimulated
by:• Secretin:
▫Occurs in response to duodenal pH < 4.5.▫Stimulates production of HC03
- by pancreas.▫Stimulates the liver to secrete HC03
- into the bile. • CCK:
▫Occurs in response to fat and protein content of chyme in duodenum.
▫Stimulates the production of pancreatic enzymes.▫Enhances secretin.▫Stimulates contraction of the sphincter of Oddi.
Digestion and Absorption of Carbohydrates
• Salivary amylase:▫ Begins starch
digestion.• Pancreatic amylase:
▫ Digests starch to oligosaccharides.
▫ Oligosaccharides hydrolyzed by brush border enzymes.
• Glucose is transported by secondary active transport with Na+
into the capillaries.
Insert fig. 18.32
Digestion and Absorption of Protein•Digestion begins in the stomach when
pepsin digests proteins to form polypeptides.
•In the duodenum and jejunum:▫Endopeptidases cleave peptide bonds in the
interior of the polypeptide: Trypsin. Chymotrypsin. Elastase.
▫Exopeptidases cleave peptide bonds from the ends of the polypeptide: Carboxypeptidase. Aminopeptidase.
Digestion and Absorption of Protein (continued)
• Free amino acids absorbed by cotransport with Na+.
• Dipeptides and tripeptides transported by secondary active transport using a H+ gradient to transport them into the cytoplasm.
• Hydrolyzed into free amino acids and then secreted into the blood.
Insert fig. 18.33
Digestion and Absorption of Lipids•Arrival of lipids in the duodenum serves
as a stimulus for secretion of bile.•Emulsification:
▫Bile salt micelles are secreted into duodenum to break up fat droplets.
•Pancreatic lipase and colipase hydrolyze triglycerides to free fatty acids and monglycerides.▫Colipase coats the emulsification droplets
and anchors the lipase enzyme to them.▫Form micelles and move to brush border.
Digestion and Absorption of Lipids (continued)
•Free fatty acids, monoglycerides, and lysolecithin leave micelles and enter into epithelial cells.▫Resynthesize triglycerides and
phospholipids within cell. Combine with a protein to form
chylomicrons.•Secreted into central lacteals.
Transport of Lipids•In blood, lipoprotein lipase hydrolyzes
triglycerides to free fatty acids and glycerol for use in cells.
•Remnants containing cholesterol are taken to the liver. ▫Form VLDLs which take triglycerides to cells.▫Once triglycerides are removed, VLDLs are
converted to LDLs. LDLs transport cholesterol to organs and blood
vessels.•HDLs transport excess cholesterol back
to liver.
Absorption of Fat