Module 8 - Drugs Acting on GIT.pptx

Full Transcript

Module 8
Drugs Acting on the
Gastrointestinal System

MA. ROCHELLYN F. MAPA, RN
Instructor
Drugs and GI System
GIT is basically a hollow, muscular
tube that begins at the mouth and
ends at the anus
encompasses the pharynx, stomach,
and the small and large intestines
to digest and absorb food and fluids and
excrete metabolic wastes
Lesson 1
Antiulcerant Drugs

MA. ROCHELLYN F. MAPA, RN
Instructor
Antacids
group of inorganic chemicals that
neutralize stomach acid
OTC
used alone or with combination with other
drugs to treat peptic ulcers*
include magnesium hydroxide, aluminum
hydroxide, simethicone, magaldrate
(aluminum- magnesium complex),
calcium carbonate, sodium
bicarbonate**
Antacids
Pharmacokinetics
neutralize gastric acid*
distributed throughout the GIT and are
eliminated primarily in the feces

Pharmacodynamics
the acid-neutralizing action of antacids
reduces the total amount in the GIT
allowing peptic ulcers time to heal**
Antacids
Pharmacotherapeutics
used alone or with other drugs to relieve pain
and
promote healing in PUD
relieve symptoms of acid indigestion,
heartburn, dyspepsia or GERD*

Drug Interactions
interfere with the absorption of oral drugs if
given at the same time
absorption of digoxin, iron salts, isoniazid,
quinolones, and tetracyclines may be reduced
if taken within 2 hours of antacids
 H2 Receptor
Antagonists
H2 blockers
commonly prescribed include
cimetidine, nizatidine, ranitidine
and famotidine

Pharmacokinetics
cimetidine, nizatidine, and ranitidine
are absorbed rapidly and
completely from GIT
famotidine is not absorbed
completely
food and antacids may reduce
absorption
distributed widely through the body,
metabolized by the liver and excreted in
H2 Receptor
Antagonists
Pharmacodynamics
block histamine from stimulating the acid-
secreting parietal cells of the stomach
blocking gastric acid secretions and
promote healing of
ulcer by eliminating its cause*

Pharmacotherapeutics
treatment of active duodenal ulcer or
benign
gastric ulcer
treatment of pathologic GI hypersecretory* conditions
such as Zollinger-Ellison Syndrome**
reduce gastric acid production and prevent stress ulcers in
severely ill patients and in those with reflux esophagitis or
upper GI bleeding***
H2 Receptor
Antagonists
Drug Interactions
antacids reduce the absorption of
cimetidine, nizatidine, and famotidine
cimetidine may increase the blood levels
of oral anticoagulants, propranolol,
benzodiazepines, TCAs, theophylline,
procainamide, quinidine, lidocaine,
phenytoin, calcium channel blockers,
cyclosporine, carbamazepine and
narcotic analgesics by reducing their
metabolism in the liver and subsequent
excretion
cimetidine inhibits metabolism of ethyl
alcohol in the stomach, resulting in
higher blood alcohol levels
H2 Receptor
Antagonists
Adverse

Reactions
headache, dizziness, malaise, muscle pain,
nausea, diarrhea or constipation, rashes,
itching, loss of sexual desire and impotence
famotidine and nizatidine produce few adverse
reactions with headache as the most common
followed by constipation or diarrhea and rash
Proton Pump Inhibitors
disrupt the chemical binding in the
stomach cells to reduce acid production,
lessening irritation and allowing peptic
ulcers to better heal*
include rabeprazole, pantoprazole,
omeprazole, lansoprazole,
esomeprazole**

Pharmacokinetics
given orally in enteric-coated formulas to
bypass the stomach because they’re
highly acid labile
when in small intestine, they are
dissolved, and absorption is rapid
highly protein-bound and are extensively
Proton Pump Inhibitors
Pharmacodynamics
block the last step in the secretion of
gastric acid by combining with hydrogen,
potassium and adenosine triphosphate in
the parietal cells of the stomach*

Pharmacotherapeutics
short term treatment of active gastric
ulcers, active duodenal ulcers, erosive
esophagitis, symptomatic GERD that is
not responsive to other therapies, active
peptic ulcers associated with H. pylori
infection in combination with antibiotics,
long term treatment of hypersecretory
states such as Zollinger-Ellison syndrome
Proton Pump Inhibitors
Drug Interactions
interfere with the metabolism of diazepam,
phenytoin and warfarin causing increased half-
lives and elevated plasma concentrations of
these drugs

Contraindications
known allergy to the drug or its components
caution in pregnant or lactating women*

Side Effects and Adverse Reactions**
CNS effects of dizziness and headache are
common; GI effects include abdominal pain,
diarrhea, nausea and vomiting, dry mouth and
tongue atrophy; URT symptoms include cough,
Other Peptic Ulcer Drugs
Sucralfate
gastrointestinal protectant
works locally in the stomach, rapidly
reacting with hydrochloric acid to form a
thick, paste-like substance that adheres to
the gastric mucosa and especially to
ulcers*
also inhibits pepsin activity in gastric juices,
preventing further breakdown of proteins
in the stomach, including the protein wall
of the stomach
rapidly absorbed after oral administration,
metabolized in the liver, and excreted in the
feces; it crosses the placenta and may enter
breast milk
Other Peptic Ulcer Drugs
Sucralfate
should not be given to any person with known
allergy to the drug or any of its components to
prevent hypersensitivity reactions
should not be given to individuals with renal
failure or undergoing dialysis*
caution in patients who are pregnant or
lactating**
adverse effects associated with this drug are
primarily related to its GI effects such as
constipation***, diarrhea, nausea, indigestion,
gastric discomfort, and dry mouth; others include
dizziness, sleepiness, vertigo, skin rash, and back
pain
if aluminum salts are combined with sucralfate, there
is a risk of high aluminum levels and aluminum
Other Peptic Ulcer Drugs
Misoprostol
synthetic prostaglandin*
inhibits gastric acid secretion and
increases bicarbonate and mucus
production in the stomach thus
protecting the stomach lining
primarily used to prevent NSAID-induced
gastric ulcers in patients who are at risk
for complications from a gastric ulcer**
given orally; rapidly absorbed from the
GIT, metabolized in the liver, and
excreted in the urine; crosses placenta
and enters breast milk
Other Peptic Ulcer Drugs
Misoprostol
contraindicated to patients with allergy to
any part of the drug
contraindicated during pregnancy because
it is an abortifacient
caution should be used during lactation and in
patients with hepatic or renal impairment*
adverse effects associated with this drug are
primarily related to its GI effects – nausea,
diarrhea, abdominal pain, flatulence, vomiting,
dyspepsia, and constipation; Genitourinary
effects – which are related to the actions of
prostaglandins on the uterus, include
miscarriages, excessive bleeding, spotting,
cramping, hypermenorrhea, dysmenorrhea, and
Lesson 2

Laxatives
MA. ROCHELLYN F. MAPA,RN
Instructor
Chemical Stimulants
directly stimulate the nerve plexus in the
intestinal wall, causing increased
movement and the stimulation of local
reflexes
include bisacodyl (Dulcolax), cascara,
castor oil, and senna (Senokot)

Pharmacokinetics
most of these agents are minimally
absorbed and exert their therapeutic
effect directly in the GIT*
castor oil has an onset of action of 2-
6 hrs; 6-8 hrs (others)**
Chemical Stimulants
Pharmacotherapeutics
castor oil is used when a thorough
evacuation of the intestine is desired*
bisacodyl acts in a similar manner but is
somewhat milder in effect; can also be
given in a water enema to stimulate the
activity in lower GIT
cascara is milder than castor oil and is often
used
when effects are needed overnight
senna is available orally in tablet and
syrup form and as a rectal suppository
Chemical Stimulants
Contraindications and Cautions
allergy to any component of the drug*
acute abdominal disorders (appendicitis, diverticulitis,
and ulcerative colitis)**
use with caution in patients with heart block,
coronary artery disease, or debilitation***
use with caution in pregnancy and lactation*

Adverse Effects
GI effects such as diarrhea, abdominal cramping, and
nausea (most common)
CNS effects such as dizziness, headache, and
weakness**
sweating, palpitations, flushing and fainting***
cathartic dependence*
Bulk Stimulants
also known as mechanical stimulants
rapid-acting, aggressive laxatives that
cause the fecal matter to increase in
bulk*
include magnesium sulfate (Epsom salts),
magnesium citrate (Citrate of Magnesia),
magnesium hydroxide (Milk of Magnesia),
lactulose (Constilac), polycarbophil
(FiberCon), psyllium (Metamucil),
polyethylene glycol (MiraLax),
polyethylene glycol electrolyte solution
(GoLYTELY), and sodium picosulfate with
magnesium oxide (Prepopix)
Bulk Stimulants
Pharmacokinetics
taken orally
directly effective within the GIT and are not generally
absorbed systemically
rapidly acting, causing effects as they pass through
the GIT

Contraindications and Cautions
allergy to the drug or any of its components
acute abdominal disorders
used with caution in heart block, CAD, debilitation,
pregnancy and lactation
polyethylene and glycol electrolyte solution should
be used with caution in any patient with history of
seizures*
Bulk Stimulants
Pharmacotherapeutics
lactulose, a saltless osmotic laxative that pulls fluid out of the
venous system
and into the lumen of the small intestine
magnesium citrate and hydroxide, milder and slower-acting
laxatives and work by saline pull*
magnesium sulfate, exerts a hypertonic pull against the
mucosal wall**
polycarbophil*, stimulates local activity; milder and less
irritating than many
other bulk stimulants
polyethylene glycol and polyethylene glycol electrolyte solution,
hypertonic fluids containing many electrolytes that pull fluid out
of the intestinal wall to increase the bulk of intestinal contents
psyllium, gelatin-bulk stimulant; similar to polycarbophil in action
Bulk Stimulants
Adverse Effects
GI effects such as diarrhea, abdominal
cramping, and
nausea
CNS effects including dizziness,
headache and weakness*
sweating, palpitations, flushing, and
fainting**

Drug Interactions
the administration of laxatives and other
medications should be separated by at least
30 minutes*
increased risk of neuromuscular blockade
when using nondepolarizing neuromuscular
Lubricants
make defecation easier without
stimulating the movement of the GIT*
include docusate (Colace), glycerin
(Sani-Supp), and
mineral oil

Pharmacotherapeutics
docusate has a detergent action on the
surface of the
intestinal bolus**
glycerin is hyperosmolar laxative that is used in
suppository form to gently evacuate the
rectum without systemic effects higher in the
GIT
mineral oil is the oldest of these laxatives; not
Lubricants
Pharmacokinetics
not absorbed systemically and are excreted in
the
feces
docusate and mineral oil are given orally
glycerin is available as a rectal suppository
or as a liquid for rectal retention

Contraindications and Cautions
allergy to any component of the drug*
acute abdominal disorders**
used with caution in heart block, CAD, and
debilitation*
caution should be used during
pregnancy and lactation**
Lubricants
Adverse Effects
most common are GI effects such as diarrhea,
abdominal cramping, and nausea
leakage and staining may be a problem when
mineral oil is used, and the stool cannot be
retained by external sphincter
CNS effects including dizziness, headache, and
weakness are not uncommon*
sweating, palpitations, flushing, and fainting
have been reported after laxative use**

Drug Interactions
frequent use of mineral oil can interfere
with the absorption of the fat-soluble
vitamins A,D,E and K
Lesson 3
Gastrointestinal
Stimulants

MONECELLE JOY D. PESINABLE, RN
Instructor
Gastrointestinal Stimulants
stimulate parasympathetic activity or
make the GI tissues more sensitive to
parasympathetic activity
include dexpanthenol (Ilopan) and
metoclopramide
(Reglan)

Pharmacotherapeutics
increase GI secretions and motility on a
general level
throughout the tract*
indicated when more rapid movement of GI
contents is desirable
dexpanthenol works by increasing
acetylcholine levels and stimulating the
Gastrointestinal Stimulants
Pharmacokinetics
dexpanthenol is given by IM and reaches peak levels
within 4 hours
metoclopramide is given orally or by IM or IV infusion
and has a peak effect by all routes in 60-90 mins
metabolized in the liver and excreted in the feces and
urine
metoclopramide crosses the placenta and enters breast
milk
dexpanthenol may cross the placenta and enter breast
milk

Contraindications and Cautions
should not be used in patients with a history of allergy
to any of these drugs or with GI obstruction or
Gastrointestinal Stimulants
Adverse Effects
most common effects include nausea, vomiting,
diarrhea,
intestinal spasm, and cramping
others include declining blood pressure and
heart rate, weakness and fatigue*

Drug Interactions
metoclopramide has been associated with
decreased absorption of digoxin from the
GIT**
decreased immunosuppressive effects and increased
toxicity of cyclosporine have occurred when combined
with metoclopramide***
increased sedation can occur if either of these
Lesson 4
Antidiarrheals

MONECELLE JOY D. PESINABLE, RN
Instructor
Antidiarrheals
block stimulation of the GIT for symptomatic
relief from diarrhea
include bismuth subsalicylate, crofelemer,
loperamide,
opium derivatives

Pharmacotherapeutics
slow the motility of the GIT through direct action on
the lining of the GIT to inhibit local reflexes (bismuth
subsalicylate) through direct action on the muscles of
the GIT to slow activity (loperamide), or through
action on CNS centers that cause GI spasm and
slowing (opium derivatives)
indicated for the relief of symptoms of acute and
chronic diarrhea, reduction of volume of discharge
Antidiarrheals
Pharmacokinetics
bismuth subsalicylate is absorbed from the GIT
after oral administration, metabolized in the
liver, and excreted in the urine; it crosses the
placenta*
loperamide is slowly absorbed after oral
administration, metabolized in the liver, and
excreted in the urine and feces; it may cross
the placenta and enter breast milk
opium derivative, a category C-III controlled
substance, is readily absorbed after oral
administration, metabolized in the liver, and
excreted in the urine; crosses the placenta and
enters breastmilk
Crofelemer is minimally absorbed, and its
Antidiarrheals
Contraindications and Cautions
should not be given to anyone with known allergy to
the
drug or any of its components
caution should be used in pregnancy and lactation*
care should be taken in individuals with any history
of GI obstruction and acute abdominal conditions**
or diarrhea due to poisonings*** or with hepatic
impairment*

Adverse Effects
constipation, distention, abdominal discomfort,
nausea, vomiting, dry mouth, and toxic
megacolon**
others include fatigue, weakness, dizziness, and