Week 9- Alterations in Gastrointestinal Function-Student PDF

Summary

This document is a lecture about alterations in gastrointestinal function. It covers topics such as gastritis, GERD, PUD and different aspects of the gastrointestinal system, including pathophysiology and clinical presentations. It also includes patient assessment and clinical manifestations.

Full Transcript

Alterations in
Gastrointestinal
Function
KARA SEALOCK EdD MEd BN RN CNCC (C) CCNE
NOVEMBER 1 ST AND 3 RD , 2022
 By the End of this Lecture You Will:
Critically reflect upon the overall anatomy and physiology of the gastrointestinal
system and how dysfunction leads to significant changes systemically
Explain pathophysiology and effects on the body related to:
▪ Gastritis
▪ Gastroesophageal Reflux Disease (GERD) Stomach and
▪ Peptic Ulcer Disease (PUD) Intestinal
▪ Gastrointestinal (Upper and Lower) Bleed Dysfunction
▪ Obstruction/Ileus
▪ Hepatitis
▪ Acute Liver Dysfunction Liver and
▪ Hepatic Encephalopathy
▪ Cholelithiasis and Cholecystitis Gall Bladder
▪ Fulminant Hepatic Failure
Begin to prioritize patient conditions related to nursing assessment and clinical
manifestations
Objectives for this lecture:

By the end students will be able to identify at least 5 common
issues that occur in the gastrointestinal system
Students will be able to explain dysfunction associated with the
stomach, intestine and liver
Students will be able to explain at least 3 differences in
pathophysiology and assessment of the stomach/intestinal
system, and liver
Students will continue to apply previously learned concepts
associated with gastrointestinal/ liver dysfunction through critical
thinking exercises
 Abdominal Assessment

Subjective Data: Objective Data:
▪ Appetite Inspect
▪ Dysphagia (contour, symmetry, umbilicus, skin,
▪ Food intolerance hair, movement and demeanor)
▪ Abdominal pain
Ausculate
▪ Nausea/vomiting
▪ Bowel habits (hyperactive, hypoactive and absent)
▪ Past abdominal history Percuss
▪ Medications Palpate
▪ Nutritional assessment
Objective Data
Figure 35-1, p. 863,
Power-Kean et al.,
(2023)
Stomach and Intestinal
Dysfunction
 Gastritis
▪Inflammation of the stomach
▪May have many causes: acute or chronic
▪ Acute is usually due to local irritants
▪ May or may not be symptomatic
▪ Chronic leads to atrophy of the glandular epithelium of the stomach
▪ H. pylori gastritis is most common
▪ Autoimmune and multifocal least common but increases risk of
carcinoma
▪ Chemical from reflux of duodenal contents, pancreatic secretions, bile
 Gastritis
▪Pathophysiology:
▪ Occurs as a result of the breakdown of the normal gastric mucosal barrier
▪ Hydrochloric acid moves back into the mucosa
▪ Results in tissue edema, disruption of capillary walls with loss of plasma into the gastric lumen and
possible hemorrhage

▪Clinical Manifestations:
▪ Anorexia, nausea and vomiting, epigastric tenderness and a feeling of fullness
▪ Hemorrhage is commonly associated with alcohol abuse
▪ Acute gastritis is self limiting, lasting from a few hours to days with complete healing
▪ Chronic gastritis, patients lose intrinsic factor (a substance secreted by gastric mucosa that is essential
for absorption of cobalamin (vitamin B12) leading to cobalamin deficiency → changes in RBC
production→ anemia and neurological complications

▪Nursing Assessment:
▪ GI: Nausea/vomiting, pain, blood noted in stool or emesis, nutritional intake, ETOH,
Causes of
Gastritis

Table 44-13,
p. 1011,
Tyerman &
Cobbett
(2023)
http://library.med.utah.edu/WebPath/GIHTML/GI016.html
 Gastroesophageal Reflux Disease
▪Acronym GERD
▪Backwards movement of stomach contents into esophagus
▪Pathophysiology:
▪Backflow regulated by a sphincter at stomach entrance; transient
relaxation common after meals, especially fatty foods
▪Clinical Manifestation:
▪Most common symptom epigastric pain or heartburn, sometimes
belching, chest pain
▪Respiratory symptoms include: wheezing, coughing, and dyspnea
▪Otolaryngologic symptoms include: hoarseness, sore throat, lump in
the throat (globus sensation), and choking
 Gastroesophageal Reflux Disease
▪Nursing Assessment:
▪NEURO: dysphagia, pain (PQRST); CV: identify if chest pain is
cardiac in nature or a result of GERD, tachypnea, changes in BP;
RESP: sore throat, lump in throat, hoarseness of cords, wheezing,
coughing, dyspnea, crackles if aspiration pneumonia has occurred;
GI: nutritional status, odynophagia (painful swallowing),
heartburn, nausea/vomiting, weight loss
https://www.choc.org/programs-services/gastroenterology/gerd/
 Gastroesophageal Reflux Disease
Complication: Barrett
esophagus -scarring,
edema, spasm
(strictures)

https://www.mayoclinic.org/diseases-
conditions/barretts-
esophagus/symptoms-causes/syc-
20352841
 Peptic Ulcer Disease
▪ Group of disorders resulting from exposure of upper GI tract to acid-pepsin secretions.
Mostly duodenal and gastric; duodenal much more common. Men 55-70 most
commonly affected
▪ Caused often by H. pylori, Non-Steriodal Anti-Inflammatory Drugs (NSAIDs)
▪ Pathophysiology:
▪ Only develop in the presence of an acid environment
▪ Mucosa barrier becomes impaired, and back-diffusion of acid lead to PUD
▪ Can affect all layers of mucosa and eventually penetrate through
▪ Clinical Manifestations:
▪ Primary symptom is pain usually on empty stomach; relieved by food or antacids*
▪ Exacerbations occur
http://www.medicinenet.com/peptic_ulcer/page2.htm
 Peptic Ulcer Disease

Complications include hemorrhage, gastric outlet
obstruction (from edema, spasm, contraction of scar tissue),
perforation (which can lead to peritonitis)

Fig 36-6, p. 893,
Power-Kean et
al., (2023)
https://www.healthclop.com/differences-of-peptic-gastric-
and-duodenal-ulcer/
 Gastrointestinal Bleed
▪Can happen anywhere in GI tract- (UGIB or LGIB)
▪Site of bleeding indicated by colour and texture: bright red to tarry black
(melena)
▪ Upper GI often coffee-ground material (partially digested) or bright red
▪ Brighter red means bleeding closer to the source; darker means further from source
(e.g. source is duodenum, which is high up, blood in stools will be dark; hemorrhoids
often produce bright red blood)
▪ May be hard to pinpoint source; e.g. with hypermotility blood may be bright red even
if source is high in GI tract

▪Think EMERGENCY Situation!!!
▪Patients may also develop lower GI bleeding where primary symptom is
frank red blood
Fig 36-1, pg. 887, Power-
Kean et al., (2023)
 Gastrointestinal Bleed
▪Nursing Assessment (IPAP’s):
▪NEURO: LOC, alert, orientated, lethargic, dizziness, light headedness, anxiety,
confusion, stupor, coma (due to low cerebral blood flow); CV: color, hemodynamic
status- is the patient pale, pink, grey, cyanotic, low CO, low BP, tachycardia, changes in
perfusion, capillary refill, cool to touch, changes in pulses especially in lower
extremities, chest pain or angina present, dysrhythmias (AF); RESP: tachypnea, dyspnea,
cyanosis, crackles due to pulmonary edema or heart failure; GI: absent of hypoactive
bowel sounds, epigastric tenderness, anorexia; RENAL: urine output, < or > 30 cc/hr
(due to decreased blood flow to kidneys), monitoring for tubular necrosis, colour,
consistency, frequency, 24 hour fluid balance

▪LAB Values: CBC (Hgb, platelets, hematocrit), All electrolytes with careful attention to
potassium, creatinine, BUN, GFR
 Obstruction/Ileus

What is an obstruction?
▪ Any condition that prevents normal flow of chime through intestine
▪ Loss of intestinal motility in the absence of an ileus
▪ Classified as simple or functional

Primary Cause of Small Primary Cause of Large Bowel
Bowel Obstruction: Obstruction:
Adhesions * Malignancy
Hernia Volvulus
Tumors Strictures related to
diverticulitis
Pathophysiology of Intestinal Obstruction
Figure 36-5, p. 892, Power-
Kean et al., (2023)
 Intestinal Obstruction

▪Clinical Manifestations:
▪Symptoms based on degree and duration of obstruction
▪May be sudden and dramatic symptoms of pain (intermittent),
vomiting, distention, borborygmus**, peristaltic rushes,
restlessness and awareness of peristaltic movements
▪Treatment based on cause. May respond to
decompression, but may require surgery
 Stomach and Intestinal Dysfunction
Key Assessment Points
Changes or Absent Bowel Sounds
Complaints of Nausea, Vomiting, Anorexia and Distention
Abnormalities noted in Lab Values
GI Pain
▪Usually sharp or burning
▪May be steady or intermittent
▪May be referred
▪As with all pain, assessment of timing, quality, and intensity of pain
is key
Liver and Gallbladder
Dysfunction
 Liver and Gall Bladder
Liver Structure and Function

Fig 35-15, p. 874,
Power-Kean et al.,
(2023)
 Liver Structure and Function

STRUCTURE FUNCTION
Largest; divided into R & L lobes Multi-skilled organ
Located RUQ Secretes bile
Main blood supply from hepatic Metabolism of Bilirubin
artery and portal vein. Portal vein Hematologic(hematopoiesis,
drains from alimentary canal, clotting, storage)
spleen and pancreas.
Blood drains into sinusoids, and Metabolism of Nutrients (CHO,
from there into central veins and CHON, Fat)
then to Inferior Vena Cava Detoxifies (at risk for further
Hepatic circulation important b/c injury)
obstruction leads to portal Stores Minerals (Vitamins B12, D,
hypertension A, E, and K)
 Hepatitis A
▪Pathophysiology:
▪ Widespread inflammation of the liver tissue
▪ Liver damage is mediated by cytotoxic cytokines and natural killer cells that
cause lysis of infected hepatocytes
▪ Damage results from liver necrosis
▪ Inflammation of periportal areas may interrupt flow of bile
▪ Hepatitis A is transmitted through feces (fecal-oral route; contaminated water
and food; blood)
▪ Hepatitis A has an incubation period of 2-7 weeks.
▪Clinical Manifestations: Fatigue, nausea vomiting, fever, hepatomegaly,
jaundice, dark urine, anorexia, rash, but is usually a mild disease
 Fulminant Viral Hepatitis
▪ Clinical syndrome that results in severe impairment or necrosis of the liver cells
▪May occur with Hepatitis B or C virus
▪Tylenol overdoses are common to cause this severe syndrome
▪ Edematous hepatocytes and patchy areas of necrosis and inflammatory cell
infiltrates disrupt the parenchyma
▪Acute liver failure develops within 6-8 weeks after initial symptoms of hepatitis
▪Clinical Manifestations:
▪ Anorexia, vomiting, abdominal pain, progressive jaundice, followed by ascites
and gastrointestinal bleed
 Jaundice
▪ May occur as a result of liver dysfunction
▪Results from 1. extrahepatic (post-hepatic) obstruction to bile flow,
2. intrahepatic obstruction, 3. prehepatic excessive production of
unconjugated bilirubin
▪Conjugated bilirubin cannot flow out of the liver because of
obstruction or inflammation of the bile ducts→ stools become light
or clay coloured
▪Pruritis can occur due to bile salts accumulating under the skin
▪Urine may become dark brown or brownish red
Mechanisms
of Jaundice

Fig 36-14, pg. 909,
Power-Kean et al.,
(2023)
 Portal Hypertension
▪Abnormally high blood pressure in the portal venous system caused by resistance to portal
blood flow
▪Pathophysiology:
▪ Intrahepatic result from vascular remodelling with intrahepatic shunts, thrombosis, inflammation or
fibrosis such as in cirrhosis of the liver, viral hepatitis, or schistosomiasis (parasitic infection)
▪ Posthepatic causes occur from hepatic vein thrombosis or cardiac disorders that impair the pumping
ability of the right side of the heart (RV HF); blood backs up and there is increased pressure in the portal
system
▪ Prehepatic causes occur with narrowing of the hepatic portal vein
▪ Long term complications include: varices, splenomegaly, hepatopulmonary syndrome and
portopulmonary hypertension

▪Clinical Manifestations:
▪ Most common clinical manifestation is vomiting of blood from bleeding esophageal varices, then slow,
chronic bleeding from varices causes anemia or melena
 Portal Hypertension

▪ Backup leads to varices, ascites and right
sided heart failure

▪ Varices can result in profound bleed: melena,
frank red blood, vomiting

▪ Rapid treatment needed - volume
replacement, drugs, endoscopy, balloon
tamponade, surgery
▪ (portacaval shunt)
Fig 35-6, pg. 865, Power-Kean
et al., (2023)
 Non-Alcoholic Fatty Liver Disease (NAFLD) and
Non-Alcoholic Steatohepatitis (NASH)

Nonalcoholic Fatty Liver Disease(NAFLD)
▪Hepatocytes are infiltrated with fat (triglycerides)
▪Occurs in absence of alcohol
▪Associated with obesity, high levels of cholesterol and triglycerides,
metabolic syndrome and type 2 diabetes
▪May develop NASH
Nonalcoholic Steatohepatitis (NASH)
▪Hepatocellular injury, inflammation and fibrosis
▪May progress to cirrhosis and end-stage liver disease
https://www.stockwinners.com/blog/tag/
nonalcoholic-fatty-liver-disease-nafld/
 Cirrhosis of the Liver
▪Pathophysiology:
▪Irreversible inflammatory, fibrotic liver disease
▪Fibrosis occurs when the liver tries to regenerate after an injury but the
regenerative process is disorganized
▪Overgrowth of new and fibrous tissue distorts the structure, resulting in
lobules of irregular size and shape impeding blood flow
▪Leads to poor cellular nutrition, and hypoxia causing inadequate flow
and scar tissue decreasing the function of the liver
 Cirrhosis of the Liver
▪ Clinical Manifestations:
▪Abnormal liver function tests; AST, ALT, GGT, Alk Phos,
▪Normal blood values; Albumin, Bilirubin (initially but then increases as
the disease progresses), PTT
▪Initially, patient’s complain of abdominal pain, fatigue, slight weight
loss, and enlargement of the liver and the spleen
▪As the illness progresses, patients develop: jaundice, skin lesions,
peripheral neuropathy, portal hypertension, esophageal and gastric
varices, peripheral edema and ascites, hepatic encephalopathy,
hepatorenal syndrome
 Ascites

Sodium, water and protein accumulate
in peritoneal cavity due to pressure changes in
lymph system, capillaries. Oncotic and osmotic
pressures rise
May require paracentesis as pressures in
abdomen increase
Sodium restriction, diuretics
Colloids to increase oncotic pressure
Fig 36-12, p. 907,
Power-Kean et al.,
(2023)
 Ascites
▪Accumulation of fluid in the peritoneal cavity reducing amount of fluid available for normal
physiological functions
▪Most common complication of cirrhosis but can also occur with right sided heart failure,
abdominal malignancies, nephrotic syndrome, and malnutrition
▪Pathophysiology:
▪ Contributing factors include: portal hypertension, decreased synthesis of albumin by the liver,
splanchnic arterial vasodilation, and renal sodium and water retention

▪Clinical Manifestations:
▪ Increased abdominal distention, increased abdominal girth, and weight gain
▪ Dyspnea caused by decreased lung capacity leading to increase in respiratory rate
▪ Peripheral edema
▪ May develop bacterial peritonitis (fever, chills, abdominal pain, decreased bowel sounds, and cloudy
ascitic fluid)
Fig 36-15, p. 911,
Power-Kean et al.,
(2023)
 Fig 36-13, p. 907,
Fig 34-14, p. 917
Power-Kean et al., (2023)
 Hepatic Encephalopathy
▪AKA portosystemic encephalopathy
▪Pathophysiology:
▪Complex neurologic syndrome characterized by impaired cognitive
function, asterixis, and EEG changes
▪May develop rapidly and become an EMERGENCY situation quickly
▪Increased amounts of Ammonia and GABA (inhibitory transmitter) may
contribute to reduced LOC
▪Clinical Manifestations:
▪subtle changes in personality, memory loss, irritability, lethargy and sleep
disturbances are common. Symptoms can progress to confusion, flapping
tremor of the hands, stupor, convulsions and coma
▪Treatment: lactulose, lactulose, lactulose
http://www.youtube.com/watch?v=atvlbGXlUU4
 Anatomy of the Gallbladder

http://www.cancer.gov/cancertopics/pdq/treatment/gallbladder/Patient/page1
 Gallbladder: Structure and Function
▪Saclike organ
▪Primary function is to store and concentrate bile between meals
▪Bile is an alkaline, bitter tasting, yellowish green fluid that contains
bile salts, cholesterol, bilirubin, electrolytes, and water
▪Aids in digestion of fats
▪Bile is released in response to food
▪Conditions slowing or obstructing flow of bile out of the gallbladder
lead to gallbladder disease
 Disorders of the Gallbladder
Cholelithiasis (Gallstones)
▪Pathophysiology
▪ Gallstones are formed from impaired metabolism of cholesterol, bilirubin, and bile salts
▪ 3 types of gallstones: cholesterol (most common), pigmented (black-hard, brown-soft), and
mixed
▪ Form when there is decreased motility and biliary stasis
▪ Stones may lay dormant and silent until they become lodged in the cystic or common duct,
causing pain when the gallbladder contracts
▪Clinical Manifestations:
▪ Often asymptomatic
▪ Epigastric and RUQ pain and intolerance to fatty foods are cardinal manifestations
▪ Vague symptoms include heartburn, flatulence, epigastric discomfort, pruritus, jaundice,
and foot intolerances particularly to fats and cabbage
▪ Biliary colic (pain) occurs 30 to several hours after eating a fatty meal
 Disorders of the Gallbladder
Cholecystitis
▪Pathophysiology:
▪ Can be acute or chronic
▪ Caused by the lodging of a gallstone in the cystic duct
▪ Gallbladder becomes distended and inflamed
▪ Colic pain but decreased blood flow can result in ischemia, necrosis, and
perforation of the gallbladder
▪Clinical Manifestations:
▪ Fever, leukocytosis, rebound tenderness, and abdominal muscle guarding
▪ Serum bilirubin and alkaline phosphatase (ALP) may be elevated
Fig 36-16, p. 915,
Power-Kean et al., (2023)
 Gallbladder Disorder
▪Nursing Assessment:
▪ RUQ or epigastric pain may be referred
▪ May be severe- peak in 30 minutes and can last for several hours
▪ Pain may be dull, constant and radiate to back, waist, shoulder, and scapula
▪ Lab tests with cholelithiasis and biliary colic often normal
▪ Monitor for high WBC in cholecystitis
▪ AST, ALT may be elevated with CBD stone
▪ Serum amylase may be elevated
▪ Increased bilirubin
▪ Urine culture and sensitivity to rule out pyelonephritis or renal stones
 Diagnostic Tests Associated with
Gallbladder Disorder
▪ERCP (Endoscopic Retrograde ▪Plain x-rays (show calcium ring
Cholangiopancreatography) on some stones, air in biliary
tree, other sources of
▪Radiographic and endoscopic; obstruction)
diagnosis & treatment
▪Ultrasound most common and
▪Computed Tomography Scan (CT probably most reliable with least
misses 20%) risk (90-95% sensitive for
cholecystitis)
▪Scintigraphy (HIDA) (nuclear
scanning)
Endoscopic Retrograde Cholangiopancreatography
 Key Points to Remember
▪Can you perform a full abdominal assessment with knowledge of physiological
landmarks and anatomy and physiology related to GI assessment?
▪Explain the “why” associated with GI assessment and connections to other systems
▪Identify and apply concepts of V/Q mismatching related to multiple respiratory
conditions
▪ Do you understand the pathophysiology, clinical manifestations and nursing
assessment related to :
▪ Dysfunction of the Stomach and Intestines
▪ Gastritis, GERD, PUD, UGIB, LGIB, Obstruction/Ileus
▪ Dysfunction of the Liver and Gall Bladder
▪ Hepatitis, Acute Liver Dysfunction, Hepatic Encephalopathy, Cholelithiasis and
Cholecystitis, Fulminant Hepatic Failure