Gastritis & Gastropathy

The term "gastropathy" should be used to denote conditions in which there is epithelial or endothelial damage without inflammation, and "gastritis" should be used to denote conditions in which there is histologic evidence of inflammation. In clinical practice, the term "gastritis" is commonly applied to three categories: (1) erosive and hemorrhagic "gastritis" (gastropathy); (2) nonerosive, nonspecific (histologic) gastritis; and (3) specific types of gastritis, characterized by distinctive histologic and endoscopic features diagnostic of specific disorders. Erosive & Hemorrhagic "Gastritis" (Gastropathy) Essentials of Diagnosis

Most commonly seen in alcoholic or critically ill patients, or patients taking NSAIDs. Often asymptomatic; may cause epigastric pain, nausea, and vomiting. May cause hematemesis; usually not significant bleeding.

General Considerations The most common causes of erosive gastropathy are drugs (especially NSAIDs), alcohol, stress due to severe medical or surgical illness, and portal hypertension ("portal gastropathy"). Uncommon causes include caustic ingestion and radiation. Erosive and hemorrhagic gastropathy typically are diagnosed at endoscopy, often being performed because of dyspepsia or upper gastrointestinal bleeding. Endoscopic findings include subepithelial hemorrhages, petechiae, and erosions. These lesions are superficial, vary in size and number, and may be focal or diffuse. There usually is no significant inflammation on histologic examination. Major risk factors for stress gastritis include mechanical ventilation, coagulopathy, trauma, burns, shock, sepsis, central nervous system injury, liver failure, kidney disease, and multiorgan failure. The use of enteral nutrition reduces the risk of stress-related bleeding. Clinical Findings Symptoms and Signs Erosive gastropathy is usually asymptomatic. Symptoms, when they occur, include anorexia, epigastric pain, nausea, and vomiting. There is poor correlation between symptoms and the number or severity of endoscopic abnormalities. The most common clinical manifestation of erosive gastritis is upper gastrointestinal bleeding, which presents as hematemesis, "coffee grounds" emesis, or bloody aspirate in a patient receiving nasogastric suction, or as melena. Because erosive gastritis is superficial, hemodynamically significant bleeding is rare. Laboratory Findings The laboratory findings are nonspecific. The hematocrit is low if significant bleeding has occurred; iron deficiency may be found.

Special Examinations Upper endoscopy is the most sensitive method of diagnosis. Although bleeding from gastritis is usually insignificant, it cannot be distinguished on clinical grounds from more serious lesions such as peptic ulcers or esophageal varices. Hence, endoscopy is generally performed within 24 hours in patients with upper gastrointestinal bleeding to identify the source (see endoscopy). An upper gastrointestinal series is sometimes obtained in lieu of endoscopy in patients with hemodynamically insignificant upper gastrointestinal bleeds to exclude serious lesions but is insensitive for the detection of gastritis. Differential Diagnosis Epigastric pain may be due to peptic ulcer, gastroesophageal reflux, gastric cancer, biliary tract disease, food poisoning, viral gastroenteritis, and functional dyspepsia. With severe pain, one should consider a perforated or penetrating ulcer, pancreatic disease, esophageal rupture, ruptured aortic aneurysm, gastric volvulus, and myocardial colic. Causes of upper gastrointestinal bleeding include peptic ulcer disease, esophageal varices, Mallory-Weiss tear, and arteriovenous malformations. Specific Causes & Treatment Stress Gastritis Prophylaxis Stress-related mucosal erosions and subepithelial hemorrhages develop within 72 hours in the majority of critically ill patients (see endoscopy). Clinically overt bleeding occurs in 6%, but clinically important bleeding in < 3%. Bleeding is associated with a higher mortality rate but is seldom the cause of death. In critically ill patients, pharmacologic prophylaxis with intravenous H2-receptor antagonists, oral sucralfate, and an oral, rapid-release suspension of omeprazole plus sodium bicarbonate (Zegerid) has been shown to reduce the incidence of clinically overt and significant bleeding by 50%. At this time, the optimal, cost-effective regimen for the reduction of stress-related mucosal bleeding is uncertain. Prophylaxis should be routinely administered upon admission to critically ill patients with risk factors for significant bleeding. Two of the most important risk factors are coagulopathy (platelets < 50,000/mcL or INR > 1.5) and respiratory failure with the need for mechanical ventilation for over 48 hours. When these two risk factors are absent, the risk of significant bleeding is only 0.1%. Although most critically ill patients have normal or decreased acid secretion, numerous studies have shown that maintaining intragastric pH > 4 reduces the incidence of clinically significant stress-related bleeding. Continuous intravenous infusions of H2-receptor antagonists provide adequate control of intragastric pH in most patients in the following doses over 24 hours: cimetidine (9001200 mg), ranitidine (150 mg), or famotidine (20 mg). After 4 hours of infusion, the pH should be checked by nasogastric aspirate and the dose doubled if the pH is under 4.0. For patients with nasoenteric tubes, immediate-release omeprazole (40 mg at 1 and 6 hours on day 1; then 40 mg once daily beginning on day 2) may be preferred to intravenous H2-receptor antagonists because of lower cost, ease of administration, and comparable efficacy. Although intravenous proton pump inhibitors also

are widely used for this indication, their efficacy and optimal dosing have not been established in controlled trials. Sucralfate suspension (1 g orally every 46 hours) is effective for the prevention of stressrelated bleeding. However, there is a higher incidence of clinically important upper gastrointestinal bleeding with sucralfate (4%) versus H2-receptor antagonists (2%) with no difference in nosocomial pneumonia in more recent studies. In most ICUs, intravenous H2receptor antagonists or proton pump inhibitors are preferred because of their ease of administration. Treatment Once bleeding occurs, patients should receive continuous infusions of a proton pump inhibitor (esomeprazole or pantoprazole, 80 mg intravenous bolus, followed by 8 mg/h continuous infusion) as well as sucralfate suspension, 1 g orally every 4 to 6 hours. Endoscopy should be performed in patients with clinically significant bleeding to look for treatable causes, especially stress-related peptic ulcers with active bleeding or visible vessels. When bleeding arises from diffuse gastritis, endoscopic hemostasis techniques are not helpful. NSAID Gastritis Of patients receiving NSAIDs in clinical trials, 2550% have gastritis and 1020% have ulcers at endoscopy; however, symptoms of significant dyspepsia develop in about 5%. In population surveys, the rate of dyspepsia is increased 1.5- to 2-fold with NSAID use. However, dyspeptic symptoms correlate poorly with significant mucosal abnormalities or the development of adverse clinical events (ulcer bleeding or perforation). Given the frequency of dyspeptic symptoms in patients taking NSAIDs, it is neither feasible nor desirable to investigate all such cases. Patients with alarm symptoms or signs, such as severe pain, weight loss, vomiting, gastrointestinal bleeding, or anemia, should undergo diagnostic upper endoscopy. For other patients, symptoms may improve with discontinuation of the agent, reduction to the lowest effective dose, or administration with meals. Proton pump inhibitors have demonstrated efficacy in controlled trials for the treatment NSAID-related dyspepsia. Although superiority to H2-receptor antagonists for relief of NSAID-related dyspepsia has not been established, proton pump inhibitors have demonstrated superiority for healing of NSAID-related ulcers in the setting of continued NSAID use. Therefore, an empiric 24 week trial of an oral proton pump inhibitor (omeprazole, rabeprazole, or esomeprazole 2040 mg/d; lansoprazole, 30 mg/d; pantoprazole, 40 mg/d) is recommended for patients with NSAID-related dyspepsia, especially those in whom continued NSAID treatment is required. If symptoms do not improve, diagnostic upper endoscopy should be conducted. Alcoholic Gastritis Excessive alcohol consumption may lead to dyspepsia, nausea, emesis, and minor hematemesisa condition sometimes labeled "alcoholic gastritis." However, it is not proven that alcohol alone actually causes significant erosive gastritis. Therapy with H2-receptor antagonists, proton pump inhibitors, or sucralfate for 24 weeks often is empirically prescribed.

Portal Hypertensive Gastropathy Portal hypertension commonly results in gastric mucosal and submucosal congestion of capillaries and venules (see endoscopy); (see endoscopy), which is correlated with the severity of the portal hypertension and underlying liver disease. Usually asymptomatic, it may cause chronic gastrointestinal bleeding in 10% of patients and, less commonly, clinically significant bleeding with hematemesis. Treatment with propranolol or nadolol reduces the incidence of recurrent acute bleeding by lowering portal pressures. Patients who fail propranolol therapy may be successfully treated with portal decompressive procedures (see section on treatment of esophageal varices).

Nonerosive, Nonspecific Gastritis

The diagnosis of nonerosive gastritis is based on histologic assessment of mucosal biopsies. Endoscopic findings are normal in many cases and do not reliably predict the presence of histologic inflammation. The main types of nonerosive gastritis are those due to H pylori infection, those associated with pernicious anemia, and lymphocytic gastritis. (See Specific Types of Gastritis below.) Helicobacter pylori Gastritis H pylori is a spiral gram-negative rod that resides beneath the gastric mucous layer adjacent to gastric epithelial cells. Although not invasive, it causes gastric mucosal inflammation with PMNs and lymphocytes. The mechanisms of injury and inflammation may in part be related to the products of two genes, vacA and cagA. In developed countries the prevalence of H pylori is rapidly declining. In the United States, the prevalence rises from < 10% in non-immigrants under age 30 years to over 50% in those over age 60 years. The prevalence is higher in non-whites and immigrants from developing countries and is correlated inversely with socioeconomic status. Transmission is from person to person, mainly during infancy and childhood; however, the mode of transmission is unknown. Acute infection with H pylori may cause a transient clinical illness characterized by nausea and abdominal pain that may last for several days and is associated with acute histologic gastritis with PMNs. After these symptoms resolve, the majority progress to chronic infection with chronic, diffuse mucosal inflammation (gastritis) characterized by PMNs and lymphocytes. Although chronic H pylori infection with gastritis is present in 3050% of the population, most persons are asymptomatic and suffer no sequelae. Three gastritis phenotypes occur which determine clinical outcomes. Most infected people have a mild, diffuse gastritis that does not disrupt acid secretion and seldom causes clinically important outcomes. About 15% of infected people have inflammation that predominates in the gastric antrum but spares the gastric body (where acid is secreted). People with this phenotype tend to have increased gastrin; increased acid production; and increased risk of developing peptic ulcers, especially duodenal ulcers. About 1% of infected adults have inflammation that predominates in the gastric body. Over time, this may lead to destruction of acid-secreting glands with resultant mucosal atrophy, decreased acid secretion, and intestinal metaplasia. This phenotype is associated with an increased risk of gastric ulcers and gastric cancer. Chronic H pylori gastritis is associated with a 3.5- to 20-fold increased risk of gastric adenocarcinoma and low-grade B cell gastric lymphoma (mucosa-associated lymphoid tissue

lymphoma; MALToma). Eradication of H pylori may be achieved with antibiotics in over 85% of patients and leads to resolution of the chronic gastritis (see section on Peptic Ulcer Disease). Testing for H pylori is indicated for patients with either active or a past history of documented peptic ulcer disease or gastric MALToma and for patients with a family history of gastric carcinoma. Testing and empiric treatment is cost-effective in young patients (< 55 years of age) with uncomplicated dyspepsia prior to further medical evaluation. The role of testing and treating H pylori in patients with functional dyspepsia remains controversial (see Dyspepsia, above). H pylori eradication decreases the risk of gastric cancer in patients with peptic ulcer disease. Some groups recommend population-based screening of all asymptomatic persons in regions in which there is a high prevalence of H pylori and gastric cancer (such as Japan, Korea, and China) to reduce the incidence of gastric cancer. Population-based screening of asymptomatic individuals is not recommended in western countries, in which the incidence of gastric cancer is low, but should be performed in immigrants from high-prevalence regions. Noninvasive Testing for H pylori Although serologic tests are easily obtained and widely available, most clinical guidelines no longer endorse their use for testing for H pylori infection because they are less accurate than other noninvasive tests that measure active infection. Laboratory-based quantitative serologic ELISA tests have an overall accuracy of only 80%. In comparison, the fecal antigen immunoassay and [13C] urea breath test have excellent sensitivity and specificity (> 95%) at a cost of < $60. Although more expensive and cumbersome to perform, these tests of active infection are more cost-effective in most clinical settings because they reduce unnecessary treatment for patients without active infection. Recent proton pump inhibitors or antibiotics significantly reduce the sensitivity of urea breath tests and fecal antigen assays (but not serologic tests). Prior to testing, proton pump inhibitors should be discontinued 714 days and antibiotics for at least 28 days. Endoscopic Testing for H pylori Endoscopy is not indicated to diagnose H pylori infection in most circumstances. However, when it is performed for another reason, gastric biopsy specimens can be obtained for detection of H pylori and tested for active infection by urease production. This simple, inexpensive ($10) test has excellent sensitivity and specificity (90%). In patients with active upper gastrointestinal bleeding or patients recently taking proton pump inhibitors or antibiotics, histologic assessment for H pylori is preferred. Histologic assessment of biopsies from the gastric antrum and body is more definitive but more expensive ($150$250) than a rapid urease test. Histologic assessment is also indicated in patients with suspected MALTomas and, possibly, in patients with suspected infection whose rapid urease test is negative. However, serologic testing is the most cost-effective means of confirming H pylori infection in patients with a negative rapid urease test. Pernicious Anemia Gastritis Pernicious anemia gastritis is an autoimmune disorder involving the fundic glands with resultant achlorhydria and vitamin B12 malabsorption. Of patients with B12 deficiency, less than half have pernicious anemia. Most patients have malabsorption secondary to aging or

chronic H pylori infection that results in atrophic gastritis, hypochlorhydria, and impaired release of B12 from food. Fundic histology in pernicious anemia is characterized by severe gland atrophy and intestinal metaplasia caused by autoimmune destruction of the gastric fundic mucosa. Parietal cell antibodies directed against the H+-K+-ATPase pump are present in 90% of patients. Inflammation and autoimmune destruction of the acid-secreting parietal cells leads to secondary loss of fundic zymogen cells, which secrete intrinsic factor. Achlorhydria leads to pronounced hypergastrinemia (> 1000 pg/mL) due to loss of acid inhibition of gastrin G cells. Hypergastrinemia may induce hyperplasia of gastric enterochromaffin-like cells that may lead to the development of small, multicentric carcinoid tumors in 5% of patients. Metastatic spread is uncommon in lesions smaller than 2 cm. The risk of gastric adenocarcinoma is increased threefold, with a prevalence of 13%. Endoscopy with biopsy is indicated in patients with pernicious anemia at the time of diagnosis. Patients with dysplasia or small carcinoids require periodic endoscopic surveillance. Pernicious anemia is discussed in detail in Chapter 13: Blood Disorders.

Specific Types of Gastritis

A number of disorders are associated with specific mucosal histologic features. Infections Acute bacterial infection of the gastric submucosa and muscularis with a variety of aerobic or anaerobic organisms produces a rare, rapidly progressive, life-threatening condition known as phlegmonous or necrotizing gastritis, which requires broad-spectrum antibiotic therapy and, in many cases, emergency gastric resection. Viral infection with CMV is commonly seen in patients with AIDS and after bone marrow or solid organ transplantation. Endoscopic findings include thickened gastric folds and ulcerations. Fungal infection with mucormycosis and Candida may occur in immunocompromised and diabetic patients. Larvae of Anisakis marina ingested in raw fish or sushi may become embedded in the gastric mucosa, producing severe abdominal pain. Pain persists for several days until the larvae die. Endoscopic removal of the larvae provides rapid symptomatic relief. Eosinophilic Gastritis This is a rare disorder in which eosinophils infiltrate the antrum and sometimes the proximal intestine. Infiltration may involve the mucosa, muscularis, or serosa. Peripheral eosinophilia is prominent. Symptoms include anemia from mucosal blood loss, abdominal pain, early satiety, and postprandial vomiting. Treatment with corticosteroids is beneficial in the majority of patients. Mntrier Disease (Hypertrophic Gastropathy) This is an idiopathic entity characterized by giant thickened gastric folds involving predominantly the body of the stomach. Patients complain of nausea, epigastric pain, weight loss, and diarrhea. Because of chronic protein loss, patients may develop severe hypoproteinemia and anasarca. The cause is unknown. There are case reports of resolution of symptoms and improvement in histologic appearance after H pylori eradication. Dramatic improvement has been reported in a small number of patients with cetuximab, an antibody that binds epidermal growth factor receptor (EGFR). Gastric resection is required in severe

cases.