1. �DIAGNOSIS AND THERAPY OF PEPTIC ULCER�Dijagnostika i terapija peptickog ulkusa� Milorad Opacic
Center of Interventional Gastroenterology, University Hospital Rebro
Clinical Hospital Center, Zagreb, Croatia
2. Radiography in ulcer disease Sensitivity:
Single contrast < 50% of DUs
double contrast, compression, or hypotonic duodenography:
80 %of DUs
GUs also varies as a function of technique
Levine, MS. Role of the double-contrast upper gastrointestinal series in the 1990s. Gastroenterol Clin North Am 1995; 24:289.
3. Endoscopy in ulcer disease (UD) Sensitivity:
location of the ulcer
experience of the endoscopist
Experienced endoscopists detect about 90 % GD lesions
found by a second endoscopist, by radiography, or at surgery*
*Cotton, PB, Shorvon, PJ. Analysis of endoscopy and radiography in the diagnosis, follow-up and treatment of peptic ulcer disease. Clin
Gastroenterol 1984; 13:383.
Dooley, CP, Larson, AW, Stace, NH, et al. Double-contrast barium meal and upper gastrointestinal endoscopy. Ann Intern Med 1984
4. Differentiation: benign gastric ulcer / cancer Benign gastric ulcer (GU)
smooth, regular, rounded edges,
flat, smooth ulcer base
Cancer
ulcerated mass
nodular, clubbed,
fused surrounding folds
irregular or thickened margins
5. Differentiation: benign gastric ulcer / cancer Multiple biopsies
The chance of malignancy > large GUs
optimal number of biopsies
4 jumbo = 6 - 7 regular sized
first biopsy- correct diagnosis in 70%
four biopsy > 95%
Seven biopsy > 98%
Seven biopsy and cytology: 100%
Graham, DY, Schwartz, JT, Cain, GD, et al. Prospective evaluation of biopsy number in the diagnosis
of esophageal and gastric carcinoma. Gastroenterology 1982; 82:228.
6. Follow-up endoscopy to exclude malignant GU > 98% malignancies detected at initial evaluation
risk of finding gastric cancer on follow-up:
0.8% - 4.3%
If endoscopist confident that lesion was benign
NPV for cancer 0.95 - 0.99
Kochman, ML, Elta, GH. Gastric ulcers — when is enough, enough? Gastroenterology 1993; 105:1583.
Bustamante, M, Devesa, F, Borghol, A, et al. Accuracy of the initial endoscopic diagnosis in the discrimination of gastric ulcers: is endoscopic follow-up
study always needed?. J Clin Gastroenterol 2002; 35:25.
Hopper, AN, Stephens, MR, Lewis, WG, et al. Relative value of repeat gastric ulcer surveillance gastroscopy in diagnosing gastric cancer. Gastric
Cancer 2006; 9:217.
7. Histology in ulcer disease first set of biopsies: dysplasia (?)
Repeat biopsy !
missed sample
carcinoma masquerading as benign ulcer
8. �Ulcer disease; H. pylori testing �
At endoscopy: biopsy (urease testing or histology)
Negative ? second test
(Breath or stool antigen testing)
SS and SP of urease biopsy / breath testing: 90 and 95%
NPV 99% PPV 67%
9. �Natural history of UD �
widely variable
spontaneous healing
recurrence within a year or two ( 50 - 80% )
10. �Therapy of UD � General points:
eradication of H. pylori in infected individuals
antisecretory therapy
withdraw of NSAIDs, cigarettes, and
alcohol excess
no firm dietary recommendations
11. ���Antisecretory therapy after HP eradication ���
Small or moderate size DU’s or GU’s:
no additional therapy
Complicated & increased risk DU’s or GU’s :
maintenance of acid suppression
follow-up endoscopy 4 to 12 wks after HP therapy
stepping down to H2 receptor antagonist (?)
12. �Therapy of HP negative UD � false-negative testing for HP consumption of NSAIDs
DU COMPLICATED DU & GU
another HP test endoscopy & biopsy
urease test & histology
THERAPY
13. �Healing rates�
H2 ANTAGONISTS PPI
cimetidine, ranitidine, omeprazole, esomeprazole
famotidine, nizatidine lansoprazole, pantoprazole,
rabeprazole
DU DU
4 wks 70 - 80% 2 wks 63 - 93 %
8 wks 87 - 94% 4 wks 80 - 100 %
.
14. ��Antacids and sucralfate � �
15. �Endoscopic follow up after initial therapy �
Uncomplicated DU
no need for further endoscopy
GU
no clear consensus to guide management
repeat endoscopy with biopsy
16. �Prepyloric and giant ulcers � Prepyloric ulcers
different levels of acid secretion and the distribution of gastritis
slower healing
Giant ulcers
H2 receptor antagonists - slow healing and recurrences
PPI’s: 12 wks – therapy of choice
17. �Reccurent ulcer � Predisposing factors:
HP infection
regional inflammatory response
poor healing
bulb deformity
gastric metaplasia in the duodenum
NSAID use
smoking
18. �Maintenance therapy � Prevention of recurrence
High-risk subgroups:
history of complications
frequent recurrences
refractory, giant, or severely fibrosed ulcers
Long-term maintenance therapy
high-risk patients who fail H. pylori
eradication
19. �Maintenance therapy � Doses of H2 antagonists (ad bedtime)
Ranitidine 150 mg
Cimetidine 400 mg
Famotidine 20 mg
Nizatidine 150 mg
PPI
appropriate dose ?
to be used if H2 failed ?
20. �Maintenance therapy in high risk subgroups* �
DU recurrence rate (12 mo) :
H2 antagonists: 20 - 25%
Placebo: 60 - 90%
*data from largely HP-positive population
21. �Maintenance therapy in high risk subgroups* �
Highest risk of recurrence in first 3 - 6 mo of th.
Recurrence similar as in pts on placebo if MT is stopped after 1 yr
Uncomplicated recurrent disease: MT 2 yrs
Complicated disease: MT 5 yrs
*data from largely HP-positive population
22. �Reccurent ulcer treatment �
Maintenance therapy
until cure of HPin high risk group
in pts who fail HP eradication
in pts with HP negative reccurent ulcers
23. �Refractory ulcer � Etiology
Persistent H. pylori infection
NSAID use
Smoking
Impaired healing (inflammation, circulatory problems.........
Acid hypersecretory states
Impaired response to antisecretory agents
Comorbidity (uremia, cirrhosis....)
24. �Refractory ulcer � Treatment
HP eradication followed by standard PPI therapy
Endoscopy after 8 wks, repeat biopsy in GU
6 - 24 mo of sustained full dose antisecretory therapy
maximal medical therapy before recommending elective surgery
