Development of Type I Gastric Carcinoid in Patients With Chronic Atrophic Gastritis
Development of Type I Gastric Carcinoid in Patients With Chronic Atrophic Gastritis
Development of Type I Gastric Carcinoid in Patients With Chronic Atrophic Gastritis
*Dipartimento Medico-Chirurgico di Scienze Cliniche, Tecnobiomediche e Medicina Traslazionale, SantAndrea Hospital, School of Medicine, University Sapienza, Rome, Italy. Department of Pathology, University of Parma, Parma, Italy. Department of Pathology, SantAndrea Hospital, School of Medicine, University Sapienza, Rome, Italy. Centro Ricerche Fate Bene Fratelli, San Pietro Hospital, Rome, Italy. Department of Public Health Sciences, University Sapienza, Rome, Italy.
SUMMARY Background Long-term observational studies assessing the incidence of type I gastric carcinoid (typeIGC) in patients with chronic atrophic gastritis are few. Aim To evaluate the occurrence of typeIGC at diagnosis and during follow-up and to identify patient features associated with the presence of typeIGC in a cohort of chronic atrophic gastritis patients. Methods Three hundred and sixty-seven chronic atrophic gastritis patients [245 women, age 54 (1879) years] underwent regular follow-up by gastroscopy. The incidence of typeIGC was determined in chronic atrophic gastritis patients with at least 2 years of follow-up (n = 214). Baseline clinical and histological features were analysed as factors associated with the presence of typeIGC by univariate analysis. Results Type I gastric carcinoid was diagnosed in nine (2.4%) patients at the moment when chronic atrophic gastritis was diagnosed. After 1463 personyears, six patients developed typeIGC with an annual incidence rate (person-year) of 0.4%. Patients with typeIGC had signicantly higher levels of gastrin, chromogranin A and more frequently the presence of body polyps and ECL-dysplasia compared with chronic atrophic gastritis patients without typeIGC. Conclusions This cohort study shows that typeIGC is a rare complication in patients with chronic atrophic gastritis, and the presence of body polyps and ECLdysplasia at gastroscopic histologic evaluation is strongly associated with the presence of typeIGC. Aliment Pharmacol Ther 2011; 33: 13611369
Correspondence to: Dr B. Annibale, Dipartimento Medico-Chirurgico di Scienze Cliniche, Tecnobiomediche e Medicina Traslazionale, SantAndrea Hospital, School of Medicine, University Sapienza, Via di Grottarossa 1035, Rome 00189, Italy. E-mail: [email protected]
Publication data Submitted 20 December 2010 First decision 29 December 2010 Resubmitted 11 March 2011 Accepted 26 March 2011 EV Pub Online 15 April 2011
1361
L. Vannella et al. INTRODUCTION Gastric carcinoids (GC) or gastric neuroendocrine tumours are tumours derived from enterochromafn-like (ECL) cells which are localised in the gastric fundus and corpus. The main role of ECL-cells is the secretion of histamine that, in turn, stimulates acid secretion by parietal cells.1 GC are classied into three subgroups, type I to type III, with different pathogenic causes and outcomes.24 Type I lesions are more frequent, up to 80% of the total and are gastrin-dependent tumours which are associated with atrophic gastritis.5Gastrin, released by G-cells in the gastric antrum, is the main factor that regulates the release of histamine and produces trophic effects upon ECL-cells.6 In chronic atrophic gastritis (CAG), the loss of appropriate glands in the body leads to achlorhydria, and consequently, hypergastrinaemia. The chronic elevation of gastrin stimulates ECL-hyperplasia and sometimes the development of type I gastric carcinoid (typeIGC).7, 8 Given that only a small group of CAG patients develop typeIGC, factors other than gastrin are necessary for the progression of ECL-cells to typeIGC. Recently, several large studies in different countries have reported an increasing incidence of all gastric neuroendocrine tumours.9, 10 Although older studies reported a prevalence rate of typeIGC between 1 and 12.5% in patients with CAG,1113 an estimate of typeIGC incidence in patients with this specic condition is unknown. In fact, long-term observational studies assessing the incidence of typeIGC in CAG patients are few.1315 For this reason, the aim of the present study was to evaluate the occurrence of typeIGC at diagnosis and during follow-up and to identify patient features associated with the presence of typeIGC in a cohort of CAG patients. METHODS
Patients and study design Between 1992 and 2008, we diagnosed the presence of CAG in 367 (245 women, median age 54 years, range 1879 years) patients referred to our Unit for unexplained anaemia or long-standing dyspepsia, as described in detail elsewhere.16 Patients underwent gastroscopy with biopsies and those with proven histological diagnosis of CAG were informed about the increased risk of gastric neoplasia associated with CAG and about the need for regular follow-up by gastroscopy. Personal and clinical data, family history for gastric neoplasia and smoking habit were recorded for all patients during a
1362
clinical interview. Of the initial population, 102 patients dropped-out because four patients died from causes notrelated to CAG and 98 patients refused to participate in further follow-up. Thus the study population included 265 patients (177 women, median age 54 years, range 2079 years) (see Figure 1). The incidence of typeIGC was determined in CAG patients with at least 2 years of follow-up [n = 214; median follow-up 6.3 (217) years], after the exclusion of prevalent typeIGC, because this interval of time was considered sufcient for the development of a new lesion of typeIGC. Regarding demographic (gender and age) and clinical features (severity of atrophy), there were no signicant differences between patients of the initial CAG group (n = 367), of the baseline population (n = 265) and of follow-up population. Diagnosis of CAG was based on the presence of fasting gastrin above upper normal values and the histological conrmation of gastric body (corpus and fundus) atrophy based on three biopsies taken from the gastric antrum (within 3 cm of the pyloric ring, lesser and greater curve, anterior or posterior wall) and three biopsies from the body along the greater curve.16, 17 The degree of gastritis was assessed according to the updated Sydney System.18 Atrophy of the gastric body mucosa was dened as focal or complete replacement of oxyntic glands by metaplastic pyloric or intestinal glands. Atrophy of the antral mucosa was dened as focal or complete disappearance of antral glands or their replacement by intestinal metaplastic epithelium.16 The ECL-cell status was assessed according to the Solcia classication.19 Hyperplasia was dened by ECL cells proliferation <150 lm and classied as: normal pattern, simple, linear, micronodular and adenomatoid. The diagnosis of dysplasia was based on ECL proliferation between 150 and 500 lm, while that of carcinoid on ECL proliferation >500 lm. MEN-I diagnosis was excluded.20, 21 In case of a visible lesion, additional biopsies were obtained. All biopsies were examined independently by two experienced pathologists (CB, EP), unaware of the clinical data of the patients. In the event of disagreement, the biopsies were re-examined simultaneously by both pathologists until agreement was reached.16 Pernicious anaemia was dened as low haemoglobin concentration, MCV > 100 together with low B12 vitamin levels, responding to intramuscular B12 vitamin treatment.22 Iron deciency anaemia was dened as low haemoglobin concentration, MCV < 80 and ferritin<30 ng mL.22 The diagnosis of autoimmune thyroid
Aliment Pharmacol Ther 2011; 33: 13611369 2011 Blackwell Publishing Ltd
Excluded patient from the study because: n = 4 died for other causes n = 98 lost at follow-up
Follow-up protocol The rst follow-up gastroscopy was scheduled at intervals between 2 and 4 years after diagnosis of CAG and the same baseline bioptic sampling was repeated.24 If typeIGC was detected, an extensive bioptic sampling of at least ten biopsies (two biopsies in antrum, four in gastric body and four in the fundus) of the gastric mucosa was taken after 6 and 12 months.13 If typeIGC was not conrmed at two following gastroscopies, patients were followed by the general follow-up protocol. Polypoid lesions up to 5 mm was removed by forceps, otherwise an electrocautery snare was used. All patients with a diagnosis of typeIGC underwent at least one imaging procedure for the tumour staging (Octreoscan, CT-scan, Magnetic Resonance Imaging). Data analysis and statistical evaluation Type I gastric carcinoid at diagnosis and during followup in CAG patients was evaluated and prevalence and incidence rates (person-year) were calculated. Quantitative data are presented as medians and ranges or, absolute counts and percentages. MannWhitney and Fisher exact test were used when appropriate. Univariate analysis was performed to identify patient features associated with the presence of typeIGC. The following baseline patient characteristics were analysed: age at CAG diagnosis, gender, presence of atrophic pangastritis dened as the concomitant presence of atrophy in the gastric antrum and body, presence of pernicious anaemia, gastrin, pepsinogen I, CgA, presence of PCA, presence of dyspepsia, presence of gastric polyp, presence of ECL-dysplasia, smoking habits, presence of H. pylori, family history for gastric cancer and presence of AITD. A P value of less than 0.05 was considered statistically signicant.
disease (AITD) was based on the presence of thyroid autoantibodies and thyroiditis signs at ultrasound evaluation irrespective of thyroid function as previously described.23 Plasma gastrin levels were determined by radioimmunoassay using antiserum 4562, kindly supplied by Prof. J.F. Rehfeld, Copenhagen, Denmark, as previously described (gastrin normal values 40 pg mL).13 Chromogranin A (CgA) levels were assessed by ELISA kit (Dako A S, Glostrup, Denmark) (CgA normal values 98 ng mL); Pepsinogen I was measured using a commercial RIA kit (Pepsik; Sorin, Saluggia, Italy; normal values 2080 ng mL); Parietal cell antibodies (PCA) were measured by immunouorescence and Helicobacter pylori IgG antibodies using an ELISA commercial kit (GAP test IgG, Biorad, Milan, Italy).16 Helicobacter pylori infection was considered positive when the bacterium (Giemsa stain) was detected at histology and or on the basis of a positive IgG titre for H. pylori.17 Bismuth-based triple regimen eradication therapy was prescribed in the case of H. pylori positivity and, after 6 months, the absence of H. pylori at histology and a decrease by at least 50% in the initial titre of H. pylori IgG was the criterion for the successful cure of infection.17
Aliment Pharmacol Ther 2011; 33: 13611369 2011 Blackwell Publishing Ltd
RESULTS
Occurrence of typeIGC Type I gastric carcinoid were diagnosed in 9 out of 367 (2.4%) patients at the moment of the initial diagnosis of CAG [six women, median age 59 (range 4072) years]. As shown in Table 1, all typeIGC patients but one presented polyps of the body with a diameter between 0.3 and 3 cm at gastroscopy. In six out of nine (66.7%) patients with typeIGC, the body gastric mucosa presented a severe atrophy, in the remaining cases the atrophy was moderate. The alterations of ECL-pattern associated with typeIGC were micronodular hyperplasia (n = 4; 44.5%) and dysplasia (n = 5; 55.5%). Further details of CAG patients with typeIGC such as the presence of pernicious
1363
1364
L. Vannella et al.
Table 1 | Baseline features of 15 CAG patients with prevalent and incident typeIGCs
Gastrin (pg mL) 305 975 975 570 690 680 2000 1150 1183 1090 500 220 2800 565 1475 240 3 230 3 370 3 120 3 No No Yes Yes 405 2 No 150 3 Yes 547 2 No 150 3 Yes 167 2 Yes 250 3 Yes Body polyp of 0.5 cm Body polyp of 0.3 cm Body polyp of 0.5 cm Body polyp of 3 cm Normal mucosa Body polyp of 0.5 cm Body polyp of 0.5 cm Normal mucosa Body polyp of 1.2 cm Body polyp of 0.4 cm 245 3 No Body polyp of 0.5 cm 140 3 No Normal mucosa 150 3 No Body polyp of 0.6 cm 175 3 Yes Body polyp of 0.5 cm At diagnosis At diagnosis At diagnosis At diagnosis At diagnosis At diagnosis At diagnosis At diagnosis At 31-month follow-up At 31-month follow-up At 41-month follow-up At 7-month follow-up At 59-month follow-up At 18-month follow-up 60 2 No Body polyp of 0.5 cm At diagnosis No At 4-month follow-up No At 6, 15, 32-month follow-up No At 3, 5-month follow-up No No No metastasis after total gastrectomy At 35, 46, 64-month follow-up No No At 13, 18, 50-month follow-up No At 30, 37, 61-month follow-up CgA (ng mL) Body atrophy* Pernicious anaemia Endoscopic ndings Detection of typeIGC Recurrence
Patients
Gender
Age (years)
45
67
40
40
66
72
59
61
55
10
47
11
67
12
69
13
65
14
23
15
49
Table 2 | Baseline clinical, biochemical and histological features of 214 CAG patients with and without typeIGC
TypeIGC n = 15 Age, years (range) Female gender, n (%) Gastrin, pg mL, median (range) Pepsinogen I, ng mL, median (range) Chromogranin A, ng mL, median (range) Pernicious Anaemia, n (%) Family history for gastric cancer, n (%) Smoking habit, n (%) PCA, n (%) Helicobacter pylori positivity, n (%) Dyspepsia, n (%) AITD, n (%) ECL-dysplasia*, n (%) Atrophic pangastritis, n (%) Body atrophy, n (%) Mild Moderate Severe 0 4 (26.6) 11 (73.4) 22 (11.3) 55 (27.4) 122 (61.3) 0.37 1 0.4 59 (2372) 9 (60) 832.5 (2202800) 10 (328) 171 (60405) 7 (46.6) 3 (20) 8 (53.3) 14 (93.3) 7 (46.6) 7 (46.6) 9 (60) 7 (46.6) 2 (13.3) CAG n = 199 54 (2277) 137 (68.8) 500 (502700) 10 (379) 100 (30280) 98 (49.2) 18 (9) 81 (40.7) 158 (79.3) 84 (42.2) 43 (21.6) 91 (46) 0 44 (22.1) P 0.39 0.7 0.01 0.6 0.0001 1 0.13 0.39 0.3 0.79 0.05 0.29 <0.000001 0.5
PCA, parietal cell antibodies; CAG, chronic atrophic gastritis; AITD, autoimmune thyroid disease. Data are expressed as median or proportions (percentage). MannWhitney test or Fisher-test were used for the comparison of baseline features between two groups. Signicant p-values are in bold. * ECL-dysplasia was concurrent at typeIGC in ve prevalent and two incident cases.
Aliment Pharmacol Ther 2011; 33: 13611369 2011 Blackwell Publishing Ltd
1365
L. Vannella et al.
Table 3 | Comparison of gastric polyps in CAG patients with and without typeIGC
Polypoid lesion Gastric location Antrum Body Antrum and body Size <0.5 cm 0.51 cm >1 cm Numbers Single Multiple Sessile Pedunculated 5 12 (41.6) 7 12 (58.3) 12 12 (100) 0 8 15 (53.3) 7 15 (46.7) 12 15 (80) 3 15 (20) ns ns ns ns 9 12 (75) 2 12 (16.7) 1 12 (8.3) 7 15 (46.7) 6 15 (40) 2 15 (13.3) ns ns ns 0 12 (80) 0 6 (3) 7 (3.5) 2 (1) ns 0.000001 ns TypeIGC* n = 15 CAG n = 199 P
Concomitant GI ndings During an overall median follow-up of 6.3 (217) years, three intestinal-type adenocarcinomas were diagnosed [two women; median age 51 (5177) years]. All three were located in the gastric antrum and were diagnosed 8, 5 and 1 years after diagnosis of CAG. The stage of the gastric cancer was T2N1M0 in the male patient and T1N0M0 in the two female patients. After gastrectomy, two patients died, one for neoplastic disease progression and the other for complications after surgery. At the end of the study, one female patient was alive and free of neoplasia.
Endoscopic appearance
Data are expressed as proportions (percentage) and Fishertest was used for the comparison between the two groups. Signicant p-values are in bold. * Reported polypoid lesions refer to gastroscopy performed at the moment of typeIGC diagnosis. Reported polypoid lesions refer to baseline gastroscopy. Three patients had intramucosal carcinoids.
Management and follow-up of typeIGC All patients with polypoid lesions up to 12 mm underwent endoscopic polypectomy. Endoscopic polypectomy failed on the polyp of 3 cm because of its hard consistency. The patient, a man aged 55, underwent total gastrectomy. At histological evaluation, the tumour extended from the mucosa to the submucosa and inltrated the muscularis propria. Immunohistochemistry showed positivity for CgA and VMAT-2 with Ki67 proliferation index lower than 1%. In three out of 19 local lymph nodes removed during the surgery a metastatic endocrine tumour was found. When typeIGC was diagnosed, CT-scan and Octreoscan were performed and resulted negative. In 6 out of 15 (40%) patients with typeIGC, there was a recurrence of the tumour, but all patients with lesions that were small (up to 1 cm) underwent endoscopic polypectomy (see Table 1). At the end of the study, all the patients were alive and in good health.
1366
DISCUSSION In the present work, we followed-up a cohort of CAG patients for 1463 person-years and found an annual incidence rate (person-year) for the typeIGC of 0.4%. Recently, large studies on population-based data in different countries have reported an increasing incidence of GC among all gastric malignancies and an increase of these among all gastrointestinal carcinoid lesions.9, 10 This increase could be partially explained by the increased diffusion of diagnostic gastroscopy25 and correlates temporally with the increasing use of proton pump inhibitors.26 To our knowledge, few studies have evaluated the real incidence of typeIGC in patients with CAG because the surveillance of CAG was not recommended.27 An old study by Kokkola et al. described eight new cases of typeIGC in 416 patient-years which corresponds to an annual incidence of 2%.14 Sjoblom et al. studied 196 patients with pernicious anaemia, but gastroscopy was performed only in 70 of these patients.15 After 1397 patient-years, two new cases of typeIGC were reported on hospital registries among the initial group of 196 patients. This gure should correspond to an annual incidence rate of 0.1%, but in this study not all patients underwent gastroscopy and the incidence rate can only be obtained indirectly. These differences in the typeIGC incidence rates could be explained by the patient selection. CAG can have a wide range of clinical presentations as already reported.28 Patients included in our series had dyspepsia, iron deciency anaemia or pernicious anaemia. In particular, the latter was present in almost 50% of our patients, while previous studies included exclusively patients with pernicious anaemia. In our previous study, we diagnosed one new case of typeIGC in a smaller sample of CAG patients (n = 96) for a shorter period of observation (median time of 2.5 years) which corresponds to an annual incidence of 0.4%.13 Thus, in the present study, increasing both the cohort of
Aliment Pharmacol Ther 2011; 33: 13611369 2011 Blackwell Publishing Ltd
remaining were adenomas. Hyperplastic polyps are very common among all benign epithelial gastric polyps34, 35 and more frequently associated with CAG.36, 37 Importantly, some authors have reported an increased risk of neoplastic progression also for this type of lesions. Moreover, CAG has an increased risk of gastric adenocarcinoma.14, 15 As a consequence, each polyp found at gastroscopy should be removed and histologically examined. Different approaches were proposed for the management of typeIGC such as surgery,38 endoscopic polypectomy,1, 4, 12 somatostatin analogues39, 40 and an endoscopic follow-up without any specic treatment.41, 42 We used a conservative management by endoscopic follow-up and performing polypectomy of all visible polypoid lesions. Only one patient, in whom the endoscopic approach failed, underwent gastrectomy. This patient had a deeper neoplastic lesion in the gastric wall, extended to muscularis propria and metastatic involvement of three lymph nodes. Thus, the surgery in this particular case was appropriate. After surgery, imaging procedures (CT-scan and Octreoscan) for the staging did not reveal metastatic involvement of the other organs. The possibility of more invasive lesions among typeIGC is already described in the literature43, 44 and for patients with larger polyps, local surgical tumour resection is recommended.45 Finally, in our study, the rate of recurrence of the typeIGC during follow-up was almost of 40%. This high recurrence rate could be explained by typeIGC misdiagnosis during the previous gastroscopy, by bioptic sampling errors or the continuous trophic effect of hypergastrinemia on the gastric mucosa. Endoscopic follow-up every 612 months, as suggested also by ENETS guidelines, allowed us to identify recurrent lesions or new lesions (incidence-cases) when they had a small size and were easily removable by polypectomy without complications.46 This approach was safe, and the 100% survival of all typeIGC within the study period is in keeping with previous works.41, 44 Our study has some limitations. The rst is the high number of CAG patients who dropped-out during the follow-up, almost 27%. We do not know the clinical outcomes of these CAG patients and, as a consequence, the incidence rate could be underestimated. However, we know that this group of patients did not present demographic or baseline clinical features different from the CAG patients who remained in the study and we retain that the main ndings of this study remain generally valid.
1367
L. Vannella et al.
Moreover, the power of the statistical analysis was limited by the small number of case-ndings of typeIGC. However, larger number of case-ndings could be obtained only by performing studies with larger cohorts and a longer period of observation. In conclusion, this cohort study implies that typeIGC is a rare complication in patients with CAG and the presence of body polyps at gastroscopy and ECL-dysplasia at histological evaluation are strongly associated with the presence of typeIGC.
ACKNOWLEDGEMENTS Declaration of personal interests: None. Declaration of funding interests: This work was supported by grants from the Italian Ministry for University and Research, PRIN, COFIN 2007 and University Sapienza Roma 20072009, Italy.
REFERENCES
1. Burkitt MD, Pritchard DM. Review article: pathogenesis and management of gastric carcinoid tumours. Aliment Pharmacol Ther 2006; 24: 130520. 2. Rindi G, Bordi C, Rappel S, et al. Gastric carcinoids and neuroendocrine carcinomas: pathogenesis, pathology, and behavior. World J Surg 1996; 20: 16872. 3. Rindi G, Luinetti O, Cornaggia M, et al. Three subtypes of gastric argyrophil carcinoid and the gastric neuroendocrine carcinoma: a clinicopathologic study. Gastroenterology 1993; 104: 9941006. 4. Mulkeen A, Cha C. Gastric carcinoid. Curr Opin Oncol 2005; 17: 16. 5. Bordi C, DAdda T, Azzoni C, et al. Pathogenesis of ECL cell tumors in humans. Yale J Biol Med 1998; 71: 27384. 6. Dockray GJ, Varro A, Dimaline R, et al. The gastrins:their production and biological activities. Annu Rev Physiol 2001; 63: 11939. 7. Creutzfeldt W. The achlorhydria-carcinoid sequence: role of gastrin. Digestion 1988; 39: 6179. 8. Bordi C, DAdda T, Azzoni C, et al. Hypergastrinemia and gastric enterochromafn-like cells. Am J Surg Pathol 1995; 19(Suppl. 1): S819. 9. Modlin IM, Lye KD, Kidd M. A 50-year analysis of 562 gastric carcinoids: small tumor or larger problem? Am J Gastroenterol 2004; 99: 2332. 10. Ellis L, Shale MJ, Coleman MP. Carcinoid tumors of the gastrointestinal tract: trends in Incidence in England Since 1971. Am J Gastroenterol 2010; 105: 25639. 11. Lehtola J, Karttunen T, Krekela I, et al. Gastric carcinoids with minimal or no macroscopic lesion in patients with pernicious anemia. Hepatogastroenterology 1985; 32: 726. 12. Modlin IM, Lye KD, Kidd M. Carcinoid tumors of the stomach. Surg Oncol 2003; 12: 15372. 13. Annibale B, Azzoni C, Corleto VD, et al. Atrophic body gastritis patients with enterochromafn-like cell dysplasia are at increased risk for the development of type I gastric carcinoid. Eur J Gastroenterol Hepatol 2001; 13: 144956. 14. Kokkola A, Sjoblom SM, Haapiainen R, et al. The risk of gastric carcinoma and carcinoid tumours in patients with pernicious anaemia. A prospective followup study. Scand J Gastroenterol 1998; 33: 8892. 15. Sjoblom SM, Sipponen P, Miettinen M, et al. Gastroscopic screening for gastric carcinoids and carcinoma in pernicious anemia. Endoscopy 1988; 20: 526. 16. Annibale B, Marignani M, Azzoni C, et al. Atrophic body gastritis: distinct features associated with H. pylori infection. Helicobacter 1997; 2: 5764. 17. Lahner E, Bordi C, Di Giulio E, et al. Role of H. pylori serology in atrophic body gastritis after eradication treatment. Aliment Pharmacol Ther 2002; 16: 50714. 18. Dixon MF, Genta RM, Yardley JH, et al. Classication and grading of gastritis. The updated Sydney System. International Workshop on the Histopathology of Gastritis, Houston 1994. Am J Surg Pathol 1996; 20: 116181. 19. Solcia E, Bordi C, Creutzfeldt W, et al. Histopathological classication of nonantral gastric endocrine growths in man. Digestion 1988; 41: 185200. 20. Berna MJ, Annibale B, Marignani M, et al. A prospective study of gastric carcinoids and enterochromafn-like cell changes in multiple endocrine neoplasia type 1 and Zollinger-Ellison syndrome: identication of risk factors. J Clin Endocrinol Metab 2008; 93: 158291. 21. Bordi C, Corleto VD, Azzoni C, et al. The antral mucosa as a new site for endocrine tumors in multiple endocrine neoplasia type 1 and Zollinger-Ellison syndromes. J Clin Endocrinol Metab 2001; 86: 223642. 22. Lahner E, Norman GL, Severi C, et al. Reassessment of intrinsic factor and parietal cell autoantibodies in atrophic gastritis with respect to cobalamin deciency. Am J Gastroenterol 2009; 104: 20719. 23. Lahner E, Centanni M, Agnello G, et al. Occurrence and risk factors for autoimmune thyroid disease in patients with atrophic body gastritis. Am J Med 2008; 121: 13641. 24. Lahner E, Caruana P, DAmbra G, et al. First endoscopic-histologic follow-up in patients with body-predominant atrophic gastritis: when should it be done? Gastrointest Endosc 2001; 53: 4438. 25. Modlin IM, Sandor A, Tang LH, et al. A 40-year analysis of 265 gastric carcinoids. Am J Gastroenterol 1997; 92: 6338. 26. Hodgson N, Koniaris LG, Livingstone AS, et al. Gastric carcinoids: a temporal increase with proton pump introduction. Surg Endosc 2005; 19: 16102. 27. Hirota WK, Zuckerman MJ, Adler DG, et al. Standards of Practice Committee, American Society for Gastrointestinal Endoscopy. ASGE guideline: the role of endoscopy in the surveillance of premalignant conditions of the upper GI tract. Gastrointest Endosc 2006; 63: 57080. 28. Marignani M, Delle Fave G, Mecarocci S, et al. High prevalence of atrophic body gastritis in patients with unexplained microcytic and macrocytic anemia: a prospective screening study. Am J Gastroenterol 1999; 94: 76672. 29. Stockbrugger RW, Menon GG, Beilby JO, et al. Gastroscopic screening in 80 patients with pernicious anaemia. Gut 1983; 24: 11417. 30. Borch K, Renvall H, Kullman E, et al. Gastric carcinoid associated with the syndrome of hypergastrinemic atrophic gastritis. A prospective analysis of 11 cases. Am J Surg Pathol 1987; 11: 435 44. 31. Modlin IM, Gustafsson BI, Moss SF, et al. Chromogranin A biological function and clinical utility in neuro endoAliment Pharmacol Ther 2011; 33: 13611369 2011 Blackwell Publishing Ltd
1368
32.
43.
33.
44.
45.
34.
35.
46.
36.
Aliment Pharmacol Ther 2011; 33: 13611369 2011 Blackwell Publishing Ltd
1369