Sporadic Fundic Gland Polyps With Low-Grade Dysplasia: A Large Case Series Evaluating Pathologic and Immunohistochemical Findings and Clinical Behavior

Abstract: Objectives: Fundic gland polyps (FGPs) occur in two clinicalFundic gland polyps (FGPs) are the most common type of gastric polyp. 1,2 They typically occur in the body and fundus of the stomach and are composed of cystically dilated oxyntic glands lined by attenuated chief, parietal, and mucous neck cells. The polyp surface is lined by gastric foveolar epithelium. FGPs occur in two different clinical settings, sporadic and syndromic (familial adenomatous polyposis, or FAP).Sporadic FGPs have been reported in 0.… Show more

“…Dysplasia in d‐FGPs is generally described as occurring with surface foveolar and glandular mucous neck cells, with parietal and chief cells being uninvolved . In rare instances, dysplasia of parietal cells was hinted at but not definitely observed in our study, given the focal dysplasia within non‐foveolar, non‐mucous neck cells (Figure F) and possible nuclear β‐catenin staining within parietal cells (Figure C), although this was difficult to evaluate on IHC sections.…”

“…The development of malignancy in FGPs is extremely rare, with very few cases having been reported in the literature; it has been reported that FAP patients do not have an increased risk of gastric carcinoma . The adenomatous polyposis coli (APC)–β‐catenin pathway has been implicated in the development of dysplastic (and non‐dysplastic) FGPs in FAP patients, and immunohistochemistry (IHC) for β‐catenin can accordingly be positive in dysplastic nuclei …”

“…Although dysplasia appears to be more likely to occur in syndromic FGPs, multiple authors have reported d‐FGPs in non‐syndromic patients as well . This subset of d‐FGPs, which also show APC–β‐catenin abnormalities, has undergone scrutiny in recent years, but is less well studied overall.…”

“…9 The adenomatous polyposis coli (APC)b-catenin pathway has been implicated in the development of dysplastic (and non-dysplastic) FGPs in FAP patients, 6 and immunohistochemistry (IHC) for b-catenin can accordingly be positive in dysplastic nuclei. [10][11][12] Although dysplasia appears to be more likely to occur in syndromic FGPs, multiple authors have reported d-FGPs in non-syndromic patients as well. 6,8,[12][13][14] This subset of d-FGPs, which also show APC-b-catenin abnormalities, [13][14][15] has undergone scrutiny in recent years, but is less well studied overall.…”

“…[10][11][12] Although dysplasia appears to be more likely to occur in syndromic FGPs, multiple authors have reported d-FGPs in non-syndromic patients as well. 6,8,[12][13][14] This subset of d-FGPs, which also show APC-b-catenin abnormalities, [13][14][15] has undergone scrutiny in recent years, but is less well studied overall. Having noticed that our patient population appears to be enriched for non-syndromic d-FGPs, we undertook this study to compare clinical and pathological characteristics across syndromic and non-syndromic cases.…”

Comparison of dysplastic fundic gland polyps in patients with and without familial adenomatous polyposis

“…Dysplasia in d‐FGPs is generally described as occurring with surface foveolar and glandular mucous neck cells, with parietal and chief cells being uninvolved . In rare instances, dysplasia of parietal cells was hinted at but not definitely observed in our study, given the focal dysplasia within non‐foveolar, non‐mucous neck cells (Figure F) and possible nuclear β‐catenin staining within parietal cells (Figure C), although this was difficult to evaluate on IHC sections.…”

“…The development of malignancy in FGPs is extremely rare, with very few cases having been reported in the literature; it has been reported that FAP patients do not have an increased risk of gastric carcinoma . The adenomatous polyposis coli (APC)–β‐catenin pathway has been implicated in the development of dysplastic (and non‐dysplastic) FGPs in FAP patients, and immunohistochemistry (IHC) for β‐catenin can accordingly be positive in dysplastic nuclei …”

“…Although dysplasia appears to be more likely to occur in syndromic FGPs, multiple authors have reported d‐FGPs in non‐syndromic patients as well . This subset of d‐FGPs, which also show APC–β‐catenin abnormalities, has undergone scrutiny in recent years, but is less well studied overall.…”

“…9 The adenomatous polyposis coli (APC)b-catenin pathway has been implicated in the development of dysplastic (and non-dysplastic) FGPs in FAP patients, 6 and immunohistochemistry (IHC) for b-catenin can accordingly be positive in dysplastic nuclei. [10][11][12] Although dysplasia appears to be more likely to occur in syndromic FGPs, multiple authors have reported d-FGPs in non-syndromic patients as well. 6,8,[12][13][14] This subset of d-FGPs, which also show APC-b-catenin abnormalities, [13][14][15] has undergone scrutiny in recent years, but is less well studied overall.…”

“…[10][11][12] Although dysplasia appears to be more likely to occur in syndromic FGPs, multiple authors have reported d-FGPs in non-syndromic patients as well. 6,8,[12][13][14] This subset of d-FGPs, which also show APC-b-catenin abnormalities, [13][14][15] has undergone scrutiny in recent years, but is less well studied overall. Having noticed that our patient population appears to be enriched for non-syndromic d-FGPs, we undertook this study to compare clinical and pathological characteristics across syndromic and non-syndromic cases.…”

Comparison of dysplastic fundic gland polyps in patients with and without familial adenomatous polyposis

Polyps and tumour‐like lesions of the stomach

Prevalence and risk factors for fundic gland polyps