AMACR Immunostaining is Useful in Detecting Dysplastic Epithelium in Barrett's Esophagus, Ulcerative Colitis, and Crohn's Disease

Dorer, Russell; Odze, Robert D.

doi:10.1097/01.pas.0000213268.30468.b4

Cited by 119 publications

(70 citation statements)

References 41 publications

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“…10 Previous studies demonstrated the expression of AMACR to be a highly specific marker in Barrett's neoplastic lesions. 7,8 Columnar epithelial cell changes indefinite for dysplasia were positive in 3/30 cases in these studies. Follow-up was available for 11 of these patients with columnar epithelial cell changes indefinite for dysplasia.…”

mentioning

confidence: 89%

“…7,8 AMACR is known to be expressed in prostate and colon cancer. Both studies demonstrated the expression of AMACR as a highly specific marker in Barrett's neoplastic lesions.…”

Section: Ink4amentioning

confidence: 99%

“…The slides were stained with the monoclonal anti-AMACR antibody p504S (clone 13H4, 1:500 dilution; Bioprime, Germany; Dako Autostainer; LSAB Detection System, #K5005). Two different pathologists evaluated the immunohistochemical stainings for the presence and the extent of AMACR expression in a blinded fashion, designating samples according to Lisovsky et al, 7 as negative (0 to o5% cells positive), 1 þ (5-14% of cells positive), …”

Section: Immunohistochemistrymentioning

confidence: 99%

“…6 Recently, two studies focused on a-methylacyl coenzyme A racemase (AMACR) in Barrett's neoplastic lesions, an enzyme known to be expressed in prostate and colon cancer. [7][8][9] AMACR catalyzes the racemization of a-methyl-branched carboxylic coenzyme A thioesters. This protein was originally identified in the mitochondria and peroxisomes of rat liver cells.…”

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confidence: 99%

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Expression of α-methylacyl coenzyme A racemase in the dysplasia carcinoma sequence associated with Barrett’s esophagus

Scheil-Bertram¹,

Lorenz²,

Ell³

et al. 2008

Modern Pathology

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Two different studies demonstrated a-methylacyl coenzyme A racemase (AMACR) to be a highly specific marker in Barrett's neoplastic lesions. Reactive atypia was positive in 3/30 cases in these studies. We present a retrospective study of early Barrett's adenocarcinoma treated with surgery (2000-2005, n ¼ 29; M:F ¼ 5:1, median age 67 years). We analyzed the role of AMACR expression in reactive and neoplastic lesions associated with the disease of 77 different specimens (60 biopsy and 17 surgical specimens) of these patients. In our cohort, 70% of cases demonstrated infiltration of the submucosa, 38% were poorly differentiated, and/or 31% demonstrated lymph vessel infiltration. We used a multi-tissue array, with reactive and neoplastic samples for each patient to analyze the immunoreactivity of AMACR. Barrett's epithelium that was negative for dysplasia and columnar epithelial cell changes indefinite for dysplasia (n ¼ 30) did not demonstrate AMACR immunoreactivity. AMACR immunoreactivity was demonstrated in 27% (8/30) of cases of Barrett's epithelium with columnar epithelial cell changes indefinite for dysplasia. Altogether 91% of cases with low-grade dysplasia were AMACR-positive and 96% of cases with high-grade dysplasia and early Barrett's adenocarcinoma were positive for AMACR. In summary, the sensitivity of AMACR expression in low-grade dysplasia and subsequent early Barrett's adenocarcinoma was significantly higher in our study compared with previous data. This might be a new diagnostic marker for dysplasia carcinoma sequence in Barrett's low-grade neoplastic lesions. Further studies are required to investigate this point with well-defined controls having at least 5-years follow-up.

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mentioning

confidence: 89%

“…7,8 AMACR is known to be expressed in prostate and colon cancer. Both studies demonstrated the expression of AMACR as a highly specific marker in Barrett's neoplastic lesions.…”

Section: Ink4amentioning

confidence: 99%

Section: Immunohistochemistrymentioning

confidence: 99%

mentioning

confidence: 99%

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Expression of α-methylacyl coenzyme A racemase in the dysplasia carcinoma sequence associated with Barrett’s esophagus

Scheil-Bertram¹,

Lorenz²,

Ell³

et al. 2008

Modern Pathology

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“…Immunohistochemical markers, such as a-methyl coenzyme A racemase (AMACR), p53, caspase 3, and survivin, are promising as ancillary tests to facilitate the grading of dysplasia and to diagnose early adenocarcinoma in Barrett's esophagus. [8][9][10] Increased cell division with an expanded proliferation zone is consistently observed in gastrointestinal epithelial dysplastic lesions such as inflammatory bowel disease-associated dysplasia 11 and gastric dysplasia. 12 In Barrett's esophagus, dysplastic lesions have elevated proliferation index on Ki67 immunohistochemical staining.…”

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confidence: 99%

Anti-phosphorylated histone H3 expression in Barrett's esophagus, low-grade dysplasia, high-grade dysplasia, and adenocarcinoma

Goodarzi

Correa

Ajani³

et al. 2009

Modern Pathology

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The high interobserver variability in grading dysplasia in Barrett's esophagus demands a biomarker that can be applied in routine surgical pathology practice. Immunohistochemistry for phosphorylated histone H3 is a reliable marker of identifying mitotic figures and has not been evaluated in Barrett's esophagus-associated neoplastic lesions. We retrospectively studied the expression of phosphorylated histone H3 in 88 endoscopic biopsy samples of Barrett's esophagus without dysplasia (n ¼ 19), indefinite for dysplasia (n ¼ 11), low-grade dysplasia (n ¼ 27), high-grade dysplasia (n ¼ 19), or adenocarcinoma (n ¼ 12) from a sample of 54 patients. The samples were included after consensus diagnosis of two gastrointestinal pathologists on the hematoxylineosin (HE)-stained sections. Anti-phosphorylated histone H3-labeled mitotic figures were counted per 10 consecutive high-power fields (HPFs) in three distinct regions: surface epithelium, upper 2/3, and lower 1/3 of the crypts. Anti-phosphorylated histone H3-labeled mitotic counts for the three compartments of the crypts and the total scores for Barrett's esophagus, indefinite for dysplasia, low-grade dysplasia, high-grade dysplasia, and adenocarcinoma were compared using the Mann-Whitney U test. For each compartment, the number of anti-phosphorylated histone H3-positive nuclei was higher in low-grade dysplasia than in Barrett's esophagus without dysplasia or indefinite for dysplasia (Po0.001), but no difference was found between Barrett's esophagus without dysplasia and indefinite for dysplasia. High-grade dysplasia biopsies had significantly more anti-phosphorylated histone H3-labeled mitotic figures in the surface epithelium than the low-grade dysplasia (Po0.001). Adenocarcinoma had higher anti-phosphorylated histone H3-labeled mitotic figures than the highgrade dysplasia (Po0.001). Our data support the previous findings of expansion of the proliferative zone and importance of surface mitotic figure in the progression of Barrett's esophagus-low-grade dysplasia-highgrade dysplasia. In addition, phosphorylated histone H3 is a potential supportive marker to histology in differentiating low-grade dysplasia from indefinite for dysplasia and high-grade dysplasia from adenocarcinoma in the mucosal biopsy samples.

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Inflammatory Disorders of the Large Intestine

Jain

Warren

Riddell

2012

Morson and Dawson's Gastrointestinal Pathology

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AMACR Immunostaining is Useful in Detecting Dysplastic Epithelium in Barrett's Esophagus, Ulcerative Colitis, and Crohn's Disease

Cited by 119 publications

References 41 publications

Expression of α-methylacyl coenzyme A racemase in the dysplasia carcinoma sequence associated with Barrett’s esophagus

Expression of α-methylacyl coenzyme A racemase in the dysplasia carcinoma sequence associated with Barrett’s esophagus

Anti-phosphorylated histone H3 expression in Barrett's esophagus, low-grade dysplasia, high-grade dysplasia, and adenocarcinoma

Inflammatory Disorders of the Large Intestine

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