Cases of adenocarcinoma in Barrett’s esophagus (BE) are on the increase in Western countries. Clinical and histological studies suggest a successive progression from gastroesophageal reflux disease (GERD) to columnar-lined esophagus, also known as BE, to dysplasia with a high risk of malignancy. The pathogenesis of this sequence has yet to be completely elucidated, since more cases of BE, dysplasia and adenocarcinoma were recently found among patients without GERD symptoms than those that underwent endoscopy because of GERD (1). This result depends on the identifying criteria indicative for BE used by the endoscopist who obtains the biopsy. The management of BE remains controversial. Various guidelines exist and the international consensus over issues, such as recognition of short-segment disease and surveillance policies for uncomplicated and dysplastic disease, is lacking (2).

The histological diagnosis of BE involves the presence of columnar epithelium with goblet cells in the esophageal mucosa. Dysplasia-intraepithelial neoplasia (IEN) serves as a morphological marker for increased cancer risk. The most important diagnostic markers of IEN are poor maturation, excessive crowding of glands and cytonuclear features. It is believed that the development of BE with intestinal goblet-type cells is related to the process of proliferation and differentiation of pluripotential epithelial stem cells in response to local injury, chronic inflammation as well as the repair process being altered (3–5). The practical utility of mucin stainings, endocrine cell count, assessment of cell proliferation (Ki-67 and PCNA), expression of EGF, TGFα and p53 is limited regarding the diagnosis and differentiation of dysplastic and non-dysplastic BE (6,7).

One of the factors related to esophageal adenocarcinoma pathogenesis is an aberrant arachidonic acid (AA) metabolism through cyclooxygenase (COX) and 5- and 12-lipooxygenase (5- and 12-LOX). Numerous published studies are related to the expression of stem cell markers and pro-tumorigenic enzymes 5- and 12-LOX in BE. Findings of these studies showed a positive expression in esophageal adenocarcinoma, with inconsistent results in other lesions of esophago-gastric junction mucosa (4,8,9). This study aimed to assess platelet 12-lipoxygenase (p12LOX) and stem cell markers in BE mucosa and other gastro-intestinal mucosal lesions.

The immunoreactivity of the tested antibodies varied. Stem cell marker CD117 was completely negative. The positive immunoreactivity of the remaining antibodies is collated in Table I. The majority of the cases of Barrett’s mucosa showed moderate to high immunoreactivity with p12LOX antibodies (Fig. 1a) and more than half of the cases were immunopositive for stem-cell antibodies CD44 (Fig. 1b) and nestin. The highest immunoreactivity was observed in dysplastic BE mucosa. The 5 cases of Barrett’s with IEN showed high positive immunoreactivity with p12LOX, CD44 and nestin antibodies.

In the comparative group, few clinically suspicious cases not morphologically confirmed for BE showed mild focal immunopositive reactions. A total of 3 of 17 cases in the gastric mucosal intestinal metaplasia cases showed focal immunopositivity for the tested markers restricted to the foci of low-grade mucosal dysplasia. The majority of the colorectal adenomas with low-grade dysplasia showed mild positive immunostaining for p12LOX ab7212 (rabbit, polyclonal), whereas p12LOX ab7225 (murine, monoclonal) was positive in only 1 case with negative stem cell markers.

The diagnostic incidence of BE in the endoscopical biopsy material obtained from the OG junction mucosa of patients with GERD, endoscopically suspected for BE, (13%) is comparable to the incidence reported by other studies (1,10). Our diagnostic criteria of BE and lesions suggestive for GERD gastric carditis are the same as those of Montgomery (10).

Lipoxygenases (LOXs) are significant enzymes that metabolize AA to hydroxyl-eicosatetraenoic acids (HETE) and leukotrienes involved in inflammatory and carcinogenic processes. Platelet 12-LOX metabolite 12S-HETE affects cell proliferation and apoptosis on the signal transduction pathway mediated by ERK (11). Limited information related to the role and expression of LOX in BE is currently available. 5-LOX showed immunohistochemical overexpression during esophageal adenocarcinogenesis (12). 5- and 12-LOX are regarded as pro-tumorigenic enzymes in colonic carcinogenesis and their overexpression was also described in various types of cancer [(13–16) and references therein]. The new antibodies developed for this study were the first on the market with specificity for the whole-length enzyme and with proven lack of any cross-reactivity with other human LOXs. Our studies have shown the usefulness of these new antibodies for immunohistochemical studies of parafin-embedded samples in melanoma, prostate, uteral and kidney cancers (data not shown) in addition to the gastrointestinal samples discussed in this study.

Our findings showed extremely high immunoreactivity of the two p12LOX antibodies in non-dysplastic BE and Barrett’s dysplasia, thereby confirming the pro-carcinogenic activity of platelet 12-LOX and suggesting the diagnostic utility of the two antibodies in GERD and BE.

CD44 is a cell surface molecule enrolled in cell-cell and cell-extracellular matrix protein interactions. In particular, its spliced variants 5 and 6 have been shown to play a role in the progression of certain tumors, including gastric carcinoma. According to Menges et al (9), the expression of CD44 noted in Barrett’s carcinoma did not increase compared to non-dysplastic BE and was completely negative in gastric mucosa. Other investigators (8,17) showed that CD44 progressively increases in Barrett’s dysplasia and adenocarcinoma.

Stem cell markers CD44 and nestin, as shown in our study, are potential markers of malignant transformation in BE, similar to intestinal metaplasia of the stomach (17,18). Our study results also showed that p12LOX and stem-cell immunoreactivity is much higher in BE when compared to other gastrointestinal mucosal cancer precursor lesions and suggests a more active pre-neoplastic transformation of Barrett’s mucosa.