Thus, roles of other virulent bacterial species should be further explored Selleckchem Cilomilast to explain the reasons why more advanced stages of atrophy have a higher risk for gastric cancer and to solve the so-called Asian or African enigma. Valid diagnosis of IM can only be done by histological examination of biopsied mucosa. Indeed, poor agreement between endoscopic diagnosis and that of histology was documented. In a Japanese pilot study, endoscopic diagnosis of IM had a high specificity (99%) but the sensitivity was surprisingly poor; only 12% of histologically confirmed IM was diagnosed by endoscopy.[22] However, modern endoscopic imaging modalities,
such as narrow band imaging (NBI), flexible intelligent color enhancement
(FICE), and blue-laser imaging (BLI), can facilitate identification ACP-196 molecular weight of IM and dysplastic or cancerous lesions[23-25] (Fig. 6a,b). Once IM is identified during endoscopic examinations, high levels of vigilance should be exerted to search for dysplastic or cancerous lesions, because patients with IM have a higher risk of harboring such neoplastic lesions (Fig. 6b). Also important is to eradicate H. pylori if positive. Eradication has dual benefits: reduction of inflammation by H. pylori, a major culprit of inflammation and restoration of acid secretion which can reduce bacterial overgrowth in the majority of patients.[26] Whether eradication of H. pylori can revert IM is controversial. Most of the studies, however, could not demonstrate significant improvement of IM,[2] which may be explained by the auto-regulatory mechanism of CDX2.[27] Thus, medchemexpress in the majority of cases, it is most likely that IM with genetic derangements remains after eradication therapy. As mentioned before,
continuous development of gastric cancer long after successful eradication therapy also support that patients with atrophy and/or IM are recommended to receive follow-up endoscopic examinations. If dysplastic lesions are detected during endoscopy, endoscopic mucosal resection should be considered if feasible. Even in Japan, where pathologists are well-experienced in the diagnosis of GC, biopsy-based diagnosis has to be corrected after entire lesions being checked (Table 2). This is not because some of the lesions satisfy the “invasion criteria,” but because distinct cellular and/or structural disorganization or identification of cancerous foci in adenomas (cancer in adenoma, Fig. 4a,b) can only become evident after examination of whole resected materials. Since in many Western countries, “invasive criterion” is necessary for the diagnosis of cancer; diagnosis based on biopsy alone tend to be insufficient, because it would be difficult to take biopsy materials targeted to a locally invaded area even with modern imaging modalities as the invasive front resides in the submucosa (Fig. 4a,b).
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