Background and Study Aims: Endoscopic resection has been recommended as a local curative approach for Barrett’s
neoplasia, but large series are still rare. In the present study we analyzed the histological
characteristics of endoscopic resection specimens of Barrett’s neoplasia.
Patients and Methods: 742 endoscopic resection specimens obtained from 326 patients were assessed. The
following histological characteristics were evaluated: type of neoplasia, grade of
differentiation, depth of infiltration, invasion into lymphatic and blood vessels,
and resection status (tumor-free margins were regarded as indicating R0 status).
Results: 31 patients had no neoplasia and were excluded from the analysis. Among the remaining
295 patients (711 resection specimens), histological findings were: low-grade intraepithelial
neoplasia, 1.0 %; high-grade intraepithelial neoplasia, 2.7 %; and mucosal carcinoma
80.3 %. Carcinomas infiltrating the submucosal layer were rare (sm1 7.5 %; sm2 3.7
%; sm3 4.8 %), as were those invading lymph vessels (3.5 %), and there were none with
venous invasion. Most of the carcinomas were well-differentiated (72.2 %), and many
of these (92.7 %) were limited to the mucosa, in contrast to moderately and poorly
differentiated carcinomas (73.7 % and 22.7 %, respectively). R0 status was achieved
in 74.5 % of patients; in 47.8 % this was after repeated endoscopic resection. In
26.8 % of patients, R0 resection was achieved at the first attempt.
Conclusions: Our study demonstrates that early Barrett’s neoplasms removed by endoscopic resection
are mostly limited to the mucosa, are well to moderately differentiated, and very
rarely show invasion of the lymph or blood vessels. Although these lesions seem to
be low risk with regard to metastatic spread and therefore treatable endoscopically,
improved endoscopic resection methods for achieving one-piece (en bloc) R0 resection
should be developed.
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M. Stolte, M. D.
Institute of Pathology
Preuschwitzerstr. 101 · 95445 Bayreuth · Germany ·
Fax: +49-921-4005609
Email: michael.vieth@medizin.uni-magdeburg.de