Cathepsin E Is a Marker of Gastric Differentiation and Signet-Ring Cell Carcinoma of Stomach: A Novel Suggestion on Gastric Tumorigenesis | Zendy

Maki KonnoShimizu | Zendy; Nobutake Yamamichi | Zendy; Ken-ichi Inada | Zendy; Natsuko KageyamaYahara | Zendy; Kazuya Shiogama | Zendy; Yu Takahashi | Zendy; Itsuko AsadaHirayama | Zendy; Mitsue Yamamichi-Nishina | Zendy; Chiemi Nakayama | Zendy; Satoshi Ono | Zendy; Shinya Kodashima | Zendy; Mitsuhiro Fujishiro | Zendy; Yutaka Tsutsumi | Zendy; Masao Ichinose | Zendy; Kazuhiko Koike | Zendy

Open Access

Cathepsin E Is a Marker of Gastric Differentiation and Signet-Ring Cell Carcinoma of Stomach: A Novel Suggestion on Gastric Tumorigenesis

Author(s) -

Maki KonnoShimizu,

Nobutake Yamamichi,

Ken-ichi Inada,

Natsuko KageyamaYahara,

Kazuya Shiogama,

Yu Takahashi,

Itsuko AsadaHirayama,

Mitsue Yamamichi-Nishina,

Chiemi Nakayama,

Satoshi Ono,

Shinya Kodashima,

Mitsuhiro Fujishiro,

Yutaka Tsutsumi,

Masao Ichinose,

Kazuhiko Koike

Publication year - 2013

Publication title -

plos one

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.99

H-Index - 332

ISSN - 1932-6203

DOI - 10.1371/journal.pone.0056766

Subject(s) - intestinal metaplasia , adenocarcinoma , cathepsin e , pathology , signet ring cell carcinoma , stomach , cancer , biology , medicine , cathepsin , biochemistry , cathepsin o , enzyme

Gastric cancer (GC) presents various histological features, though the mechanism underlying its diversity is seldom elucidated. It is mainly classified into well differentiated tubular adenocarcinoma (tub1), moderately differentiated tubular adenocarcinoma (tub2), poorly differentiated adenocarcinoma (por), signet-ring cell carcinoma (sig), mucinous adenocarcinoma (muc), and papillary adenocarcinoma (pap). By screening, we found cathepsin E (CTSE) expresses universally in sig-type, occasionally in por-type, and rarely in tub1/tub2-type GC cell lines. In surgically-resected specimens, CTSE was immunostained in 50/51 sig-type (98.0%), 3/10 tub1-type (30.0%), 7/18 tub2-type (38.9%), 15/26 por-type (57.7%), 4/10 pap-type (40.0%), and 0/3 muc-type (0.0%) GC. In endoscopically-resected specimens, 6/7 sig-type (85.7%), 7/52 tub1-type (13.7%), 5/12 tub2-type (41.7%), 2/7 pap-type (28.6%) GC and 0/6 adenoma (0.0%) expressed CTSE. For non-malignant tissues, CTSE is universally expressed in normal fundic, pyloric, and cardiac glands of stomach, but hardly in other digestive organs. In the precancerous intestinal metaplasia of stomach, CTSE is mostly observed in mixed gastric-and-intestinal type and deficient in solely-intestinal type. CTSE expression is positively correlated with gastric marker MUC5AC ( p <0.0001) and negatively correlated with intestinal marker MUC2 ( p = 0.0019). For sig-type GC, in both tumors and background mucosa, expression of MUC5AC and CTSE is high whereas that of MUC2 is low, indicating that sig-type GC reflects the features of background mucosa. For gastric adenoma and tub1/tub2-type GC, more undifferentiated tumors tend to show higher expression of CTSE with MUC5AC and lower expression of MUC2 in tumors, but they tend to present lower expression of CTSE, MUC5AC and MUC2 in background mucosa. These suggest that more malignant gastric adenocarcinoma with stronger gastric and weaker intestinal properties tend to arise from background mucosa with decreased both gastric and intestinal features. In conclusion, CTSE is a marker of both gastric differentiation and signet-ring cell carcinoma, which should shed light on the mechanism of gastric tumorigenesis.

The content you want is available to Zendy users.

Already have an account? Click here to sign in.

Having issues? You can contact us here

Accelerating Research