Comparative histochemical study of alimentary tracts with special reference to the mucous neck cells of the stomach

Suganuma, Tatsuo; Katsuyama, Tsutomu; Tsukahara, Masanori; Tatematsu, Masae; Sakakura, Yasunori; Murata, Fusayoshi

doi:10.1002/aja.1001610206

Cited by 93 publications

(63 citation statements)

References 14 publications

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“…The latter, which includes cardiac gland cells, mucous neck cells, and pyloric gland cells, possess class III mucin, as identified by paradoxical concanavalin A staining (Katsuyama and Spicer 1978;Suganuma et al 1981;Ota et al 2001). In normal human tissues, class III mucin is expressed in gastric gland mucous cells, Brunner's gland cells, and mucous cells of the accessory glands of the pancreaticobiliary tract (Katsuyama and Spicer 1978;Suganuma et al 1981;Ota et al 1991Ota et al ,1998Nakamura et al 1998). Class III mucin is also expressed in gastric metaplasia of the gallbladder (Tsutsumi et al 1984) and mucinous metaplasia of the pancreas (Matsuzawa et al 1992;Ota et al 2001;Zhang et al 2001), and in carcinoma of stomach (Akamatsu and Katsuyama 1990;Lesuffleur et al 1994;Fujimori et al 1995;Nakamura et al 1998;Ota et al 2001), bile duct (Kijima et al 1989;Ota et al 1995), gallbladder (Tsutsumi et al 1984), and pancreas (Matsuzawa et al 1992;Nakamura et al 1998;Ota et al 2001), as well as in mucinous bronchioloalveolar cell carcinoma of the lung (Honda et al 1998;Ota et al 2001) and adenoma malignum of the uterine cervix (Ishii et al ,1999 Several years ago, Ishihara et al (1996) raised a specific monoclonal antibody (MAb) against gastric mucin, designated HIK1083, which recognizes N -acetylglucosamin ␣ 1 → 4galactose ␤ → R (GlcNAc ␣ 1 → 4Gal ␤ → R).…”

mentioning

confidence: 99%

Expression of Gastric Gland Mucous Cell-Type Mucin in Normal and Neoplastic Human Tissues

Nakajima

Ota²,

Zhang³

et al. 2003

J Histochem Cytochem.

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S U M M A R YGastric gland mucous cells produce class III mucin, which is also found in Brunner's glands and mucous glands along the pancreaticobiliary tract, and in metaplasia and adenocarcinomas differentiating towards gastric mucosa. Recently, we showed that class III mucin possesses GlcNAc ␣ 1 → 4Gal ␤ → R, formed by ␣ 1,4-N -acetylglucosaminyltransferase ( ␣ 4GnT). Examining the tissue-specific expression of mucin epitopes is useful to clarify celllineage differentiation and to identify the site of origin of metastatic carcinomas in histological specimens. Formalin-fixed, paraffin-embedded tissue sections from esophagus, stomach, colon, liver, pancreas, lung, kidney, prostate, breast, and salivary gland resected for carcinoma, as well as salivary gland adenoma, colon adenoma, and metastatic adenocarcinoma of lymph nodes from stomach, pancreas, colon, and breast, were immunostained for MUC6, ␣ 4GnT, and GlcNAc ␣ 1 → 4Gal ␤ → R. These were all expressed in normal, metaplastic, and adenocarcinoma tissues of stomach, pancreas, and bile duct, and in pulmonary mucinous bronchioloalveolar carcinomas. Cells expressing ␣ 4GnT uniformly expressed GlcNAc ␣ 1 → 4Gal ␤ → R. Only MUC6 was expressed in normal salivary glands, pancreas, seminal vesicles, renal tubules, and colon adenomas, and in normal tissue and adenocarcinomas of prostate and breast. No tissues showed immunoreactivity for ␣ 4GnT alone. Immunohistochemistry (IHC) profiles were similar for metastatic carcinomas and primary carcinoma tissues. The IHC profiles for MUC6, ␣ 4GnT, and GlcNAc ␣ 1 → 4Gal ␤ → R may be diagnostically relevant.

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mentioning

confidence: 99%

Expression of Gastric Gland Mucous Cell-Type Mucin in Normal and Neoplastic Human Tissues

Nakajima

Ota²,

Zhang³

et al. 2003

J Histochem Cytochem.

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“…According to Suganuma and coworkers [12], amphibians were the first vertebrates to develop true mucous neck cells, which are the precursors of chief cells via intermediate cells [31]. In anurans, mucins are produced by goblet cells found in the esophagus and the intestines, but also by epithelial cells and mucous neck cells in the stomach [43].…”

Section: Discussionmentioning

confidence: 99%

“…Histochemical studies indicate differences regarding the qualitative expression of neutral, sulfated, and carboxylated mucosubstances [10,11]. The mucosubstances, which phylogenetically first appeared in mucous neck cells of the gastric glands of anurans [12], have already been reported for Rana aurora aurora [13], Bufo viridis [14], Rana perezi [15], Bufo melanostictus [3], and Bufo marinus [16], indicating variability among anuran species. Furthermore, different types of carbohydrates were identified in secretory cells in the stomach of Bufo viridis [17,18] and Rana esculenta [19].…”

Section: Introductionmentioning

confidence: 99%

Histochemical and Immunohistochemical Analysis of the Stomach of Rhinella icterica (Anura, Bufonidae)

Machado-Santos

Pelli-Martins

Figueiredo

et al. 2014

Journal of Histology

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The stomach of Rhinella icterica was analyzed at light microscopy, employing histochemical techniques, lectin histochemistry, and immunohistochemistry for identifying enteroendocrine cells (EC). Although the stomach was composed of fundic and pyloric regions, its wall is formed by mucosa, submucosa, muscularis, and serosa. The mucosa was lined by a simple columnar mucous epithelium, supported by loose connective tissue. Several tubular, simple glands were composed of mucous neck cells, containing oxynticopeptic cells and EC cells. The mucous neck cells were rich in neutral glycoconjugates. The oxynticopeptic cells were predominant in fundic glands, exhibiting weaker alcianophilic reaction at their apical cytoplasm. Serotonin (5-HT) immunoreactive (IR) cells occurred throughout the entire stomach, preferentially located among mucous cells at upper part of the fundic glands. The muscularis mucosae, formed of smooth muscle, separated the mucosal layer from the submucosa, both of which were constituted by loose connective tissue, but without glands. Lymphoid modules occurred in the mucosa at the boundary at the stomach and the gut. In addition, the muscularis was constituted by two sublayers, the circular internal and the longitudinal external, being recovered by the connective tissue of the serosa.

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“…Surface mucous cells stain blue with galactose oxidase cold thionin Schiff reaction (GOCTS) [55] or stain red with galactose oxidase Schiff reaction (GOS) [34,35,62], and show immunoreactivity to cathepsin E [74]. In contrast, glandular mucous cells exhibit class III Con A reactivity with paradoxical Concanavalin A staining (PCS) [1,33,34,37,46,55,72,75] and show immunoreactivity to lysozyme [17,58], pepsinogens [17,75]. With immunostaining for pepsinogens, secretory granules of the mucous neck cells and chief cells stained for pepsinogen type I [17,75].…”

Section: Characterization Of Gastric Mucous Cellsmentioning

confidence: 99%

“…We and others have previously described the different histochemical reactivities of these two types of mucous cells, surface mucous cells and glandular mucous cells [33,34,36,37,55,63,72,76]. Surface mucous cells stain blue with galactose oxidase cold thionin Schiff reaction (GOCTS) [55] or stain red with galactose oxidase Schiff reaction (GOS) [34,35,62], and show immunoreactivity to cathepsin E [74].…”

Section: Characterization Of Gastric Mucous Cellsmentioning

confidence: 99%

Application of Mucin Histochemistry for Pathological Diagnosis. Expression of Gastric Phenotypes in Metaplastic and Neoplastic Lesions and its Relation to the Organoid Differentiation.

Ota

Katsuyama

Akamatsu

et al. 1995

Acta Histochem. Cytochem

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Comparative histochemical study of alimentary tracts with special reference to the mucous neck cells of the stomach

Cited by 93 publications

References 14 publications

Expression of Gastric Gland Mucous Cell-Type Mucin in Normal and Neoplastic Human Tissues

Expression of Gastric Gland Mucous Cell-Type Mucin in Normal and Neoplastic Human Tissues

Histochemical and Immunohistochemical Analysis of the Stomach of Rhinella icterica (Anura, Bufonidae)

Application of Mucin Histochemistry for Pathological Diagnosis. Expression of Gastric Phenotypes in Metaplastic and Neoplastic Lesions and its Relation to the Organoid Differentiation.

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