Differential expression of CD95, Bcl‐2, and Bax in rat gastric chief and parietal cells

Neu, Bruno; Herrmuth, H.; Ernst, Friedlinde; Vaupel, Wolfgang; Reindl, Wolfgang; Hutzler, Peter; Atkinson, Michael J.; Classen, Meinhard; Schepp, Wolfgang

doi:10.1002/jemt.1106

Cited by 5 publications

(15 citation statements)

References 37 publications

(41 reference statements)

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“…Chief cell cultures made from these highly purified cells were used 2 days after seeding, but it was not mentioned whether they were confluent or not. Additionally, it was demonstrated that cultures made from highly purified chief cells showed a significant reduction in the expression of some proteins found in mature chief cells in vivo (20). Our results show that chief cells in culture must be confluent with a high cell density to, both functionally and structurally, express a phenotype that is similar to chief cells, in vivo.…”

Section: Discussionmentioning

confidence: 53%

“…Although this has been accomplished before with chief cells isolated from the dog stomach (2,26,27), such a culture system in rodent species has not been described. In previous studies using chief cells isolated from the rat stomach, cultures were made either by using mixed mucosal cells with no purification (30,31) or by preparing highly purified chief cells (85 Ϯ 11% pure) by elutriation and Percoll density gradient centrifugation (20). Chief cell cultures made from these highly purified cells were used 2 days after seeding, but it was not mentioned whether they were confluent or not.…”

Section: Discussionmentioning

confidence: 99%

“…For this, cells isolated by collagenase digestion were purified by centrifugal elutriation to yield cultures with a high transepithelial resistance (TER) and low permeability that maintained differentiated function as shown by agonist-induced pepsinogen secretion (2,26). Since the procedure was developed, short-term cultures have been produced from isolated human and rabbit (10), guinea pig (25), pig (12), and rat (20,30,31) chief cells. Although isolated chief cells and short-term cultured cells from all species secrete pepsinogen (10,12,25,31), it is not currently possible to produce a confluent monolayer of chief cells with a high TER, low permeability, and high rate of agonist-induced pepsinogen secretion from a species other than dog.…”

Section: Gastric; Methods; Zymogenic Cellsmentioning

confidence: 99%

“…Animals used for this study were maintained in accordance with the guidelines of the Committee on Animals at the Beth Israel Deaconess Medical Center and all animal experiments were done with IACUC-approved protocols. Isolated chief cells were prepared from the rat stomach (Sprague-Dawley; Taconic, Germantown, NY) by density gradient and centrifugal elutriation techniques as described previously by others (3)(4)(5)(6)(7)20) and modified by us to obtain highly enriched chief cells from the rat stomach. In brief, nonfasted rats, weighing no more than 200 g, were anesthetized with pentobarbital sodium.…”

Section: Methodsmentioning

confidence: 99%

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Hepatocyte growth factor regulates the development of highly pure cultured chief cells from rat stomach by stimulating chief cell proliferation in vitro

Tashima

Zhang²,

Ragasa³

et al. 2009

American Journal of Physiology-Gastrointestinal and Liver Physi

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Tashima K, Zhang S, Ragasa R, Nakamura E, Seo JH, Muvaffak A, Hagen SJ. Hepatocyte growth factor regulates the development of highly pure cultured chief cells from rat stomach by stimulating chief cell proliferation in vitro. Am J Physiol Gastrointest Liver Physiol 296: G319 -G329, 2009. First published November 20, 2008 doi:10.1152/ajpgi.90355.2008.-The physiology of gastric epithelial cells is often studied by using cancer cell lines, which may or may not provide information relevant to normal cells. Because few models exist to study chief cell physiology in vitro, our purpose was to develop primary cultured chief cells from rodent species that are structurally and functionally similar to native chief cells. For this, isolated chief cells from the rat stomach, purified by counterflow elutriation and density gradient centrifugation, were grown in media with growth factors. Purity and the continuity of tight junctions were determined, and permeability, viability, transepithelial resistance (TER), cell number and proliferation, and pepsinogen secretion in response to carbachol were measured. When plated in media alone or with basic fibroblast growth factor, the isolated chief cells attached by 2 days and were confluent by 4 days after seeding. However, tight junctions were discontinuous, TER was less than 300 ⍀ ⅐ cm 2 , and permeability was high. In contrast, chief cells incubated with hepatocyte growth factor (HGF) were confluent in 3 days and had a TER greater than 2,000 ⍀ ⅐ cm 2 , continuous tight junctions, and low permeability. EGF was intermediate. HGF facilitated monolayer development by increasing cell number, which occurred by the proliferation of chief cells. Chief cell cultures, grown with HGF, consisted of more than 99% gastric intrinsic factor-expressing cells and showed robust pepsinogen secretion. Coexpression studies for neck and chief cell markers suggest that the cultures are a mixture of mature, immature, and transitional zone cells. This model will be useful for investigating mechanisms that regulate chief cell physiology in health and disease. gastric; methods; zymogenic cells HELICOBACTER PYLORI (HP) or felis infection in animal models including mice, guinea pigs, and Mongolian gerbils has been instrumental in helping to elucidate mechanisms that are important in the pathogenesis of corpus-predominant HP disease, including inflammation, atrophy, metaplasia, and the progression to gastric cancer (9,11,14,23,32). However, detailed mechanistic studies concerning HP infection in gastric epithelial cells are often not done because of a lack of appropriate culture models. For instance, it is difficult to study how bacterial virulence factors such as vacA and cagA alter cellspecific signaling pathways and function in gastric epithelial cells. In addition, it is currently not possible to study the way in which HP infection alters the gastric mucosal barrier, both at the surface and within gastric glands, or to determine how HP-associated inflammation influences cell-specific survival and death path...

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Section: Discussionmentioning

confidence: 53%

Section: Discussionmentioning

confidence: 99%

Section: Gastric; Methods; Zymogenic Cellsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 2 more Smart Citations

Hepatocyte growth factor regulates the development of highly pure cultured chief cells from rat stomach by stimulating chief cell proliferation in vitro

Tashima

Zhang²,

Ragasa³

et al. 2009

American Journal of Physiology-Gastrointestinal and Liver Physi

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“…Apoptosis mediated through the Fas antigen surface receptor pathway plays a central role in Helicobacter-induced gastric mucosal disease in which Fas signaling facilitates parietal and chief cell depletion early in infection (30)(31)(32). Surface Fas antigen expression is markedly up-regulated in the gastric mucosa during infection (33) and is expressed at the highest levels on chief and parietal cell populations.…”

Section: Introductionmentioning

confidence: 99%

Overcoming Fas-Mediated Apoptosis Accelerates Helicobacter-Induced Gastric Cancer in Mice

Cai

Stoicov

et al. 2005

Cancer Research

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The initiating molecular events in Helicobacter -induced gastric carcinogenesis are not known. Early in infection, Fas antigen-mediated apoptosis depletes parietal and chief cell populations, leading to architectural distortion. As infection progresses, metaplastic and dysplastic glands appear, which are resistant to Fas-mediated apoptosis. These abnormal lineages precede, and are thought to be the precursor lesions of, gastric cancer. Acquisition of an antiapoptotic phenotype before transformation of cells suggests that loss of Fas sensitivity may be an early required trait for gastric cancer. We reasoned that forced Fas-apoptosis resistance would result in earlier and more aggressive gastric cancer in our mouse model. Fas antigen-deficient (lpr) mice or C57BL/6 wild-type mice were irradiated and reconstituted with C57BL/6 marrow forming partial lpr/wt chimera or wt/wt control mice, extending the life span of the lpr and ensuring a competent immune response to Helicobacter felis infection. Infected lpr/ wt mice developed gastric cancer as early as 7 months after infection (compared with 15 months in wt/wt mice). At 10 months (90%) and 15 months (100%), mice developed aggressive invasive lesions. This earlier onset and more aggressive histology strongly argues that Fas-apoptosis resistance is an early and important feature of gastric cancer formation. (Cancer Res 2005; 65(23): 10912-20)

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Heat shock preconditioning modulates proliferation and apoptosis after superficial injury in isolated guinea pig gastric mucosa via an eicosanoid and protein synthesis‐dependent mechanism

Oksala

Paavonen

et al. 2003

APMIS

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Differential expression of CD95, Bcl‐2, and Bax in rat gastric chief and parietal cells

Cited by 5 publications

References 37 publications

Hepatocyte growth factor regulates the development of highly pure cultured chief cells from rat stomach by stimulating chief cell proliferation in vitro

Hepatocyte growth factor regulates the development of highly pure cultured chief cells from rat stomach by stimulating chief cell proliferation in vitro

Overcoming Fas-Mediated Apoptosis Accelerates Helicobacter-Induced Gastric Cancer in Mice

Heat shock preconditioning modulates proliferation and apoptosis after superficial injury in isolated guinea pig gastric mucosa via an eicosanoid and protein synthesis‐dependent mechanism

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