Your search keyword '"Intestines -- Genetic aspects"' showing total 26 results

1. DGAT1 mutation is linked to a Congenital diarrheal disorder

Author

Haas, Joel T., Winter, Harland S., Lim, Elaine, Kirby, Andrew, Blumenstiel, Brendan, DeFelice, Matthew, Gabriel, Stacey, Jalas, Chaim, Branski, David, Grueter, Carrie A., Toporovski, Mauro S., Walther, Tobias C., Daly, Mark J., and Farese, Jr., Robert V.

Subjects

Gene mutations -- Identification and classification, Intestines -- Genetic aspects, Birth defects -- Diagnosis -- Care and treatment, Diarrhea -- Diagnosis -- Care and treatment -- Genetic aspects, Health care industry

Abstract

Congenital diarrheal disorders (CDDs) are a collection of rare, heterogeneous enteropathies with early onset and often severe outcomes. Here, we report a family of Ashkenazi Jewish descent, with 2 out of 3 children affected by CDD. Both affected children presented 3 days after birth with severe, intractable diarrhea. One child died from complications at age 17 months. The second child showed marked improvement, with resolution of most symptoms at 10 to 12 months of age. Using exome sequencing, we identified a rare splice site mutation in the DGAT1 gene and found that both affected children were homozygous carriers. Molecular analysis of the mutant allele indicated a total loss of function, with no detectable DGAT1 protein or activity produced. The precise cause of diarrhea is unknown, but we speculate that it relates to abnormal fat absorption and buildup of DGAT substrates in the intestinal mucosa. Our results identify DGAT1 loss-of-function mutations as a rare cause of CDDs. These findings prompt concern for DGAT1 inhibition in humans, which is being assessed for treating metabolic and other diseases., Introduction Congenital diarrheal disorders (CDDs) are rare and heterogeneous enteropathies, often with severe clinical manifestations (1), (2). Those whose cause has been identified typically result from autosomal recessive mutations. Affected [...]

Published

2012

2. A uroguanylin-GUCY2C endocrine axis regulates feeding in mice

Author

Valentino, Michael A., Lin, Jieru E., Snook, Adam E., Li, Peng, Kim, Gilbert W., Marszalowicz, Glen, Magee, Michael S., Hyslop, Terry, Schulz, Stephanie, and Waldman, Scott A.

Subjects

Satiation -- Genetic aspects, Intestines -- Genetic aspects, Cellular signal transduction -- Genetic aspects, Appetite -- Genetic aspects, Health care industry

Abstract

Intestinal enteroendocrine cells are critical to central regulation of caloric consumption, since they activate hypothalamic circuits that decrease appetite and thereby restrict meal size by secreting hormones in response to nutrients in the gut. Although guanylyl cyclase and downstream cGMP are essential regulators of centrally regulated feeding behavior in invertebrates, the role of this primordial signaling mechanism in mammalian appetite regulation has eluded definition. In intestinal epithelial cells, guanylyl cyclase 2C (GUCY2C) is a transmembrane receptor that makes cGMP in response to the paracrine hormones guanylin and uroguanylin, which regulate epithelial cell dynamics along the crypt-villus axis. Here, we show that silencing of GUCY2C in mice disrupts satiation, resulting in hyperphagia and subsequent obesity and metabolic syndrome. This defined an appetite-regulating uroguanylin-GUCY2C endocrine axis, which we confirmed by showing that nutrient intake induces intestinal prouroguanylin secretion into the circulation. The prohormone signal is selectively decoded in the hypothalamus by proteolytic liberation of uroguanylin, inducing GUCY2C signaling and consequent activation of downstream anorexigenic pathways. Thus, evolutionary diversification of primi-tive guanylyl cyclase signaling pathways allows GUCY2C to coordinate endocrine regulation of central food acquisition pathways with paracrine control of intestinal homeostasis. Moreover, the uroguanylin-GUCY2C endocrine axis may provide a therapeutic target to control appetite, obesity, and metabolic syndrome., Introduction Body mass reflects central regulation of caloric consumption by enteroendocrine cells that sense nutrients in the gastrointestinal tract and secrete hormones that activate hypothalamic circuits limiting meal size (1). [...]

Published

2011

3. Paneth cells constitute the niche for Lgr5 stem cells in intestinal crypts

Author

Sato, Toshiro, van Es, Johan H., Snippert, Hugo J., Stange, Daniel E., Vries, Robert G., van den Born, Maaike, Barker, Nick, Shroyer, Noah F., van de Wetering, Marc, and Clevers, Hans

Subjects

Intestines -- Genetic aspects, Stem cell research -- Health aspects -- Physiological aspects, Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

Homeostasis of self-renewing small intestinal crypts results from neutral competition between Lgr5 stem cells, which are small cycling cells located at crypt bottoms (1,2). Lgr5 stem cells are interspersed between terminally differentiated Paneth cells that are known to produce bactericidal products such as lysozyme and cryptdins/defensins (3). Single Lgr5-expressing stem cells can be cultured to form long-lived, self-organizing crypt-villus organoids in the absence of non-epithelial niche cells (4). Here we find a close physical association of Lgr5 stem cells with Paneth cells in mice, both in vivo and in vitro. [CD24.sup.+] Paneth cells express EGF, TGF-α, Wnt3 and the Notch ligand Dll4, all essential signals for stem-cell maintenance in culture. Co-culturing of sorted stem cells with Paneth cells markedly improves organoid formation. This Paneth cell requirement can be substituted by a pulse of exogenous Wnt. Genetic removal of Paneth cells in vivo results in the concomitant loss of Lgr5 stem cells. In colon crypts, [CD24.sup.+] cells residing between Lgr5 stem cells may represent the Paneth cell equivalents. We conclude that Lgr5 stem cells compete for essential niche signals provided by a specialized daughter cell, the Paneth cell., In a Matrigel-based culture system containing EGF, the Wnt agonist R-spondin 1 and the BMP inhibitor noggin (4), single Lgr5 stem cells autonomously grow into crypt-like structures with de novo [...]

Published

2011

4. Hippo signaling regulates Drosophila intestine stem cell proliferation through multiple pathways

Author

Ren, Fangfang, Wang, Bing, Yue, Tao, Yun, Eun-Young, Ip, Y. Tony, and Jiang, Jin

Subjects

Stem cells -- Genetic aspects, Drosophila -- Physiological aspects, Drosophila -- Genetic aspects, Intestines -- Genetic aspects, Intestines -- Physiological aspects, Science and technology

Abstract

Intestinal stem cells (ISCs) in the Drosophila adult midgut are essential for maintaining tissue homeostasis and replenishing lost cells in response to tissue damage. Here we demonstrate that the Hippo (Hpo) signaling pathway, an evolutionarily conserved pathway implicated in organ size control and tumorigenesis, plays an essential role in regulating ISC proliferation. Loss of Hpo signaling in either midgut precursor cells or epithelial cells stimulates ISC proliferation. We provide evidence that loss of Hpo signaling in epithelial cells increases the production of cytokines of the Upd family and multiple EGFR ligands that activate JAK-STAT and EGFR signaling pathways in ISCs to stimulate their proliferation, thus revealing a unique non--cell-autonomous role of Hpo signaling in blocking ISC proliferation. Finally, we show that the Hpo pathway mediator Yorkie (Yki) is also required in precursor cells for injury-induced ISC proliferation in response to tissue-damaging reagent DSS. Yap | wts | regeneration doi/ 10.1073/pnas.1012759107

Published

2010

5. Functional and phenotypic characterization of a protein from Lactobacillus acidophilus involved in cell morphology, stress tolerance and adherence to intestinal cells

Author

O'Flaherty, Sarah J. and Klaenhammer, Todd R.

Subjects

Cells -- Physiological aspects, Cells -- Research, Intestines -- Physiological aspects, Intestines -- Research, Intestines -- Genetic aspects, Lactobacillus acidophilus -- Health aspects, Lactobacillus acidophilus -- Research, Genes -- Physiological aspects, Genes -- Research, Biological sciences

Abstract

Structural components of the cell surface have an impact on some of the beneficial attributes of probiotic bacteria. In silico analysis of the L. acidophilus NCFM genome sequence revealed the presence of a putative cell surface protein that was predicted to be a myosin cross-reactive antigen (MCRA). As MCRAs are conserved among many probiotic bacteria, we used the upp-based counterselective gene replacement system, designed recently for use in L. acidophilus, to determine the functional role of this gene (LBA649) in L. acidophilus NCFM. Phenotypic assays were undertaken with the parent strain (NCK1909) and deletion mutant (NCK2015) to assign a function for this gene. The growth of NCK2015 (ALBA649) was reduced in the presence of lactate, acetate, porcine bile and salt. Adhesion of NCK2015 to Caco-2 cells was substantially reduced for both stationary-phase (~45% reduction) and exponential-phase cells (~50% reduction). Analysis of NCK2015 by scanning electron microscopy revealed a longer cell morphology after growth in MRS broth compared to NCK1909. These results indicate a role for LBA649 in stress tolerance, cell wall division and adherence to Caco-2 cells. DOI 10.1099/mic.0.043158-0

Published

2010

6. TCF4 and CDX2, major transcription factors for intestinal function, converge on the same cis-regulatory regions

Author

Verzi, Michael P., Hatzis, Pantelis, Sulahian, Rita, Philips, Juliet, Schuijers, Jurian, Shin, Hyunjin, Freed, Ellen, Lynch, John P., Dang, Duyen T., Brown, Myles, Clevers, Hans, Liu, X. Shirley, and Shivdasani, Ramesh A.

Subjects

Transcription factors -- Health aspects, Intestines -- Health aspects, Intestines -- Genetic aspects, Gene expression -- Research, Science and technology

Abstract

Surprisingly few pathways signal between cells, raising questions about mechanisms for tissue-specific responses. In particular, Wnt ligands signal in many mammalian tissues, including the intestinal epithelium, where constitutive signaling causes cancer. Genomewide analysis of DNA cis-regulatory regions bound by the intestine-restricted transcription factor CDX2 in colonic cells uncovered highly significant overrepresentation of sequences that bind TCF4, a transcriptional effector of intestinal Wnt signaling. Chromatin immunoprecipitation confirmed TCF4 occupancy at most such sites and cooccupancy of CDX2 and TCF4 across short distances. A region spanning the single nucleotide polymorphism rs6983267, which lies within a MYC enhancer and confers colorectal cancer risk in humans, represented one of many co-occupied sites. Co-occupancy correlated with intestine-specific gene expression and CDX2 loss reduced TCF4 binding. These results implicate CDX2 in directing TCF4 binding in intestinal cells. Co-occupancy of regulatory regions by signal-effector and tissue-restricted transcription factors may represent a general mechanism for ubiquitous signaling pathways to achieve tissue-specific outcomes. context specificity of signaling | genome-wide chromatin immunoprecipitation | signaling | Wnt signaling in intestine | tissue-specific gene regulation doi/ 10.1073/pnas.1003822107

Published

2010

7. Nod2 is required for the regulation of commensal microbiota in the intestine

Author

Petnicki-Ocwieja, Tanja, Hrncir, Tomas, Liu, Yuen-Joyce, Biswas, Amlan, Hudcovic, Tomas, Tlaskalova-Hogenova, Helena, and Kobayashi, Koichi S.

Subjects

Microbiota (Symbiotic organisms) -- Health aspects, Intestines -- Genetic aspects, Intestines -- Health aspects, Crohn's disease -- Development and progression, Crohn's disease -- Genetic aspects, Genetic regulation -- Research, Science and technology

Abstract

Mutations in the Nod2 gene are among the strongest genetic risk factors in the pathogenesis of ileal Crohn's disease, but the exact contributions of Nod2 to intestinal mucosal homeostasis are not understood. Here we show that Nod2 plays an essential role in controlling commensal bacterial flora in the intestine. Analysis of intestinal bacteria from the terminal ilea of Nod2-deficient mice showed that they harbor an increased load of commensal resident bacteria. Furthermore, Nod2-deficient mice had a diminished ability to prevent intestinal colonization of pathogenic bacteria. In vitro, intestinal crypts isolated from terminal ilea of Nod2-deficient mice were unable to kill bacteria effectively, suggesting an important role of Nod2 signaling in crypt function. Interestingly, the expression of Nod2 is dependent on the presence of commensal bacteria, because mice re-derived into germ-free conditions expressed significantly less Nod2 in their terminal ilea, and complementation of commensal bacteria into germ-free mice induced Nod2 expression. Therefore, Nod2 and intestinal commensal bacterial flora maintain a balance by regulating each other through a feedback mechanism. Dysfunction of Nod2 results in a break-down of this homeostasis. commensal bacteria | Crohn's disease | mouse | NLR

Published

2009

8. A multiplex human syndrome implicates a key role for intestinal cell kinase in development of central nervous, skeletal, and endocrine systems

Author

Lahiry, Piya, Jian Wang, Robinson, John F., Turowec, Jacob P., Litchfield, David W., Lanktree, Matthew B., Gloor, Gregory B., Puffenberger, Erik G., Strauss, Kevin A., Martens, Mildred B., Ramsay, David A., Rupar, C. Anthony, Siu, Victoria, and Hegele, Robert A.

Subjects

Endocrine gland diseases -- Genetic aspects, Human genome -- Research, Intestines -- Genetic aspects, Intestines -- Physiological aspects, Phosphotransferases -- Research, Biological sciences

Abstract

Several studies are conducted for the characterization of endocrine-cerebro-osteodysplasia (ECO), a multiplex human syndrome. The syndrome is shown to implicate a very important role for the intestinal cell kinase in the development of the central nervous, skeletal and the endocrine systems.

Published

2009

9. Dietary modulation of GALT

Author

Sanderson, Ian R.

Subjects

Gene expression -- Control, Intestines -- Properties, Intestines -- Genetic aspects, Food/cooking/nutrition

Abstract

Changes in diet greatly affect the mucosal immune system, particularly in diseases such as Crohn's disease and necrotizing enterocolitis. This article examines the hypothesis that alterations in the luminal environment of the intestine regulate the expression of genes in the enterocyte responsible for signaling to immune cells. Genes expressed by the epithelium orchestrate leukocytes in the lamina propria. For example, chemokine expression in the mouse intestinal epithelium, through transgenic means, induced the recruitment of neutrophils and lymphocytes into intestinal tissues. Diet alters the expression of the genes responsible for signaling by a variety of pathways. The introduction of a normal diet to a weanling mouse up-regulates MHC class II expression through a particular isoform of the class II transactivator, a protein that acts in the nucleus. SCFA concentrations in the intestinal lumen vary markedly with diet. SCFAs increase IL-8 and insulin-like growth factor binding protein-2 expression by inhibiting histone deacetylase activity in the enterocyte. Down-regulation of gene expression by butyrate can act through acetylation of the inhibitory transcription factor Sp3. The review therefore describes a number of molecular pathways, explaining how changes in diet may alter leukocyte recruitment by regulating enterocyte gene expression. Myofibroblasts enhance enterocyte chemotactic activity by cleaving inactive precursors; and myofibroblast genes also are regulated by SCFA. It is likely that other similar regulatory mechanisms remain to be discovered.

Published

2007

10. Membrane recruitment of NOD2 in intestinal epithelial cells is essential for nuclear factor-[kappa]B activation in muramyl dipeptide recognition

Author

Barnich, Nicolas, Aguirre, Jose E., Reinecker, Hans-Christian, Xavier, Ramnik, and Podolsky, Daniel K.

Subjects

Epithelium -- Research, Epithelium -- Genetic aspects, Intestines -- Research, Intestines -- Genetic aspects, Cytology -- Research, Biological sciences

Abstract

Nucleotide oligomerization domain (NOD) 2 functions as a mammalian cytosolic pathogen recognition molecule, and mutant forms have been genetically linked to Crohn's disease (CD). NOD2 associates with the caspase activation and recruitment domain of RIP-like interacting caspase-like apoptosis regulatory protein kinase (RICK)/RIP2 and activates nuclear factor (NF)-[kappa]B in epithelial cells and macrophages, whereas NOD2 mutant 3020insC, which is associated with CD, shows an impaired ability to activate NF-[kappa]B. To gain insight into the molecular mechanisms of NOD2 function, we performed a functional analysis of deletion and substitution NOD2 mutants. NOD2, but not NOD2 3020insC mutant, associated with cell surface membranes of intestinal epithelial cells. Membrane targeting and subsequent NF-[kappa]B activation are mediated by two leucine residues and a tryptophan-containing motif in the COOH-terminal domain of NOD2. The membrane targeting of NOD2 is required for NF-[kappa]B activation after the recognition of bacterial muramyl dipeptide in intestinal epithelial cells.

Published

2005

11. A study of regional gut endoderm potency by analysis of Cdx2 null mutant chimaeric mice

Author

Beck, Felix, Chawengsaksophak, Kallayanne, Luckett, Jenni, Giblett, Susan, Tucci, Joseph M., Brown, Jane, Poulsom, Richard, Jeffery, Rosemary, and Wright, Nicholas A.

Subjects

Developmental biology -- Research, Genetic recombination -- Analysis, Intestines -- Genetic aspects, Intestines -- Physiological aspects, Cloning -- Genetic aspects, Epithelium -- Genetic aspects, Epithelium -- Physiological aspects, Y chromosome -- Genetic aspects, Y chromosome -- Physiological aspects, Gene expression -- Physiological aspects, Biological sciences

Abstract

Inactivation of Cdx2 by homologous recombination results in the development of forestomach epithelium at ectopic sites in pericaecal areas of the midgut of heterozygote mice. Local factors subsequently result in the secondary induction of tissues exhibiting an orderly sequence of tissue types between the ectopic forestomach tissue and the surrounding colon. Clonal analysis of this secondarily generated tissue using Y chromosome painting in chimaeric mice indicates that once differentiated to express Cdx2, host colonic epithelium can only form small intestinal-type epithelium, while Cdx2 mutant cells give rise to a succession of gastric-type tissue but never to a small intestine morphology. Our results indicate a difference in potency between forestomach and midgut precursor endodermal cells. Keywords: Cdx2; Homeobox; Intercalation; Gut development

Published

2003

12. Phenotype variation in two-locus mouse models of Hirschsprung disease: tissue-specific interaction between Ret and Ednrb

Author

McCallion, Andrew S., Stames, Erine, Conlon, Ronald A., and Chakravarti, Aravinda

Subjects

Hirschsprung's disease -- Physiological aspects, Hirschsprung's disease -- Genetic aspects, Intestines -- Genetic aspects, Nervous system -- Research, Neural crest -- Genetic aspects, Science and technology

Abstract

Clinical expression of Hirschsprung disease (HSCR) requires the interaction of multiple susceptibility genes. Molecular genetic analyses have revealed that interactions between mutations in the genes encoding the RET receptor tyrosine kinase and the endothelin receptor type B (EDNRB) are central to the genesis of HSCR. We have established two locus noncomplementation assays in mice, using allelic series at Ednrb in the context of Ret kinase-null heterozygotes, to understand the clinical presentation, incomplete penetrance, variation in length of aganglionic segment, and sex bias observed in human HSCR patients. Titration of Ednrb in the presence of half the genetic dose of Ret determines the presentation of an enteric phenotype in these strains, revealing or abrogating a sex bias in disease expression depending on the genotype at Ednrb. RET and EDNRB signaling pathways are also critical for the normal development of other tissues, including the kidneys and neural crest-derived melanocytes. Our data demonstrate that interaction between these genes is restricted to the enteric nervous system and does not affect renal, coat color, and retinal choroid development.

Published

2003

13. The origin of mesoderm in phoronids

Author

Freeman, Gary and Martindale, Mark Q.

Subjects

Developmental biology -- Research, Mesoderm -- Genetic aspects, Neurons -- Genetic aspects, Intestines -- Genetic aspects, Biological sciences

Abstract

Descriptive studies of phoronid development have concluded that the mesoderm of these animals originates from the endoderm during gastrulation. This interpretation has been tested by labeling one blastomere of 4- through 16-cell embryos and examining the position and germ layers occupied by the labeled clones of cells in the larva. No 2 injections gave rise to identical clones of cells, suggesting that the cleavage program does not generate cells of unique identity and that cell fates are established at later developmental time points. In many cases, a relatively large sector composed of ectodermal cells was labeled. When these labeled cells were adjacent to the mouth or anus of the larva, muscle and mesenchyme cells originated from the labeled clones. Under these circumstances, nerve cells also originated from these labeled sectors. These labeling studies also showed that endodermal cells can give rise to mesodermal and neural cells. These results suggest that nerve and muscle cells are induced to form at ectodermal-endodermal boundaries from both germ layers. These marking experiments also confirmed the observation that nerve cells originate both from the apical organ and the trunk region and show for the first time that the intestine originates by ingression of posterior ectoderm. Key Words: actinotroch larva; cell labeling; origin of mesoderm; origin of neural cells; origin of intestine; interactions at germ layer boundaries.

Published

2002

14. Iron treatment downregulates DMT1 and IREG1 mRNA expression in Caco-2 cells

Author

Martini, Ligia A., Tchack, Laurie, and Wood, Richard J.

Subjects

Iron deficiency diseases -- Genetic aspects, Intestines -- Genetic aspects, Genetic research -- Analysis, Food/cooking/nutrition

Abstract

Iron deficiency is the most common nutritional disorder worldwide, whereas pathologic elevations of body iron stores can occur under certain circumstances due to genetic abnormalities or in association with other diseases. The intestine is the exclusive locus of homeostatic regulation of body iron stores, which is accomplished by changes in iron absorption efficiency by largely unknown molecular mechanisms in response to alterations in body iron stores. Recently, a number of novel genes involved in iron metabolism, such as the iron uptake transporter DMT1/DCT1/Nramp2 and the iron export transporter IREG1/ferroportin1/MTP1, have been identified, providing important insights about molecular aspects of intestinal iron absorption and its regulation. The aim of this study was to investigate the effects of iron treatment on DMT1 and IREG1 mRNA expression in Caco-2 cells, a human intestinal cell line. Exposure of the cells to iron (200 [micro]mol/L ferric nitrilotriacetic acid for 72 h) significantly decreased transferrin receptor mRNA (80%), DMT1 mRNA (57%) and IREG1 mRNA (52%). These observations are consistent with the notion of parallel regulation of these iron-responsive genes in vivo to protect the enterocyte from iron toxicity and mediate a decreased efficiency of intestinal iron absorption to prevent iron overload. J. Nutr. 132: 693-696, 2002. KEY WORDS: * iron absorption * ferroportin1 * DCT1 * Nramp2 * iron responsive protein * MTP1

Published

2002

15. Modulation of intestinal gene expression by dietary zinc status: effectiveness of cDNA arrays for expression profiling of a single nutrient deficiency

Author

Blanchard, Raymond K., Moore, J. Bernadette, Green, Calvert L., and Cousins, Robert J.

Subjects

Gene expression -- Research, Intestines -- Genetic aspects, Zinc in the body -- Evaluation, Mammals -- Health aspects, Science and technology

Abstract

Mammalian nutritional status affects the homeostatic balance of multiple physiological processes and their associated gene expression. Although DNA array analysis can monitor large numbers of genes, there are no reports of expression profiling of a micronutrient deficiency in an intact animal system. In this report, we have tested the feasibility of using cDNA arrays to compare the global changes in expression of genes of known function that occur in the early stages of rodent zinc deficiency. The gene-modulating effects of this deficiency were demonstrated by real-time quantitative PCR measurements of altered mRNA levels for metallothionein 1, zinc transporter 2, and uroguanylin, all of which have been previously documented as zinc-regulated genes. As a result of the low level of inherent noise within this model system and application of a recently reported statistical tool for statistical analysis of microarrays [Tusher, V.G., Tibshirani, R. & Chu, G. (2001) Proc. Natl. Acad. Sci. USA 98, 5116-5121], we demonstrate the ability to reproducibly identify the modest changes in mRNA abundance produced by this single micronutrient deficiency. Among the genes identified by this array profile are intestinal genes that influence signaling pathways, growth, transcription, redox, and energy utilization. Additionally, the influence of dietary zinc supply on the expression of some of these genes was confirmed by real-time quantitative PCR. Overall, these data support the effectiveness of cDNA array expression profiling to investigate the pleiotropic effects of specific nutrients and may provide an approach to establishing markers for assessment of nutritional status. nutrition | microarray | micronutrient

Published

2001

16. Coordination of ges-1 expression between the Caenorhabditis pharynx and intestine

Author

Marshall, Sean D.G. and McGhee, James D.

Subjects

Developmental biology -- Physiological aspects, Embryology, Experimental -- Reports, Caenorhabditis elegans -- Genetic aspects, Pharynx -- Genetic aspects, Intestines -- Genetic aspects, Biological sciences

Abstract

We have previously shown that the Caenorhabditis elegans gut-specific esterase gene (Ce-ges-1) has the unusual ability to be expressed in different modules of the embryonic digestive tract (anterior pharynx, posterior pharynx, and rectum) depending on sequence elements within the Ce-ges-1 promoter. In the present paper, we analyze the expression of the ges-1 homolog (Cb-ges-1) from the related nematode Caenorhabditis briggsae and show that Cb-ges-1 also has the ability to switch expression between gut and pharynx + rectum. The control of this expression switch centres on a tandem pair of WGATAR sites in the Cb-ges-1 5'-flanking region, just as it does in Ce-ges-1. We use sequence alignments and subsequent deletions to identify a region at the 3'-end of both Ce-ges-1 and Ce-ges-1 that acts as the ges-1 cryptic pharynx enhancer whose activity is revealed by removal of the 5' WGATAR sites. This region contains a conserved binding site for PHA-4 (the C. elegans ortholog of forkhead/HNF3 [alpha], [beta], [gamma] factors), which is expressed in all cells of the developing pharynx and a subset of cells of the developing rectum. We propose a model in which the normal expression of ges-1 is controlled by the gut-specific GATA factor ELT-2. We propose that, in the pharynx (and rectum), PHA-4 is normally bound to the ges-1 3'-enhancer sequence but that the activation function of PHA-4 is kept repressed by a (presently unknown) factor binding in the vicinity of the 5' WGATAR sites. We suggest that this control circuitry is maintained in Caenorhabditis because pharyngeal expression of ges-1 is advantageous only under certain developmental or environmental conditions. Key Words: Caenorhabditis elegans; Caenorhabditis briggsae; ges-1; gene expression; intestine; pharynx; elt-2; pha-4.

Published

2001

17. Differential activities of the RET tyrosine kinase receptor isoforms during mammalian embryogenesis

Author

De Graaff, Esther, Srinivas, Shankar, Kilkenny, Carol, D'Agati, Vivette, Mankoo, Baljinder S., Costantini, Frank, and Pachnis, Vassilis

Subjects

Cytochemistry -- Research, Mammals -- Reproduction, Protein tyrosine kinase -- Physiological aspects, Embryology, Experimental -- Research, Kidneys -- Genetic aspects, Nerves -- Genetic aspects, Intestines -- Genetic aspects, Hirschsprung's disease -- Genetic aspects, Cell differentiation -- Research, Biological sciences

Abstract

The RET tyrosine kinase receptor isoforms and differential activities in mammalian embryogenesis are discussed. Targeted mutagenesis was used to generate mice that express RET9 or RET51. Some RET9 transgenes can rescue kidney agenesis in RET-deficient mice or can cause kidney hypodysplasia in wild-type animals. Mice without RET9 lack enteric ganglia from the colon. Human mutations of c-RET bring on Hirschsprung's disease.

Published

2001

18. Effects of Escherichia coli Nissle 1917 and Ciprofloxacin on small intestinal epithelial cell mRNA expression in the neonatal piglet model of human rotavirus infection

Author

Paim, Francine C., Langel, Stephanie N., Fischer, David D., Kandasamy, Sukumar, Shao, Lulu, Alhamo, Moyasar A., Huang, Huang-Chi, Kumar, Anand, Rajashekara, Gireesh, Saif, Linda J., and Vlasova, Anastasia N.

Subjects

Genotypes -- Properties, Host-bacteria relationships, Intestines -- Genetic aspects, Endothelium -- Genetic aspects, Gene expression -- Observations, Messenger RNA -- Properties, Escherichia coli -- Genetic aspects, Health

Abstract

We evaluated the effects of the probiotic Escherichia coli Nissle 1917 (EcN) and the antibiotic Ciprofloxacin (Cipro) on mRNA expression of intestinal epithelial cells (IEC) in gnotobiotic (Gn) piglets colonized with a defined commensal microflora (DMF) and inoculated with human rotavirus (HRV) that infects IECs. We analyzed mRNA levels of IEC genes for enteroendocrine cells [chromogranin A (CgA)], goblet cells [mucin 2 (MUC2)], transient amplifying progenitor cell [proliferating cell nuclear antigen (PCNA)], intestinal epithelial stem cell (SOX9) and enterocytes (villin). Cipro treatment enhanced HRV diarrhea and decreased the mRNA levels of MUC2 and villin but increased PCNA. These results suggest that Cipro alters the epithelial barrier, potentially decreasing the numbers of mature enterocytes (villin) and goblet cells secreting protective mucin (MUC2). These alterations may induce increased IEC proliferation (PCNA expression) to restore the integrity of the epithelial layer. Coincidental with decreased diarrhea severity in EcN treated groups, the expression of CgA and villin was increased, while SOX9 expression was decreased representing higher epithelial integrity indicative of inhibition of cellular proliferation. Thus, EcN protects the intestinal epithelium from damage by increasing the gene expression of enterocytes and enteroendocrine cells, maintaining the absorptive function and, consequently, decreasing the severity of diarrhea in HRV infection. Keywords: Probiotic, Antibiotic, Commensal microflora, Gnotobiotic piglets, Human rotavirus, Intestinal epithelial cell-specific genes, Author(s): Francine C. Paim[sup.1] , Stephanie N. Langel[sup.1] , David D. Fischer[sup.1] , Sukumar Kandasamy[sup.1] , Lulu Shao[sup.1,2] , Moyasar A. Alhamo[sup.1] , Huang-Chi Huang[sup.1] , Anand Kumar[sup.1,3] , Gireesh [...]

Published

2016

19. The GATA-factor elt-2 is essential for formation of the Caenorhabditis elegans intestine

Author

Fukushige, Tetsunari, Hawkins, Mark G., and McGhee, James D.

Subjects

Caenorhabditis elegans -- Research, Intestines -- Genetic aspects, Gene expression -- Research, Genetic code -- Identification and classification, Biological sciences

Abstract

The Caenorhabditis elegans elt-2 gene encodes a single-finger GATA factor, previously cloned by virtue of its binding to a tandem pair of GATA sites that control the gut-specific ges-1 esterase gene. In the present paper, we show that elt-2 expression is completely gut specific, beginning when the embryonic gut has only two cells (one cell cycle prior to ges-1 expression) and continuing in every cell of the gut throughout the life of the worm. When elt-2 is expressed ectopically using a transgenic heat-shock construct, the endogenous ges-1 gene is now expressed in most if not all cells of the embryo; several other gut markers (including a transgenic elt-2-promoter::1acZ reporter construct designed to test for elt-2 autoregulation) are also expressed ectopically in the same experiment. These effects are specific in that two other C. elegans GATA factors (elt-1 and elt-3) do not cause ectopic gut gene expression. An imprecise transposon excision was identified that removes the entire elt-2 coding region. Homozygous elt-2 null mutants die at the L1 larval stage with an apparent malformation or degeneration of gut cells. Although the loss of elt-2 function has major consequences for later gut morphogenesis and function, mutant embryos still express ges-1. We suggest that elt-2 is part of a redundant network of genes that controls embryonic gut development; other factors may be able to compensate for elt-2 loss in the earlier stages of gut development but not in later stages. We discuss whether elements of this regulatory network may be conserved in all metazoa. Key Words: C. elegans; GATA factor; elt-2; gut development.

Published

1998

20. A physicians' wish list for the clinical application of intestinal metagenomics

Author

Klymiuk, Ingeborg, Hogenauer, Christoph, Halwachs, Bettina, Thallinger, Gerhard G., Fricke, W. Florian, and Steininger, Christoph

Subjects

Genomics -- Research, Genetic research, Intestines -- Genetic aspects, Microbial colonies -- Genetic aspects, Microbiological research, Biological sciences

Abstract

Introduction The intestine is one of the most diverse and complex bacterial habitats of the human body, harboring ~1,000 bacterial phylotypes [1]. Recent studies have associated the human intestinal microbiome [...]

Published

2014

21. Balancing import and export in development

Author

Affolter, Markus, Marty, Thomas, and Bigano, M. Alessandra

Subjects

Genetic disorders -- Research, Developmental biology -- Research, Neural tube -- Genetic aspects, Intestines -- Genetic aspects, Genetic transcription -- Regulation, Biological sciences

Abstract

Characterization of the homeoprotein-containing regulatory complexes, when it comes, will be helpful to elucidation of molecular mechanisms that underlie the control of morphological diversity by Hox genes in animal development. Effects of hexapeptide mutations in vivo on targets that are well defined will make the investigation of the HOX proteins possible in the absence of cooperativity. Mutations in homeodomains that get rid of DNA binding may give some insight into composition of the complex on in vivo targets.

Published

1999

22. The intestinal stem cell

Author

Barker, Nick, Wetering, Marc van de, and Clevers, Hans

Subjects

Intestines -- Genetic aspects, Epithelium -- Research, Stem cells -- Research, Cell proliferation -- Research, Biological sciences

Published

2008

23. Intestinal integrity and Akkermansia muciniphila, a mucin-degrading member of the intestinal microbiota present in infants, adults, and the elderly

Author

Collado, M. Carmen, Derrien, Muriel, Isolauri, Erika, de Vos, Willem M., and Salminen, Seppo

Subjects

Mucins -- Chemical properties, Polymerase chain reaction -- Usage, Intestines -- Microbiology, Intestines -- Genetic aspects, Biological sciences

Abstract

The quantification of the mucin-degrading bacterium Akkermansia muciniphila found in the human intestinal tract is demonstrated. The bacterium colonizes in early life, develops in a year in adults and decreases in the elderly.

Published

2007

24. Using a Novel Gut Culture System to Analyze the Influence of Known and Novel Genes on Intestinal Epithelial Differentiation

Author

Abud, H. E., Johnstone, C. N., Watson, N., Tebbutt, N. C., Ernst, M., and Heath, J. K.

Subjects

Intestines -- Genetic aspects, Epithelium -- Analysis, Developmental genetics -- Research, Biological sciences

Abstract

We aim to study the development of endoderm and the differentiation of the intestinal epithelium in mice, using embryonic gut culture, ES cell differentiation, and mouse models. We have established an innovative mouse embryonic gut culture system (caternary culture) in our laboratory that maintains the three-dimensional architecture of the gut. This provides an opportunity to directly study the function of genes in a system that closely mimics the development and differentiation of the gut in vivo. The development of the epithelial cell layer in caternary cultures has been studied in detail using light and electron microscopy and immunohistochemistry for molecular markers of gut development. We have also demonstrated that plasmids encoding genes can be introduced into the epithelial cell layer using a low-voltage electroporation technique. The effects of expressing mutant versions of components of the APC, Ras, and TGF[Beta] signaling pathways on intestinal cell biology will be examined using this system. Along side this work, we also aim to identify novel genes that can promote intestinal differentiation using a unique screening strategy in embryonic stem (ES) cells. This is based on a unique ES cell line generated in our laboratory that contains a LacZ marker gene under the control of the A33 promoter (a definitive marker of intestinal epithelium). The ultimate objective of this project is to screen an expression library for genes that can promote intestinal differentiation.

Published

2001

25. Fructose-1,6-biphosphate in rat intestinal preconditioning: involvement of nitric oxide

Author

Sola, A, Rosello-Catafau, J, Gelpi, E, and Hotter, G

Subjects

Intestines -- Genetic aspects, Fructose -- Genetic aspects, Reperfusion injury -- Genetic aspects, Nitric oxide -- Genetic aspects, Health, Genetic aspects

Abstract

Abstract Background and aims--Inhibition of glyceraldehyde-3-phosphate dehydrogenase (GAPDH) by nitric oxide (NO) in intestinal preconditioning could modify the rate of formation of glycolytic intermediates. Fructose-1,6-biphosphate (F16BP) is a glycolytic intermediate [...]

Published

2001

26. Regulation of Intestinal Apolipoprotein B mRNA Editing Levels by a Zinc-Deficient Diet and cDNA Cloning of Editing Protein in Hamsters

Author

Reaves, Scott K., Wu, John Y. J., Wu, Yan, Fanzo, Jessica C., Wang, Yi Ran, Lei, Polin P., and Lei, Kai Y.

Subjects

Hamsters as laboratory animals -- Usage, Zinc in the body -- Health aspects, Low density lipoproteins -- Physiological aspects, Intestines -- Genetic aspects, Gene expression -- Measurement, Food/cooking/nutrition

Abstract

This study was conducted to investigate the influence of dietary zinc on intestinal apoB mRNA editing in hamsters. Apolipoprotein B-48 (apoB-48) is synthesized from the same gene as apoB-100 by a post-transcriptional, site-specific cytidine deamination, a process known as apoB mRNA editing, A cDNA encoding the hamster apoB mRNA editing enzyme was obtained by reverse transcriptase-polymerase chain reaction (RT-PCR) and the deduced amino acid sequence was found to possess high amino acid sequence identity to apoB mRNA editing enzymes from several other species. Editing activity was detected in the small intestine and colon but, like humans, none was detected in the liver. Analysis by RT-PCR indicated that the small intestine possessed the highest expression of editing enzyme mRNA abundance, whereas both liver and small intestine expressed relatively high levels of apoB mRNA. The influence of dietary zinc on intestinal apoB mRNA editing levels was examined in Golden Syrian hamsters (7 wk old) assigned to one of the following three dietary treatments: Zn-adequate (ZA, 30 mg Zn/kg diet), Zn-deficient (ZD, [is less than] 0.5 mg Zn/kg diet), or Zn-replenished (ZDA, ZD hamsters receiving ZA diet for last 2 d) for 7 wk. Hamsters consuming the ZD diet had modestly but significantly lower intestinal editing activity than ZA hamsters. Intestinal editing activity in the ZDA group, was not different from that of ZA hamsters. Data derived from these studies contribute to the understanding of lipoprotein metabolism in hamsters, a suitable model for the study of atherosclerosis. J. Nutr. 130: 2166-2173, 2000. KEY WORDS: * hamsters * dietary zinc * cardiovascular disease * cholesterol * low density lipoprotein

Published

2000