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1. Activation of μ opioid receptors modulates inflammation in acute experimental colitis

Author

Anselmi, L, Huynh, J, Duraffourd, C, Jaramillo, I, Vegezzi, G, Saccani, F, Boschetti, E, Brecha, NC, De Giorgio, R, and Sternini, C

Subjects
Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Digestive Diseases, Genetics, Animals, Colitis, Cytokines, Dextran Sulfate, Disease Models, Animal, Enkephalin, Ala(2)-MePhe(4)-Gly(5)-, Inflammation, Mice, Mice, Inbred C57BL, Receptors, Opioid, mu, antiapoptotic factor, cytokines, inflammatory indexes, transcriptional nuclear factor-kB, Antiapoptotic factor, Inflammatory indexes, Transcriptional nuclear factor-kB, Clinical Sciences, Neurosciences, Medical Physiology, Gastroenterology & Hepatology, Clinical sciences, Medical physiology
Abstract

Backgroundμ opioid receptors (μORs) are expressed by neurons and inflammatory cells, and mediate immune response. We tested whether activation of peripheral μORs ameliorates the acute and delayed phase of colitis.MethodsC57BL/6J mice were treated with 3% dextran sodium sulfate (DSS) in water, 5 days with or without the peripherally acting μOR agonist, [D-Ala2, N-Me-Phe4, Gly5-ol]-Enkephalin (DAMGO) or with DAMGO+μOR antagonist at day 2-5, then euthanized. Other mice received DSS followed by water for 4 weeks, or DSS with DAMGO starting at day 2 of DSS for 2 or 3 weeks followed by water, then euthanized at 4 weeks. Disease activity index (DAI), histological damage, and myeloperoxidase assay (MPO), as index of neutrophil infiltration, were evaluated. Cytokines and μOR mRNAs were measured with RT-PCR, and nuclear factor-kB (NF-kB), the antiapoptotic factor Bcl-xL, and caspase 3 and 7 with Western blot.Key resultsDSS induced acute colitis with elevated DAI, tissue damage, apoptosis and increased MPO, cytokines, μOR mRNA, and NF-kB. DAMGO significantly reduced DAI, inflammatory indexes, cytokines, caspases, and NF-kB, and upregulated Bcl-xL, effects prevented by μOR antagonist. In DSS mice plus 4 weeks of water, DAI, NF-kB, and μOR were normal, whereas MPO, histological damage, and cytokines were still elevated; DAMGO did not reduce inflammation, and did not upregulate Bcl-xL.Conclusions & inferencesμOR activation ameliorated the acute but not the delayed phase of DSS colitis by reducing cytokines, likely through activation of the antiapoptotic factor, Bcl-xL, and suppression of NF-kB, a potentiator of inflammation.

Published
2015

11. Action of sensory neurons in an experimental rat colitis model of injury and repair

Author

Reinshagen, M., Patel, A., Sottili, M., French, S., Sternini, C., and Eysselein, V.E.

Subjects
Neurons -- Physiological aspects, Colitis -- Physiological aspects, Inflammation -- Mediators, Biological sciences
Abstract

Sensory nerves protect the intestinal mucosa from injury and decrease inflammation in the early phases of colitis in rat. The nerves do not increase mucosal repair. Sensory nerves have no effect on inflammation during the later stages of chronic inflammation, which increases within 3-7 days of colitis induction. Sensory nerves have no significant influence on mucosal lesions, as mucosal injury is unaffected by denervation in the later stage of colitis.

Published
1996

16. Distribution and abundance of neutral endopeptidase (EC 3.424.11) in the alimentary tract of the rat

Author

Bunnett, N.W., Wu, V., Sternini, C., Klinger, J., Shimomaya, E., Payan, D., Kobayashi, R., and Walsh, J.H.

Subjects
Proteases -- Research, Alimentary canal -- Physiological aspects, Neuropeptides -- Research, Biological sciences
Abstract

Immunohistochemistry and in situ hybridization histochemistry are used to analyze how cells of neutral endopeptidase (NEP) are scattered in the alimentary tract of the rat. Western blotting, Northern blotting, and a ribonuclease insulation assay are employed to determine the comparatively excessive amounts of NEP protein and mRNA. A specific enzyme assay is used to quantify the enzymatic activity of NEP in various tissues. The branch border of the small intestine is formed by epithelial cells, which yield NEP in large amounts. The smooth muscle cells of the stomach, small intestine and colon and unknown cells in the gastric and colonic muscosa yield NEP in small amounts.

Published
1993

17. Molecular differences underlying chronic constipation vs constipated Parkinson disease patients

Author

Giancola, F., Latorre, R., Bianco, F., Repossi, R., Torresan, F., Ioannou, A., Guarino, M., Barbara, G., Chiocchetti, R., Clavenzani, P., Maurizio Mazzoni, Stanghellini, V., Cortelli, P., Sternini, C., Giorgio, R., Giancola, Fiorella, Latorre, Rocco, Bianco, Francesca, Repossi, R., Torresan, F., Ioannou, A., Guarino, M., Barbara, Giovanni, Chiocchetti, Roberto, Clavenzani, Paolo, Mazzoni, Maurizio, Stanghellini, Vincenzo, Cortelli, P., Sternini, C., and De Giorgio, Roberto

Subjects
Parkinson disease, chronic constipation, Parkinson disease, chronic constipation, NO
Published
2015

19. CLINICAL AND NEUROCHEMICAL FEATURES OF CHRONIC CONSTIPATION IN PATIENTS WITH PARKINSON DISEASE

Author

GIANCOLA, FIORELLA, LATORRE, ROCCO, SORTENI, CATERINA, BARBARA, GIOVANNI, CREMON, CESARE, CHIOCCHETTI, ROBERTO, CLAVENZANI, PAOLO, STANGHELLINI, VINCENZO, DE GIORGIO, ROBERTO, Torresan, F., Ioannou, A., Guarino, M., Vallorani, C., Sternini, C., Giancola, F., Latorre, R., Sorteni, C., Torresan, F., Ioannou, A., Guarino, M., Barbara, G., Cremon, C., Chiocchetti, R., Vallorani, C., Clavenzani, P., Stanghellini, V., Sternini, C., and De Giorgio, R.

Subjects
CHRONIC CONSTIPATION, PARKINSON DISEASE
Published
2014

20. Expression and role of 5-HT7 receptors in modulating peristalsis and accommodation in the guinea-pig ileum

Author

CERVIO E., VICINI R., DELLABIANCA A., STERNINI C., TONINI M., DE PONTI, FABRIZIO, DE GIORGIO, ROBERTO, BARBARA, GIOVANNI, STANGHELLINI, VINCENZO, Cervio E., Vicini R., De Ponti F., De Giorgio R., Barbara G., Stanghellini V., Della Bianca A., Sternini C., Tonini M., CERVIO E., VICINI R., DE PONTI F., DE GIORGIO R., BARBARA G., STANGHELLINI V., DELLABIANCA A., STERNINI C., and TONINI M.

Published
2005

21. Regulation of taste signaling molecules by high protein diet in the pig pylorus

Author

VALLORANI, CLAUDIA, LATORRE, ROCCO, MAZZONI, MAURIZIO, BACCI, MARIA LAURA, FORNI, MONICA, GIANCOLA, FIORELLA, FALCONI, MIRELLA, DE GIORGIO, ROBERTO, CLAVENZANI, PAOLO, Sternini C, s.n., Vallorani C, Latorre R, Mazzoni M, Bacci ML, Forni M, Giancola F, Falconi M, De Giorgio R, Sternini C, and Clavenzani P.

Subjects
High Protein Diet, SWINE, Taste receptor, Pyloru
Abstract

REGULATION OF TASTE SIGNALING MOLECULES BY HIGH PROTEIN DIET IN THE PIG PYLORUS Vallorani C.*[1], Latorre R.[1], Mazzoni M.[1], Bacci M.L.[1], Monica F.[1], Giancola F.[1], Falconi M.[2], De Giorgio R.[3], Sternini C.[4], Clavenzani P.[1] [1]Department of Veterinary Medical Science, University of Bologna. ~ Bologna, [2]Department of Biomedical and Neuromotorial Sciences, University of Bologna ~ Bologna, [3]Department of Medical and Surgical Sciences, University of Bologna ~ Bologna, [4]CURE/DDRC, Division of Digestive Diseases, Department of Medicine, UCLA, Los Angeles, CA, USA ~ Los Angeles Taste receptors (TRs) and their signaling molecules are widely expressed in extra‐oral sites, including the gastrointestinal (GI) tract mucosa(1). Fasting and refeeding have been shown to modify the expression of α‐ transducin / α‐gustducin in enteroendocrine cells of the pig GI tract(2), however, the effects of individual nutrients on TR‐related molecules remain unknown. The gustatory system is fundamental for detecting dietary nutrients and evoking appropriate functional responses leading to digestion and absorption. Thus, the aim of this study was to test whether a short‐ and long‐term high protein diet (3 and 30 days, respectively) affected the enteroendocrine profile of the TRs signalling molecules α‐transducin / α‐ gustducin expressing cells in the pig gastric mucosa. Twelve hybrid (LW x D) female pigs (weighing 30‐40 Kg) were subdivided in three experimental groups (n= 4 each group): A) fed standard diet (controls, CTR, 14,5% protein); B) fed high protein diet for 3 days (HP‐3, 33% protein); and C) fed high protein diet for 30 days (HP‐30, 33% protein). The protein used to supplement the diet was fish and potatoes protein. Mucosal samples from pylorus were harvested, fixed and processed for single and double labelling immunofluorescence with a mixture of the following primary antisera to Gα‐transducin (Gαtran), Gα‐gustducin (Gαgust) and 5‐hydroxytryptamine (5‐HT). In the pyloric mucosa, the average number of Gαtran immunoreactive (‐IR) cells were 111.5 ± 26.2 (CTR), 148.8 ± 13.2 (HP3), and 218.3 ± 28.8 (HP30) (CTR vs HP‐3 P< 0.04; CTR vs HP‐30 P< 0.002; HP‐3 vs HP‐30 P< 0.005), while Gαgust‐IR cells were 138.8 ± 45.1 8 (CTR), 177.3 ± 14 (HP3), 211.5 ± 29.1 (HP30) (CTR vs HP‐30 P

Published
2013

22. ALPHA‐TRANSDUCIN EXPRESSION IN THE GASTROINTESTINAL TRACT OF THE EUROPEAN SEA BASS (DICENTRARCHUS LABRAX)

Author

LATORRE, ROCCO, MAZZONI, MAURIZIO, DE GIORGIO, ROBERTO, GATTA, PIER PAOLO, BONALDO, ALESSIO, CHIOCCHETTI, ROBERTO, CLAVENZANI, PAOLO, Sternini C., Latorre R., Mazzoni M., De Giorgio R., Sternini C., Gatta P.P., Bonaldo A., Chiocchetti R., and Clavenzani P.

Subjects
GASTROINTESTINAL TRACT, ALPHA TRANSDUCIN, TASTE RECEPTORS, DICENTRARCHUS LABRAX
Abstract

The gustatory system plays the critical function of distinguishing between nutrients and non‐nutrient, potentially dangerous substances (1) allowing adaptation to different habitats (2). Different tastes are detected by G protein couple receptors and their signalling molecules,including the heterotrimeric G proteins,α‐transducin (Gαtran)and α‐gustducin(Gαgust) (3,4). Taste‐related molecules have been discovered in the gastrointestinal tract of a variety of species from fish to humans. In this study we examined the distribution and peptide content of cells expressing Gαtran‐immunoreactivity in the gastrointestinal(GI)mucosa of the sea bass. Adult European sea bass(Dicentrarchus labrax)were sampled from different tanks and euthanized by an overdose of anaesthetic. The stomach,pyloric caeca and intestine were harvested;the intestine was divided into three regions: cranial, middle and caudal. Tissue sections were processed for immunofluorescence with the following primary antisera: Gαtran, Gαgust, ghrelin(GHR), 5‐hydroxytryptamine (5‐HT), obestatin (OB), somatostatin (SOM), gastrin/cholecystokinin (GAS/CCK), glucagon‐like peptide‐1 (GLP‐1), calcitonin gene‐related peptide (CGRP) and substance P(SP). Each antibody was either used alone for single labelling or in combination with others for double labelling. Gαtran immunoreactivity was observed throughout the sea bass GI tract, but was more abundant in the stomach compared to the intestine with decreasing density of cells from the cranial to the caudal regions. Specificity of Gαtran and Gαgust immunostaining was established by Western blot analysis, which showed immunopositive bands at the expected molecular weight of ~45 and ~40 kDa, respectively, in sea bass gut tissue as well as in positive tissue (e.g. brain and eye). Staining specificity was also demonstrated by immunoblocking with the homologous peptides. Colocalization of Gαtran and Gαgust immunoreactivity was visualized in some cells in the stomach. A subpopulation of Gαtran immunoreacitve cells in the stomach also contained GHR, OB or 5‐HT immunoreactivity. Colocalization of Gαtran immumoreactivity with SOM, GAS/CCK, GLP‐1, SP, or CGRP immunistaining was not observed in any GI tract regions. Our data provide evidence that Gαtran and Gαgust are involved in chemosensory transmission in the sea bass GI enteroendocrine system. It is likely that nutrients activate taste receptors and their signalling molecules to induce the release of peptides from enteroendocrine cells, which in turn activate other cells types directly or via neural reflexes thus initiating a variety of physiological responses controlling GI functions and caloric intake. 1 Sternini C. Am J Physiol Gastrointest Liver Physiol, 2007, 292:G457‐G461. 2 Barreiro‐Iglesias et. all, Brain Behav Evol 2010,75:241‐250. 3 Mazzoni et. all, J Cell Mol Med 2013, Apr;17(4):466‐74. 4 Oike H et. all, J Neurosci, 2007, 27:5584‐5592.

Published
2013

23. Fasting/refeeding-mediated changes of α–transducin immunoreactivity in the pig GI tract

Author

MAZZONI, MAURIZIO, DE GIORGIO, ROBERTO, BOSI, PAOLO, TREVISI, PAOLO, LALATTA COSTERBOSA, GIOVANNA, CHIOCCHETTI, ROBERTO, BARBARA, GIOVANNI, STANGHELLINI, VINCENZO, CLAVENZANI, PAOLO, LATORRE R., BORTOLAMI R., TONINI M., ROZENGURT E., STERNINI C., MAZZONI M., DE GIORGIO R., BOSI P., TREVISI P., LATORRE R., LALATTA COSTERBOSA G., CHIOCCHETTI R., BARBARA G., STANGHELLINI V., BORTOLAMI R., TONINI M., ROZENGURT E., STERNINI C., and CLAVENZANI P.

Published
2009

24. Modifications to α-transducin and neuropeptide immunoreactivities evoked by feeding in the GI tract

Author

CLAVENZANI, PAOLO, MAZZONI, MAURIZIO, BOSI, PAOLO, TREVISI, PAOLO, LATORRE, ROCCO, LALATTA COSTERBOSA, GIOVANNA, CHIOCCHETTI, ROBERTO, BARBARA, GIOVANNI, STANGHELLINI, VINCENZO, CORINALDESI, ROBERTO, BORTOLAMI, RUGGERO, GORI, ALESSANDRA, DE GIORGIO, ROBERTO, TONINI M., STERNINI C., CLAVENZANI P., MAZZONI M., BOSI P., TREVISI P., LATORRE R., LALATTA COSTERBOSA G., CHIOCCHETTI R., BARBARA G., STANGHELLINI V., CORINALDESI R., BORTOLAMI R., TONINI M., GORI A., STERNINI C., and DE GIORGIO R.

Subjects
GI tract, genetic structures, sense organs, α-transducin, neuropeptide
Abstract

Taste receptors (TR1s, TR2s) for sweet and bitter along with related G-proteins (α-transducin and α-gustducin) have been localized in the GI tract mucosa of several mammals. Taste signalling molecules are now conceived to be part of a wide chemosensing system contributing to sense luminal contents. In the pig model (resembling the human gut) we established whether feeding changes, i.e. fasting and re-feeding, wereable to affect: 1) the expression of α-transducin throughout the GI tract; 2) neuropeptide coding of the cells expressing α-transducin; and 3) the spatial relationship between α-transducin cells and nerves supplying the gut. Pig stomach-to-rectum specimens (n= 12; 45 days of age), subdivided in 3 groups, i.e. control (C), fasted for 24h (F) and re-fed (R), were fixed in 4%-paraformaldehyde, embedded either in paraffin and processed for single and double labelling immunofluorescence with antibodies to: α-transducin, chromogranin-A (CgA), gastrin/cholecystokinin (Gas/CCK), somatostatin (SOM) and PGP9.5. The highest density of α-transducin-immunoreactive (IR) cells has been shown in the pylorus (C: 191±22, F: 99±28 and R: 112±51) and in the cardial mucosa (C: 79±46, F: 29±13 and R: 57±10), whereas in the intestine the highest α-transducin cell density was observed in the duodenum of C (54±22) vs. F and R (41±20,14±6, respectively). The density of α-transducin-IR cells decreased along the large intestine. The percentage of α-transducin/CgA-IR cells was reduced in the GI tract of F and R vs. C. In the jejunum,α -transducin/CCK cells decreased in F and R vs. C. Gas/α-transducin and SOM/α -transducin colocalizations have never been detected. PGP9.5 varicose nerve fibers, running either singly or in small fascicles, throughout the lamina propria of the small bowe l mucosa were seen in close spatial relationship with α-transducin cells. In conclusion, changes to α-transducin expression in neuropeptide-containing cells following F and R provide a basis to the concept that these cells participate to luminal chemosensing in the GI tract. The identification of chemosensory molecule plasticity in response to fasting and nutrients in specialized GI cells could open novel therapeutic strategies in feeding behaviour or metabolic disorders.

Published
2009

25. Changes of α-transducin immunoreactivity (IR) in the pig gastrointestinal (GI) mucosa evoked by fasting/refeeding

Author

MAZZONI, MAURIZIO, DE GIORGIO, ROBERTO, BOSI, PAOLO, TREVISI, PAOLO, LALATTA COSTERBOSA, GIOVANNA, CHIOCCHETTI, ROBERTO, BARBARA, GIOVANNI, STANGHELLINI, VINCENZO, CLAVENZANI, PAOLO, LATORRE R., BORTOLAMI R., TONINI M., ROZENGURT E., STERNINI C., MAZZONI M., DE GIORGIO R., BOSI P., TREVISI P., LATORRE R., LALATTA COSTERBOSA G., CHIOCCHETTI R., BARBARA G., STANGHELLINI V., BORTOLAMI R., TONINI M., ROZENGURT E., STERNINI C., and CLAVENZANI P.

Published
2009

26. Espressione dell’ α-transducina, una molecola della chemorecezione, in cellule endocrine e non endocrine del tratto gastrointestinale di suino

Author

CLAVENZANI, PAOLO, DE GIORGIO, ROBERTO, MAZZONI, MAURIZIO, CHIOCCHETTI, ROBERTO, BARBARA, GIOVANNI, LALATTA COSTERBOSA, GIOVANNA, RUSSO D., STERNINI C., CLAVENZANI P., DE GIORGIO R., MAZZONI M., CHIOCCHETTI R., BARBARA G., LALATTA COSTERBOSA G., RUSSO D., and STERNINI C.

Subjects
genetic structures, sense organs
Abstract

SUMMARY - Transcripts for sweet and bitter taste receptors and the gustatory G proteins, alpha-gustducin and alpha-transducin, are expressed by the oral cavity and the gastrointestinal (GI) mucosa. This study evaluated: 1) distribution of alpha-transducin in the pig GI tract; 2) type of cells expressing alpha-transducin (chromogranin-A, gastrin/cholecystokinin, somatostatin, villin) 3) relationship between alpha-transducin cells and enteric fibres. The presence of alpha-transducin-IR in enteroendocrine cells supports an active chemosensory machinery in the GI mucosa and that taste signalling molecules contribute to luminal chemosensing. These mechanisms may occur via neuro-endocrine cross-talk activating digestive or protective reflex pathways (e.g. vomiting or food aversion).

Published
2008

27. Transducin in endocrine cells of the human and pig gastrointestinal tract

Author

MAZZONI, MAURIZIO, LALATTA COSTERBOSA, GIOVANNA, CHIOCCHETTI, ROBERTO, GIONCHETTI, PAOLO, RIZZELLO, FERNANDO, BARBARA, GIOVANNI, CORINALDESI, ROBERTO, STANGHELLINI, VINCENZO, CAMPIERI, MASSIMO, DE GIORGIO, ROBERTO, CLAVENZANI, PAOLO, STERNINI C., MAZZONI M., LALATTA COSTERBOSA G., CHIOCCHETTI R., GIONCHETTI P., RIZZELLO F., BARBARA G., CORINALDESI R., STANGHELLINI V., CAMPIERI M., DE GIORGIO R., STERNINI C., and CLAVENZANI P.

Published
2007

30. Downregulation of neuronal vasoactive intestinal polypeptide in Parkinson's disease and chronic constipation

Author

Giancola, F., primary, Torresan, F., additional, Repossi, R., additional, Bianco, F., additional, Latorre, R., additional, Ioannou, A., additional, Guarino, M., additional, Volta, U., additional, Clavenzani, P., additional, Mazzoni, M., additional, Chiocchetti, R., additional, Bazzoli, F., additional, Travagli, R. A., additional, Sternini, C., additional, and De Giorgio, R., additional

Published
2016
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36. Neurology and neuropathology of the pancreatic innervation

Author

Salvioli, B., Bovara, M., Barbara, G., Ponti, F., Stanghellini, V., Tonini, M., Guerrini, S., Cesare Cremon, Degli Esposti, M., Koumandou, M., Corinaldesi, R., Sternini, C., Giorgio, R., Salvioli B., Bovara M., Barbara G., De Ponti F., Stanghellini V., Tonini M., Guerrini S., Cremon C., Degli Esposti M., Koumandou M., Corinaldesi R., Sternini C., and De Giorgio R.

Subjects
Neurons, Neuropeptide, Autonomic Pathway, Animals, Humans, Neurotransmitter, Peripheral Nerves, Pancreatic Disease, Pancreas, Enteric Nervous System
Abstract

No abstract available

Published
2002

38. Downregulation of neuronal vasoactive intestinal polypeptide in Parkinson's disease and chronic constipation.

Author

Giancola, F., Torresan, F., Repossi, R., Bianco, F., Latorre, R., Ioannou, A., Guarino, M., Volta, U., Clavenzani, P., Mazzoni, M., Chiocchetti, R., Bazzoli, F., Travagli, R. A., Sternini, C., and De Giorgio, R.

Subjects
POLYPEPTIDES, PARKINSON'S disease, CONSTIPATION, DOWNREGULATION, ESOPHAGEAL motility disorders, MESSENGER RNA
Abstract

Background Chronic constipation ( CC) is a common and severe gastrointestinal complaint in Parkinson's disease ( PD), but its pathogenesis remains poorly understood. This study evaluated functionally distinct submucosal neurons in relation to colonic motility and anorectal function in PD patients with constipation ( PD/ CC) vs both CC and controls. Methods Twenty-nine PD/ CC and 10 Rome III-defined CC patients were enrolled. Twenty asymptomatic age-sex matched subjects served as controls. Colonic transit time measurement and conventional anorectal manometry were evaluated in PD/ CC and CC patients. Colonoscopy was performed in all three groups. Colonic submucosal whole mounts from PD/ CC, CC, and controls were processed for immunohistochemistry with antibodies for vasoactive intestinal polypeptide ( VIP) and peripheral choline acetyltransferase, markers for functionally distinct submucosal neurons. The mRNA expression of VIP and its receptors were also assessed. Key Results Four subgroups of PD/ CC patients were identified: delayed colonic transit plus altered anorectal manometry (65%); delayed colonic transit (13%); altered manometric pattern (13%); and no transit and manometric impairment (9%). There were no differences in the number of neurons/ganglion between PD/ CC vs CC or vs controls. A reduced number of submucosal neurons containing VIP immunoreactivity was found in PD/ CC vs controls ( P<.05). VIP, VIPR1, and VIPR2 mRNA expression was significantly reduced in PD/ CC vs CC and controls ( P<.05). Conclusions and Inferences Colonic motor and rectal sensory functions are impaired in most PD/ CC patients. These abnormalities are associated with a decreased VIP expression in submucosal neurons. Both sensory-motor abnormalities and neurally mediated motor and secretory mechanisms are likely to contribute to PD/ CC pathophysiology. [ABSTRACT FROM AUTHOR]

Published
2017
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40. Neurokinin 1 Receptor Expression in the Rat Retina

Author

Casini, Giovanni, Rickman, D. W., Sternini, C., and Brecha, N. C.

Subjects
Neurons, Rats, Sprague-Dawley, Animals, sense organs, Receptors, Neurokinin-1, Immunohistochemistry, Article, Retina, Rats
Abstract

Tachykinin (TK) peptides influence neuronal activity in the inner retina of mammals. The aim of this investigation was to determine the cellular localization of the neurokinin 1 receptor (NK1), whose preferred ligand is the TK peptide substance P (SP), in the rat retina. These studies used a polyclonal antiserum directed to the C-terminus of rat NK1. The majority of NK1-immunoreactive (IR) cells were located in the proximal inner nuclear layer (INL), and very rarely they were found in the distal INL. Some small and large NK1-IR somata were present in the ganglion cell layer. NK1-IR processes were densely distributed across the inner plexiform layer (IPL) with a maximum density over lamina 2 of the IPL. Immunoreactive processes also crossed the INL and ramified in the outer plexiform layer where they formed a sparse meshwork. NK1-IR processes were rarely observed in the optic nerve fiber layer. Double-label immunofluorescence studies with different histochemical markers for bipolar cells indicated that NK1 immunoreactivity was not present in bipolar cells. Together, these observations indicate that NK1 immunoreactivity is predominantly expressed by amacrine, displaced amacrine, interplexiform, and some ganglion cells. Double-label immunofluorescence experiments were also performed to characterize NK1-containing amacrine cells. Sixty-one percent of the γ-aminobutyric acid (GABA)-IR cells, 71% of the large tyrosine hydroxylase (TH)-IR cells, and 100% of the small TH-IR cells contained NK1 immunoreactivity. In addition, most (91%) of the NK1-IR cells had GABA immunoreactivity. In contrast, vasoactive intestinal polypeptide-, TK-, choline acetyltransferase-, and parvalbumin-IR amacrine cells did not express NK1 immunoreactivity. Overall, the present findings suggest that SP acts directly upon several cell populations, including GABA-containing amacrine cells and ganglion cells, to influence visual information processing in the inner retina. J. Comp. Neurol. 389:496–507, 1997.

Published
1997

41. MHD activity in FTU plasmas with reversed magnetic shear

Author

Buratti, P, Micozzi, F, Tudisco, P, Acitelli, O, Angelini, L, Apicella, B, Apruzzese, M, Barbato, G, Bertocchi, E, Bracco, A, Bruschi, G, Buceti, A, Cardinali, G, Centioli, A, Cesario, C, Ciattaglia, R, Ciotti, S, Cirant, M, Cocilovo, S, Crisanti, V, De Angelis, F, De Marco, R, Esposito, F, Frigione, B, Gabellieri, D, Gatti, L, Giovannozzi, G, Gourlan, E, Granucci, C, Grolli, G, Imparato, M, Kroegler, A, Leigheb, H, Lovisetto, M, Maddaluno, L, Maffia, G, Mancuso, G, Marinucci, A, Mazzitelli, M, Mirizzi, G, Orsitto, F, Pacella, F, Panaccione, D, Panella, L, Pericoli Ridolfini, M, Pieroni, V, Podda, L, Righetti, S, Romanelli, F, Santini, F, Sassi, F, Segre, M, Simonetto, S, Sozzi, A, Sternini, C, Tuccillo, S, Valente, A, Vitale, F, Vlad, V, Zanza, G, and Zerbini, V

Subjects
Settore FIS/07 - Fisica Applicata(Beni Culturali, Ambientali, Biol.e Medicin)
Published
1997

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