Efficacy of oryzalin and associated histological changes in Cryptosporidium-infected neonatal rats

This paper reports the anti-cryptosporidial effects of, and concomitant amelioration of the histological changes in the gut of neonatal rats with intestinal cryptosporidiosis treated with the dinitroaniline, oryzalin. The ED50 was determined to be 7 mg/kg using twice daily doses administered for 3 consecutive days. A maximum inhibition of 85.5% was achieved at 25 mg/kg and this inhibition remained constant despite increasing the oryzalin dose to 200 mg/kg. Cryptosporidiosis significantly decreased the intestinal villus/crypt (VC) ratio by approximately 50% (duodenum = 2.3, jejunum = 2.5 and ileum = 1.7) when compared to uninfected untreated controls (duodenum = 4.3, jejunum = 5.9 and ileum = 4.5). Treatment with oryzalin doubled the VC ratio in the duodenum, jejunum and ileum following doses of 5 mg, 50 mg and 200 mg/kg respectively. Oryzalin concentrations in the small intestine contents and plasma were determined, using HPLC, at 0.5, 1 and 2 h after dosing. The much greater dose required to return VC ratios to normal in the ileum (200 mg/kg) compared to the duodenum (6.25 mg/kg) appeared to reflect the decreased concentration of the drug in the distal small intestine. Concentrations of oryzalin equivalent to the in vitro IC50 were maintained for 2 h in the first half of the small intestine following a single dose of 100 mg/kg.

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Intestinal calcium transport in the spontaneously hypertensive rat: response to calcium depletion

AJP Gastrointestinal and Liver Physiology ◽

10.1152/ajpgi.1986.250.4.g412 ◽

1986 ◽

Vol 250 (4) ◽

pp. G412-G419

Author(s):

H. P. Schedl ◽

D. L. Miller ◽

R. L. Horst ◽

H. D. Wilson ◽

K. Natarajan ◽

...

Keyword(s):

Vitamin D ◽

Small Intestine ◽

Calcium Transport ◽

Spontaneously Hypertensive Rat ◽

Calcium Depletion ◽

Spontaneously Hypertensive ◽

Distal Small Intestine ◽

Wistar Kyoto

We previously found intestinal Ca2+ transport to be lower in the spontaneously hypertensive (SH) as compared with the Wistar-Kyoto control (WKY) rat. These animals were fed a relatively high (1%) Ca2+ diet, and the concentration of 1 alpha,25-dihydroxycholecalciferol [1 alpha,25(OH)2D3] in serum was the same in both groups. In the present experiment we tested the possibility that the lower Ca2+ transport in the SH rat was the result of unresponsiveness to 1 alpha,25(OH)2D3. We fed diets high and low in Ca2+ and measured serum 1 alpha,25(OH)2D3 and Ca2+ transport. Serum 1 alpha,25(OH)2D3 increased in response to Ca2+ depletion at both 5 and 12 wk in both the WKY and SH rat. With high-Ca2+ diet, Ca2+ transport was lower in SH than in WKY when studied 1) in vitro in duodenum at 5 wk of age, and 2) in vivo in proximal and distal small intestine at 12 wk of age. Ca2+ transport increased in SH in response to Ca2+ depletion, but not in WKY, except in distal small intestine in vivo at 12 wk. In summary, although Ca2+ transport is lower in the SH as compared with the WKY rat when vitamin D activity is basal through feeding a high-Ca2+ diet, Ca2+ transport increases in the SH rat in response to the increase in 1 alpha,25(OH)2D3 produced by feeding a low-Ca2+ diet. We conclude that 1) the vitamin D-regulated component of mediated Ca2+ transport is intact in the SH rat and is unrelated to hypertension, and 2) mediated Ca2+ transport under basal conditions, i.e., nonvitamin D-regulated, differs in the SH and WKY rats and may be related to hypertension.

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Effect of Yersinia enterocolitica on intestinal mucin secretion

AJP Gastrointestinal and Liver Physiology ◽

10.1152/ajpgi.1989.256.2.g319 ◽

1989 ◽

Vol 256 (2) ◽

pp. G319-G327 ◽

Cited By ~ 1

Author(s):

M. Mantle ◽

E. Thakore ◽

J. Hardin ◽

D. G. Gall

Keyword(s):

Small Intestine ◽

Yersinia Enterocolitica ◽

Proximal Colon ◽

Mucin Secretion ◽

Glycoprotein Synthesis ◽

Distal Small Intestine ◽

Intestinal Mucin ◽

Graded Response

Mucin and glycoprotein synthesis and secretion were evaluated in the upper, mid, and distal small intestine and in the proximal colon of rabbits infected with Yersinia enterocolitica (YE). Infected (INF) animals were examined on day 6 and compared with pair-fed controls and unmanipulated weight-matched rabbits. Tissue mucin content in vivo and mucin secretion in vitro, measured by a specific immunoassay, were significantly elevated in all four regions of the gut of INF rabbits compared with both control groups. In vitro secretion of stored glycoprotein, prelabeled with [3H]glucosamine, was not increased in the upper and mid small intestine of INF animals but was significantly elevated in the distal small intestine and proximal colon. In vitro incorporation of [14C]glucosamine was increased in all four regions of the gut of INF rabbits, but secretion of newly synthesized [14C]glycoprotein was only significantly elevated in the distal small intestine and proximal colon. A graded response was observed down the intestinal tract of INF rabbits, with the greatest increase in mucin content, synthesis and secretion occurring in the distal small intestine and proximal colon where the morphological impact of disease is also most severe.

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Neural mediation of cholera toxin-induced mucin secretion in the rat small intestine

AJP Gastrointestinal and Liver Physiology ◽

10.1152/ajpgi.1993.265.6.g1050 ◽

1993 ◽

Vol 265 (6) ◽

pp. G1050-G1056 ◽

Cited By ~ 6

Author(s):

B. A. Moore ◽

K. A. Sharkey ◽

M. Mantle

Keyword(s):

Small Intestine ◽

Cholera Toxin ◽

Fold Increase ◽

Open Loop ◽

Sensory Nerves ◽

Loop Model ◽

Rat Small Intestine ◽

Mucin Secretion ◽

Distal Small Intestine

We examined the role of enteric nerves in cholera toxin (CT)-induced mucin secretion in proximal and distal regions of rat small intestine. Stimulation of intestinal loops with 120 micrograms (1.5 mumol) CT using an in vitro open-loop model resulted in an approximately four-fold increase in luminal mucin content over unstimulated controls in both regions of the gut. Prior treatment of loops with tetrodotoxin had no effect on the amount of mucin released in response to CT. However, permanent destruction of primary sensory afferent nerves by neonatal treatment of rats with capsaicin reduced the mucin response to CT to baseline levels in both regions. In normal animals, atropine resulted in approximately 40% inhibition of mucin secretion in both the proximal and distal small intestine. The atropine-sensitive secretory response appears to be a component of the capsaicin-sensitive response. These results suggest that choleraic mucin secretion is mediated primarily by a capsaicin-sensitive neurogenic pathway involving local activation of sensory nerves, which may then elicit mucin secretion through interaction with cholinergic nerves.

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Human milk oligosaccharides are differentially metabolised in neonatal rats

British Journal Of Nutrition ◽

10.1017/s0007114512005727 ◽

2013 ◽

Vol 110 (4) ◽

pp. 640-650 ◽

Cited By ~ 35

Author(s):

Evelyn Jantscher-Krenn ◽

Carolin Marx ◽

Lars Bode

Keyword(s):

Small Intestine ◽

Human Milk ◽

Neonatal Rats ◽

Human Milk Oligosaccharides ◽

Milk Oligosaccharides ◽

Target Organs ◽

Mother's Milk ◽

Mother’S Milk ◽

Breast Fed

Human milk oligosaccharides (HMO) are complex glycans that are highly abundant in human milk, but not in infant formula. Accumulating data, mostly from in vitro and animal studies, indicate that HMO benefit the breast-fed infant in multiple ways and in different target organs. In vitro incubation studies suggest that HMO can resist the low pH in the infant's stomach and enzymatic degradation in the small intestine and reach the colon in the same composition as in the mother's milk. The oligosaccharide composition in faeces of breast-fed infants is, however, very different from that in the mother's milk, raising questions on when, where and how HMO are metabolised between ingestion and excretion. To answer some of these questions, we established a pulse-chase model in neonatal rats and analysed HMO profiles to track their composition over time in five consecutive equal-length intestinal segments as well as in serum and urine. The relative abundance of individual HMO changed significantly within the first 2 h after feeding and already in the segments of the small intestine prior to reaching the colon. Only 3′-sialyllactose, the major oligosaccharide in rat milk, and hardly any other HMO appeared in the serum and the urine of HMO-fed rats, indicating a selective absorption of rat milk-specific oligosaccharides. The present results challenge the paradigm that HMO reach the colon and other target organs in the same composition as originally secreted with the mother's milk. The present results also raise questions on whether rats and other animals represent suitable models to study the effects of HMO.

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Porcine Small and Large Intestinal Microbiota Rapidly Hydrolyze the Masked Mycotoxin Deoxynivalenol-3-Glucoside and Release Deoxynivalenol in Spiked Batch Cultures In Vitro

Applied and Environmental Microbiology ◽

10.1128/aem.02106-17 ◽

2017 ◽

Vol 84 (2) ◽

Cited By ~ 10

Author(s):

Silvia W. Gratz ◽

Valerie Currie ◽

Anthony J. Richardson ◽

Gary Duncan ◽

Grietje Holtrop ◽

...

Keyword(s):

Small Intestine ◽

Intestinal Tract ◽

Fecal Microbiota ◽

Microbiota Composition ◽

Batch Cultures ◽

Masked Mycotoxins ◽

Distal Small Intestine ◽

Liquid Chromatography Tandem Mass

ABSTRACT Mycotoxin contamination of cereal grains causes well-recognized toxicities in animals and humans, but the fate of plant-bound masked mycotoxins in the gut is less well understood. Masked mycotoxins have been found to be stable under conditions prevailing in the small intestine but are rapidly hydrolyzed by fecal microbiota. This study aims to assess the hydrolysis of the masked mycotoxin deoxynivalenol-3-glucoside (DON3Glc) by the microbiota of different regions of the porcine intestinal tract. Intestinal digesta samples were collected from the jejunum, ileum, cecum, colon, and feces of 5 pigs and immediately frozen under anaerobic conditions. Sample slurries were prepared in M2 culture medium, spiked with DON3Glc or free deoxynivalenol (DON; 2 nmol/ml), and incubated anaerobically for up to 72 h. Mycotoxin concentrations were determined using liquid chromatography-tandem mass spectrometry, and the microbiota composition was determined using a quantitative PCR methodology. The jejunal microbiota hydrolyzed DON3Glc very slowly, while samples from the ileum, cecum, colon, and feces rapidly and efficiently hydrolyzed DON3Glc. No further metabolism of DON was observed in any sample. The microbial load and microbiota composition in the ileum were significantly different from those in the distal intestinal regions, whereas those in the cecum, colon and feces did not differ. IMPORTANCE Results from this study clearly demonstrate that the masked mycotoxin DON3Glc is hydrolyzed efficiently in the distal small intestine and large intestine of pigs. Once DON is released, toxicity and absorption in the distal intestinal tract likely occur in vivo. This study further supports the need to include masked metabolites in mycotoxin risk assessments and regulatory actions for feed and food.

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Kinetics of Mucosal Influx of Glycylsarcosine, Glycine and Leucine into Hamster Jejunum and Ileum in Vitro

Clinical Science ◽

10.1042/cs0560025 ◽

1979 ◽

Vol 56 (1) ◽

pp. 25-31 ◽

Cited By ~ 9

Author(s):

H. P. Schedl ◽

D. Burston ◽

E. Taylor ◽

D. M. Matthews

Keyword(s):

Amino Acids ◽

Small Intestine ◽

Substrate Concentration ◽

Experimental Conditions ◽

Simple Diffusion ◽

Distal Small Intestine ◽

Diffusion Component ◽

Wet Weight ◽

Kinetics Of

1. This paper describes an investigation of the kinetics of influx of the dipeptide glycylsarcosine and the amino acids glycine and l-leucine into rings of everted hamster small intestine in vitro, in proximal and distal small intestine (jejunum and ileum). Results were expressed per unit wet weight of intestine. 2. At all concentrations studied (0·1–100 mmol/l), influx of glycylsarcosine was more rapid in the jejunum than in the ileum. In contrast, at all concentrations studied, influx of glycine and leucine was more rapid in the ileum than the jejunum. 3. Estimates of the simple diffusion component in total influx were made. This component became increasingly large as the substrate concentration was raised. After correction for simple diffusion, transport of all three substrates conformed to Michaelis-Menten kinetics in both jejunum and ileum. Values for simple diffusion, apparent Kt and Vmax. are reported. 4. Possibly physiological implications of the results are discussed, and it is pointed out that under experimental conditions similar to our own, simple diffusion is too large a component in total influx to be ignored.

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Electron probe x-ray microanalysis and electron microscopy of amino acid absorption and transport by the small intestine: inhibition by chemical poisons and correlation to the elemental composition of the epithelial cells

Proceedings, annual meeting, Electron Microscopy Society of America ◽

10.1017/s0424820100142311 ◽

1986 ◽

Vol 44 ◽

pp. 134-135

Author(s):

A. J. Tousimis

Keyword(s):

Small Intestine ◽

Amino Acid ◽

Epithelial Cells ◽

Elemental Composition ◽

Isotope Labeling ◽

Structural Components ◽

X Ray ◽

Human Small Intestine ◽

Transport Studies

The elemental composition of amino acids is similar to that of the major structural components of the epithelial cells of the small intestine and other tissues. Therefore, their subcellular localization and concentration measurements are not possible by x-ray microanalysis. Radioactive isotope labeling: I131-tyrosine, Se75-methionine and S35-methionine have been successfully employed in numerous absorption and transport studies. The latter two have been utilized both in vitro and vivo, with similar results in the hamster and human small intestine. Non-radioactive Selenomethionine, since its absorption/transport behavior is assumed to be the same as that of Se75- methionine and S75-methionine could serve as a compound tracer for this amino acid.

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Evaluation of the Impact of Excipients on Albendazole Concentrations in Upper Small Intestine Using an In Vitro Biorelevant Gastrointestinal Transfer (BioGIT) System

10.26226/morressier.57d6b2bbd462b8028d88e13f ◽

2016 ◽

Author(s):

Maria Vertzoni

Keyword(s):

Small Intestine ◽

The Impact

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HISTOLOGICAL CHANGES IN THE SMALL INTESTINE IN THE ADVANCED STAGES OF BURN DISEASE

World of Medicine and Biology ◽

10.26724/2079-8334-2017-3-61-90-96 ◽

2017 ◽

Vol 13 (61) ◽

pp. 090

Author(s):

G. M. Galunko

Keyword(s):

Small Intestine ◽

Histological Changes ◽

Advanced Stages ◽

Burn Disease

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Total Synthesis and Antibacterial Screening of (±)-6,8-Dihydroxy-3- undecyl-3,4-dihydroisochromen-1-one: A Structural Analogue of Metabolites from Ononis natrix

Letters in Drug Design & Discovery ◽

10.2174/1570180815666180502114402 ◽

2019 ◽

Vol 16 (3) ◽

pp. 245-248

Author(s):

Hummera Rafique ◽

Aamer Saeed ◽

Ehsan Ullah Mughal ◽

Muhammad Naveed Zafar ◽

Amara Mumtaz ◽

...

Keyword(s):

Total Synthesis ◽

Structural Analog ◽

Diffusion Method ◽

Bacterial Strains ◽

Antibacterial Screening ◽

Maximum Inhibition ◽

Bacillus Subtilus ◽

Hydrolysis Of ◽

Direct Condensation

Background: (±)-6,8-Dihydroxy-3-undecyl-3,4-dihydroisochromen-1-one is one of the structural analog of several substituted undecylisocoumarins isolated from Ononis natrix (Fabaceae), has been successfully synthesized by direct condensation of homopthalic acid (1) with undecanoyl chloride yields isochromen-1-one (2). Methods: Alkaline hydrolysis of (2) gave the corresponding keto-acid (3), which is then reduced to hydroxy acid (4) then its cyclodehydration was carried out with acetic anhydride to afford 3,4- dihydroisochromen-1-one (5). Followed by demethylation step, the synthesis of target 6,8- dihydroxy-7-methyl-3-undecyl-3,4-dihydroisocoumarin (6) was achieved. Results: In vitro antibacterial screening of all the synthesized compounds were carried out against ten bacterial strains by agar well diffusion method. Conclusion: Newly synthesized molecules exhibited moderate antibacterial activity and maximum inhibition was observed against Bacillus subtilus and Salmonella paratyphi.

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