Acute Toxicity and Histopathological Effects of Crude Aqueous Extract of Jatropha curcas Leaves in Mice

Azubike, N.C.; Okwuosa, Chukwugozie N; Achukwu, Peter Uwadiegwu; Maduka, T.C.; Chike, Okonkwo James

doi:10.3923/rjmp.2015.340.346

Cited by 9 publications

(2 citation statements)

References 14 publications

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“…There was significant relevant hemorrhage in the intestine of rats that received dimethoate. Damages to the blood vessel could be responsible for the hemorrhage observed in these organs [35]. The result of this study also supports histopathological finding of Ateeq [36] who observed that there were congested blood vessels, hemorrhage and infiltration in the intestinal tissues and changes such as degeneration, tubular degeneration, hemorrhage, infiltration, tubular cast and compressed blood vessel in the lungs, kidney and liver of dimethoate treated mice.…”

Section: Discussionsupporting

confidence: 89%

In-vivo investigation of dimethoate toxicity on serum enzymes, target organs and intestinal tissues of albino rats

Peter Ogbu Arubi,

Jeremiah John Oloche

2023

World J. Adv. Res. Rev.

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Dimethoate is a broad spectrum organophosphate insecticide used to control agricultural, industrial and domestic pests. Despite its benefits, toxicities in non-target organisms have been widely reported. This study investigated acute and sub-chronic toxicities of dimethoate in rats. The arithmetic method of Karbar and a modification of repeated 8-week oral toxicity were adopted for the determination of acute and sub-chronic toxicities of dimethoate, respectively. Symptoms of acute toxicity evaluated include muscular weakness, respiratory distress, convulsion and death. Animals that were used for the sub-chronic toxicity studies were divided into 4 groups of 5. Groups 2, 3 and 4 were fed with feeds containing 200, 500 and 800 mg/kg dimethoate respectively, while group 1 served as the control. The weight of the animals were determined weekly for 8 weeks, and thereafter sacrificed. Blood samples were collected for biochemical tests, and the liver, kidney, lung, intestine and heart were excised and processed for histopathological analysis. The calculated median lethal dose (LD50) was 176 mg/kg. Animals in all groups gained weight progressively. However, a dose-dependent significant rise in alanine transaminase and alkaline phosphatise, but not aspartate transaminase accompanied with significant focal necrosis in liver, eosinphilic casts in kidney and intestinal ulceration in group 3 and 4 in animals. In addition, dimethoate- induced inflammation was observed in the liver, kidney, lung and intestine tissues. The derangement of biochemical parameters and relevant histopathological alterations observed in rats exposed to dimethoate are suggestive of toxicity. Therefore necessary precautionary measures should be taking during handling and use.

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Section: Discussionsupporting

confidence: 89%

In-vivo investigation of dimethoate toxicity on serum enzymes, target organs and intestinal tissues of albino rats

Peter Ogbu Arubi,

Jeremiah John Oloche

2023

World J. Adv. Res. Rev.

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“…The extract was prepared using maceration method described by Azubike et al (2015). Fresh leaves of Dryopteris filix-mas were washed with tap water and airdried at room temperature for one week.…”

Section: Preparation Of Plant Extractmentioning

confidence: 99%

Sub-chronic toxicity evaluation of Dryopteris filix-mas (L.) schott, leaf extract in albino rats

Erhirhie

Ilodigwe

2019

Braz. J. Pharm. Sci.

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This study evaluated the acute and sub-chronic toxicities of ethanol leaf extract of Dryopteris filix-mas. Acute toxicity and phytochemical tests on ethanol leaf extract were determined. In sub-chronic toxicity test, animals were treated with 62.5, 125, 250 and 500 mg/kg of extract every day for 90 days. Blood samples were collected via retro-orbital puncture for baseline studies and at 31, 61 and 91 st days for determination of hematological, kidney and liver function parameters. Liver and kidneys were harvested for histopathology analyses on 91 st day. Also, a 28 day recovery study was carried out to determine reversibility in toxicological effects. Phytochemical screening revealed the presence of tannins, phenols, flavonoids, saponins, steroids, alkaloids, terpenoids, reducing sugar and cardiac glycosides. Acute toxicity test did not show toxicity or death at 5000 mg/kg. There was significant (p<0.005) reduction in white blood cell and lymphocyte counts, significant (p<0.05) increase in some liver and kidney biomarkers as well as alterations in liver and kidney histo-architecture on 91 st days in animals that were treated with 250 and 500 mg/kg extract. However, toxicities observed on 91 st day were reversible in recovery studies. The leaf extract of Dryopteris filix-mas may be hepatotoxic and nephrotoxic when used for long periods.

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Acute and subacute dermal toxicity of ethanolic extract of Melastoma malabathricum leaves in Sprague-Dawley rats

et al. 2020

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Acute Toxicity and Histopathological Effects of Crude Aqueous Extract of Jatropha curcas Leaves in Mice

Cited by 9 publications

References 14 publications

In-vivo investigation of dimethoate toxicity on serum enzymes, target organs and intestinal tissues of albino rats

In-vivo investigation of dimethoate toxicity on serum enzymes, target organs and intestinal tissues of albino rats

Sub-chronic toxicity evaluation of Dryopteris filix-mas (L.) schott, leaf extract in albino rats

Acute and subacute dermal toxicity of ethanolic extract of Melastoma malabathricum leaves in Sprague-Dawley rats

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