Dichlorvos is highly toxic by means of the following: inhalation, absorption through skin, and ingestion. It is very volatile, and inhalation is the most common route of exposure 1. DDVP with organophosphates is readily absorbed by dermal absorption and with the effects of cholinesterase inhibition the acute illness from DDVP is limited which causes a more rapid onset of symptoms, followed by a similarly rapid recovery according to National library of medicine 2. This occurs because DDVP is rapidly metabolized and eliminated from the body. Persons with reduced liver disorders or recent exposure to cholinesterase inhibitors will be at increased risk from exposure to DDVP but alcoholic beverages may enhance the toxic effects of dichlorvos. High environmental temperatures or exposure of DDVP to light may increase the chance of its toxicity. It also causes the skin irritation, burning sensations, or actual burns. DDVP does not occur naturally in the environment and can be used as a synthetic organic chemical for insecticide in the manufactured industries. It is effective against mushroom flies, aphids, spider mites, caterpillars, thrips, and whiteflies in greenhouse, outdoor fruit, and vegetable crops. DDVP has been shown to exhibit neurotransmitter and relaxant functions 23.

MP Linn is a creeping annual or perennial herb and well known for the rapid plant movement. It contains the toxic alkaloid mimosine, which has been found to also have anti-proliferative and apoptotic effects 4. Aqueous extracts of the roots of the plant have shown significant neutralizing effects on the venom of the cobra 5 and also possess both antioxidant and antibacterial properties. MP plant has been suggested to possess low levels of toxicity. Phytochemistry has shown the compositions of MP as follows “alkaloids, flavonoid C-glycosides, sterols, terenoids, tannins, and fatty acid 6. The root of the plant has been shown to contain 10% tannin and a substance similar to adrenaline has been found within the plant leaves. The roots contain sac-like structures that release organic and organosulfur compounds including SO₂, methylsulfinic acid, pyruvic acid, lactic acid, ethanesulfinic acid, propane sulfinic acid, 2-mercaptoaniline, S-propyl propane 1-thiosulfinate, and thioformaldehyde 7.

Human consumption and exposure of dichlorvos-contaminated foods, water and environment can lead to decrease in proper liver function by a decrease in enzyme activity of the liver. Thus, MP is being investigated in the present study to determine its protective, as well as its therapeutic role on liver of mice exposed to dichlorvos.

This study used male animals to avoid the possible hormonal changes occurring in females’ oestrus cycles 11. Exposure to DDVP and MP simultaneously caused a decline in the health of the liver of treated animals which is ameliorated with MP treatment. A normal liver is healthy and free from collections and inflammatory cell 12. Several studies have shown that dichlorvos affects proper liver function during exposure 2 as DDVP is a known toxic organophosphate. The group that was fed with DDVP showed marked disruption of hepatic parenchyma, increased number of Kupffer cells, congested central vein and moderate infiltration of the inflammatory cells within the interstitial; while MP group showed hepatic tissue composed of the liver parenchyma separated by the sinusoids; Kupffer cells and the central vein appeared normal. This shows the ameliorative properties of MP, which may be due to the antioxidant properties associated with MP 13. The group that was administered with DDVP and MP concurrently showed marked periportal inflammatory cell infilterate, marked disruption of the hepatic parenchymal microanatomy as MP is not able to sufficiently ameliorate the toxic effect of DDVP as they were administered together.

The alanine aminotransferase (ALT) is a blood test that checks for liver damage 14. This enzyme is found mainly in the liver. In this study, ALT activity showed no significant effect on the liver of the administered groups when compared with the control this is because while ALT is a very versatile marker for liver pathologies, it does have its limits. It’s rarely specific, and there are many cases of liver pathology without corresponding increases in serum ALT. The body uses ALT to break down food into energy. Normally, ALT levels in the blood are low, if the liver is damaged, it will release more ALT into the blood and levels will rise. The normal value for ALT in blood is between 7 and 55 units per litre.

AST is an enzyme produced by the liver. Normally, AST levels in the blood are low. When the liver is damaged, it puts more AST into the blood, and increases the AST levels 14. AST activity was significantly increased in animals given DDVP with subsequent Mimosa treatment (DDVP+MP) compared with the control. DDVP+MP also shows significant increase in AST level when compared with animals given MP, and animals treated with DDVP only. This showed that there is significant liver damage caused by continued DDVP exposure. A high AST level is a sign of liver damage No significant difference was observed in animals treated with both dichlorvos and Mimosa concurrently (DDVP/MP).

ALP activity was significantly higher in animals treated concurrently with dichlorvos and Mimosa (DDVP/MP) compared with control. An alkaline phosphatase level test (ALP) measures the amount of alkaline phosphatase enzyme in your bloodstream. Abnormal levels of ALP in your blood most often indicate a problem with liver 14.

Total protein test is used to measure the total amount albumin and globulin in your bodyincrease in TP indicates the presence of liver disease. In this study, no significant difference was observed in the total protein level of the liver of experimental animals.

This study showed that dichlorvos caused tissue distortion in the mice with prominent toxic effects on the liver. The mimosa extract showed ameliorative effects on the liver that was exposed to DDVP.

ELA design and supervised the research. EE analyzed, interpreted the result and drafting the article. KA and AG provided research materials and organized data. SOS analyzed and helped in drafting the article. All authors reviewed and approved the final draft of the manuscript.

The authors are grateful to management of Afe Babalola University for providing a good environment to conduct this research. Authors are very grateful to Mr Fafure AA, Mr Adedeji A, Mrs kunlere O, Miss Nebo K for technical help, and support for this work and the MP plant was identified by Mr Omotayo Felix from the botany department of Ekiti state university.