1,4-Dioxane (DX) with two
oxygen atoms make it hydrophilic and infinitely soluble in water. As a synthetic organic compound, it used widely throughout industry as a
solvent.
Dioxane causes numerous human ailments such as liver damage and
kidney failure. It has been shown in research to be carcinogenic to animals, and is a potential
carcinogen to humans. Daily administration for
1,4-dioxane (100 mg/kg
body weight) in
drinking water for rats weighing 120 g, except for normal control group. Experimental animal for 42 days was followed through
body weight, serum
alkaline phosphatase, serum
creatinine,
malondialdehyde, and
catalase enzyme activity; beside histological patterns for liver, kidney, brain and ovary sections. Protection treatment has been offered using oral injection N-acetyl
cysteine (100 mg/kg b.wt.), and fresh 200 mg/kg b.wt. in diet meal for each of nabk, husk, and sycamore in separated groups.
Body weight and CAT activity have decreased by 25.8, and 68.7%, respectively. While increase has found in MDA, ALP and
creatinine values by 76, 48.9, and 67.3%, respectively. NAC showed improvement especially for MDA peroxidation marker and
creatinine for kidney disorder. On the other hand, nabk improved CAT activity and husk for ALP liver mutagenicity marker. Intoxicated DX showed
edema, kupffer cell activation,
atrophy of glomerular tuft, and
necrosis of neurons in liver, kidney and brain sections. Obviously nabk showed highly improvement in liver toxicity which is the most sensitive organ to DX as found in research.