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Query: EC:3.1.3.1 (
alkaline phosphatase
)
47,916
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
A study was conducted on 60 broiler chicks of the effect of activated charcoal (200 ppm) on the toxicity of 0.5 ppm
aflatoxin B1
(
AFB1
) in feed fed from day 1 to day 42. Activated charcoal was found to be moderately effective in reducing the harmful effects of
AFB1
as assessed by growth response and various biochemical parameters. The feeding of activated charcoal along with
AFB1
reduced the inhibitory effect of
AFB1
on bodyweights and feed intake. There was also a significant improvement in the serum aspartate aminotransferase,
alkaline phosphatase
, total proteins, calcium and phosphorus levels. However, no significant improvement was observed in cholesterol levels.
...
PMID:Toxicity of aflatoxin B1 in broiler chicks and its reduction by activated charcoal. 814 51
The hepatoprotective activity of Picroliv, a standardized iridoid glycoside fraction of Picrorhiza kurroa, has been investigated by studying the protection of biochemical and histological changes induced in livers of rats given single oral doses (7 mg/kg) of
aflatoxin B1
. Administration of
aflatoxin B1
resulted in a significant increase in 5'-nucleotidase, r-glutamyl transpeptidase, acid ribonuclease, total lipids, cholesterol and lipid peroxides in liver and transaminases,
alkaline phosphatase
and bilirubin in serum. However, the activity of glucose 6-phosphatase and levels of cytochrome P450, cytochrome b5, DNA, RNA, proteins and glycogen in liver and total proteins in serum decreased. The liver histology showed ballooned hepatocytes, degeneration, microvesicular fat, focal necrosis, bile duct hyperplasia and proliferation of oval and spindle cells in portal tracts. When Picroliv (25 mg/kg x 7 days) was given to
aflatoxin B1
toxicated rats, the majority of the biochemical and histological changes were significantly protected. The findings indicate a hepatoprotective activity of Picroliv against
aflatoxin B1
toxicity in rats.
...
PMID:Picroliv protects against aflatoxin B1 acute hepatotoxicity in rats. 847 62
The acute effects of
Aflatoxin B1
(
AFB1
) were evaluated on C57B1/6, CBA/J, and Balb/c mice challenged with a single intraperitoneal dose of the mycotoxin (60 mg/Kg animal weight). 90 mice per strain were divided into three groups of 30 animals each: the intoxicated group and control groups I and II. Intoxicated mice were injected intraperitoneally with
AFB1
dissolved in corn oil, while control I mice received corn oil only (0.01 ml/g) by the same route. Lots of 10 animals from the intoxicated and control groups were sacrificed 24, 72 and 168 hours after challenge. Control mice II remained untreated and were used as standards of normality for biochemical (hepatic and renal function) and hematological evaluation.
AFB1
was detected in the liver of C57B1/6 and CBA/J mice 24 hours (1.46 and 0.75 ng/g, respectively), 72 hours (2.30 and 0.08 ng/g, respectively), and 168 hours (2.18 and 0.25 ng/g, respectively) after challenge. The mycotoxin was also observed in the liver of B10A mice (6.20 ng/g) 72 hours post-injection. The most evident histological lesions were observed 168 hours after treatment in C57B1/6 and B10A mice. Serum levels of
alkaline phosphatase
in intoxicated C57B1/6 and B10A mice were significantly higher than those of control I and II animals. The histopathologic lesions and biochemical changes were very discrete in Balb/c and CBA/J mice. It is included that strains C57B1/6 and B10A are more susceptible than strains CBA/J and Balb/c to the acute effects of
AFB1
. Such difference probably reflects each strain's ability to biotransform and eliminate
AFB1
and its metabolites.
...
PMID:Acute effect of aflatoxin B1 on different inbred mouse strains II. 875 23
Aflatoxin B1
is an important consideration in the aetiology of human and animal hepatocellular carcinoma. The influence of the drug, Semecarpus anacardium Linn. nut extract, on hepatocarcinogenicity of
aflatoxin B1
was evaluated in adult albino male Wistar rats.
Aflatoxin B1
was administered intraperitoneally to induce hepatocellular carcinoma. These cancer bearing animals were treated with Semecarpus anacardium Linn. nut extract (200 mg/kg body weight/day) in sunflower oil orally for 14 days. The plasma and the liver tumour tissue were investigated biochemically for lactate dehydrogenase, aspartate aminotransferase, alanine aminotransferase,
alkaline phosphatase
and gamma-glutamyl transpeptidase. The elevation of plasma concentration of these enzymes were indicative of the persistent deteriorating effect of
aflatoxin B1
in cancer bearing animals. Lactate dehydrogenase and aminotransferases levels were decreased in liver, whereas
alkaline phosphatase
and gamma-glutamyl transpeptidase were increased in cancer conditions. These enzyme levels were reversed to near normal control values in drug treated animals. The analysis of marker enzyme activities clearly indicates the antitumour efficacy of Semecarpus anacardium Linn. nut extract on
aflatoxin B1
induced hepatocellular carcinoma.
...
PMID:Anticancer potency of the milk extract of Semecarpus anacardium Linn. nuts against aflatoxin B1 mediated hepatocellular carcinoma bearing Wistar rats with reference to tumour marker enzymes. 1035 53
Single doses of
aflatoxin B1
(2 mg/kg, i.p.) caused significant increases in the activities of tau-glutamyl transpeptidase, 5'-nucleotidase, acid phosphatase and acid ribonuclease, and decreases in the activities of succinate dehydrogenase and glucose-6-phosphatase in liver, after 8 weeks. The level of lipid peroxides, DNA, RNA, and cholesterol increased while glycogen decreased. It also increased the serum level of transaminases, sorbitol dehydrogenase, glutamate dehydrogenase, lactate dehydrogenase, acid phosphatase,
alkaline phosphatase
, and bilirubin. Oral administration of picroliv (25 mg/kg/day for 15 days), a standardised iridoid glycoside fraction of Picrorhiza kurroa, 6 weeks after
aflatoxin B1
toxication, significantly prevented the biochemical changes induced in liver and serum of
aflatoxin B1
treated rats. The hepatocurative effect of picroliv and silymarin, a plant based standard hepatoprotective are comparable.
...
PMID:Hepatocurative effect of picroliv and silymarin against aflatoxin B1 induced hepatotoxicity in rats. 1119 26
The effects of prolonged oral administration (21 days) of fumonisin B1 (FB1) and
aflatoxin B1
(
AFB1
) were evaluated on male Wistar rats. The animals were housed in individual metabolic cages and submitted to the following treatments: 1-0 microg
AFB1
+ 0 mg FB1/100g bw.; 2-72 microg AFB1+ 0 mg FB1/100 g bw; 3-0 microg
AFB1
+ 0.5 mg FB1 g bw; 4-0 microg
AFB1
+ 1.5 mg FB1/100 g bw; 5-72 microg
AFB1
+ 0.5 mg FB1/100g bw; 6-72 microgAFB1 + 1.5 mg FB1/100g bw. On day 21, the rats were sacrificed for evaluation. The results showed that treated animals presented differences in body weight and absolute/relative weights of liver and kidney as well as altered hepatic function and cholesterol blood levels. Rats fed with the greatest doses of
AFB1
and FB1 gained less weight (2.79 g/day) at the end of the experimental period; their blood concentrations of liver enzymes aspartate aminotransferase (AST) and
alkaline phosphatase
(AP) were above control levels (130.35 micro/l and 471.00 micro/l, respectively). Blood cholesterol increased in the groups treated with the highest dose of FB1 or FB1 associated with
AFB1
. Histopathology revealed the occurrence of apoptosis in the liver of rats exposed to FB1. The association of
aflatoxin B1
with fumonisin B1 at higher dose probably potentiated the effects of the higher dose of fumonisin B1 acting singly.
...
PMID:Effects of prolonged oral administration of fumonisin B1 and aflatoxin B1 in rats. 1150 59
The aim of the study was to determine the effect of repeated applications of
aflatoxin B1
(
AFB1
) on immunocompetent cells (CD3 T cells) and
alkaline phosphatase
in the intestinal mucosa. Mice were orally treated with
AFB1
for 24 days. The mucosa of the intestine showed a significant decrease in the number of CD3 T cells and a significantly lower level activity of
alkaline phosphatase
on day 24 in
AFB1
treated mice. Similarly, with changes in the small intestine, qualitative haematological parameters were modified in systemic immunity as lymphopenia, and neutropenia, monocytopenia.
AFB1
treated animals showed reduction in body weight gain and increased liver weight. We supposed that changes found in the small intestine are secondary to primary systemic haematological lesions. The decrease in CD3 T cells suggests a connection with the decrease in the host's resistance to infectious diseases.
...
PMID:Effect of aflatoxin B1 on CD3 T cells and alkaline phosphatase in the intestine of mice. 1204 66
This study was undertaken to evaluate the effectiveness of L-ascorbic acid (AA) in alleviating the toxicity of
aflatoxin B1
(
AFB1
) in male New-Zealand white rabbits. Five rabbits (6 months of age and mean body weight 3.12 kg) per group were assigned to 1 of 6 treatment groups: 0 mg AA and 0 mg
AFB1
/kg BW (control); 20 mg AA/kg BW; 15 microg
AFB1
/kg BW; 15 microg
AFB1
plus 20 mg AA/kg BW; 30 pg
AFB1
/kg BW; 30 pg
AFB1
plus 20 mg AA/kg BW. Rabbits were orally administered their respective doses every other day for 9 weeks, followed by a 9-week recovery period where all drugs were withdrawn. Evaluations were made for hemato-biochemical parameters and enzymatic activities. Results showed that
AFB1
significantly (p < 0.05) decreased hemoglobin (Hb), total erythrocytic count (TEC) and packed cell volume (PCV), in a dose-dependent manner, and these effects were continued during the recovery period. Ascorbic acid caused an increase in these parameters, and alleviated the negative effect of
AFB1
during the treatment period. Additionally, serum concentrations of total protein, albumin and glucose were significantly (P < 0.05) declined by treatment with the high dose of aflatoxin and these effects were continued during the recovery period. Ascorbic acid caused non-significant increases in these parameters and alleviated the harmful effect of
AFB1
. On the other hand, aflatoxin treatment caused significant increases (P < 0.05) in the activities of serum aspartate aminotransferase (AST), alanine aminotransferase (ALT) and
alkaline phosphatase
(AlP) during the treatment period in a dose dependent manner, and this effect was continued during the recovery period, especially with the high dose. Also, treatment with the high dose of aflatoxin caused significant increases (P<0.05) in cholesterol and total bilirubin. Ascorbic acid caused significant decreases in these parameters and alleviated the harmful effects of
AFB1
. Whereas, Total leukocyte count (TLC), urea and creatinine were not significantly affected by aflatoxin-treatment. Generally, it is interesting feature that the treatment with AA alone had no negative effects on most of the previous parameters. Also, the presence of AA could diminished the adverse effects of
AFB1
on most of hematological and biochemical values, and enzymatic activities in rabbits.
...
PMID:Influence of ascorbic acid supplementation on the haematological and clinical biochemistry parameters of male rabbits exposed to aflatoxin B1. 1261 57
Hepatotoxic substances such as
aflatoxin B1
(
AFB1
) produce free radical reactions during biotransformation damage to liver cells. Vitamins C and E are important natural antioxidants suppressing free radicals. This study investigated the effects of vitamins C and E on liver enzymes and other biochemical parameters in rabbits experimentally exposed to
AFB1
. The first group was control and fed the diet with dimethyl sulfoxide; the second group received 0.1 mg
AFB1
/kg diet; the third group received vitamin C (100 mg L-ascorbic acid/kg diet); the fourth group received vitamin E (100 mg alpha-tocopherol/kg diet); and the fifth group received vitamin C+vitamin E (100 mg L-ascorbic acid/kg diet+100 mg alpha-tocopherol/kg diet). Diets of the second, third, fourth and fifth groups were mixed with 0.1 mg AFB/kg diet) and feedings were continued for 10 w. Levels of aspartate transaminase, alanine transaminase,
alkaline phosphatase
, creatine phosphokinase and lactate dehydrogenase after receiving
AFB1
were significantly increased, while activities of aspartate transaminase, alanine transaminase, amylase, creatine phosphokinase and lactate dehydrogenase in groups receiving
AFB1
+ vitamins C, E or C+E were significantly lower than that of the
AFB1
-alone group. Although of the activity of
alkaline phosphatase
increased with
AFB1
exposure, it decreased with vitamin C administration. Levels of urea, triglyceride, cholesterol and albumin were affected by
AFB1
and AFB1+vitaminC.
AFB1
affected some liver enzymes and other biochemical parameters, but vitamins C, E and C+E partially prevented an increase in these liver enzymes and some the biochemical parameters induced by
AFB1
.
...
PMID:Effects of vitamin C and E on liver enzymes and biochemical parameters of rabbits exposed to aflatoxin B1. 1530 90
To elucidate the potential factors modulating exposure to
aflatoxin B1
(
AFB1
) in three Chinese populations, an epidemiologic study was conducted in Fusui County and Nanning City of Guangxi Province and Chengdu City of Sichuan Province. The incidence rates of hepatocelluar carcinoma (HCC) for males in these three regions were 92-97 per 100,000, 32-47 per 100,000, and 21 per 100,000, respectively. Eighty-nine residents from Fusui, 196 residents from Nanning, and 118 residents from Chengdu were screened for
AFB1
-albumin adduct (AAA) levels and hepatitis virus (HBV, HCV, HDV, HEV, and HGV) infections, as well as liver biochemistry (alanine aminotransferase [ALT], aspartate aminotransferase [AST],
alkaline phosphatase
[ALP], y-glutamyl transpeptidase [GGT], 5'-nucleotidase, globulin [GLO], direct bilirubin, indirect bilirubin, and bile acid levels). At least one marker of hepatitis virus (HV) infection was present in 47.2% (42/89) of subjects from Fusui, while in Nanning and Chengdu the values were 15.8% (31/196) and 22.0% (26/118), respectively. In contrast to females, a higher level of AAA was observed in males; the difference was statistically significant in both the Nanning (P = 0.023) and the Chengdu (P = 0.026) subjects. In the Chengdu group, there was a significantly higher level of AAA in cases with HV infection (P = 0.041). There was a close association between AAA level and BMI in the adults without HV infection (r = 0.148, P = 0.044). Also, AAA was closely associated with DBIL and GGT in non-HV-infected minors (P < 0.05), closely associated with ALB, GLO, and GGT in HV-infected minors (P < 0.05), and closely associated with IBIL, GLO, TBA, and AST in non-HV-infected adults (P < 0.01). The co-effect of HV infection and
AFB1
exposure may be responsible for the high risk of HCC in the Fusui region, whereas age, gender, BMI, and HV infection may modify individual aflatoxin levels. The relationship between AAA level and liver biochemistry indicates injury induced by aflatoxin to both hepatic parenchyma and biliary tract. But the associations vary with age and HV infection status.
...
PMID:Associated factors in modulating aflatoxin B1-albumin adduct level in three Chinese populations. 1581 Jun 36
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