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Enzyme
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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)
The toxic effects of bis (tributyltin) oxide (TBTO) on the rat liver were studied with an electron microscope and the accumulation sites of tin were determined with an X-ray microanalyzer. The activities of serum enzymes and the concentration of serum bilirubin were also analyzed. Male Wistar rats received an intramuscular injection of 0.5 ml/kg of TBTO. Marked swelling of the mitochondria appeared in the hepatocytes 4 h after injection of TBTO. Cytoplasmic vacuoles, which contained degenerated mitochondria, gradually increased in number in these hepatocytes. This in turn may have caused a decrease in the volume of hepatic cell cords and an enlargement of sinusoids in the entire hepatic lobule. However, fine structures of intrahepatic bile ducts were not altered. By X-ray microanalysis, tin peaks were preferentially obtained from swollen mitochondria of the hepatocytes. By polarographic analysis of the respiratory responses of mitochondria, it was demonstrated that rates of state 4 respiration and respiratory control ratio were significantly disturbed in TBTO-treated rats in comparison with those of controls. The activities of AST (aspartate aminotransferase) and ALT (alanine aminotransferase) were significantly increased after TBTO treatment, but those of
ALP
(
alkaline phosphatase
), LAP (leucine aminopeptidase) and total bilirubin were not changed. These results indicated that parenterally administered TBTO accumulated in the liver cell mitochondria and disturbed oxidative phosphorylation. Mitochondrial dysfunction might induce severe damage of the hepatocytes. Four days after injection of TBTO, hepatic structures and chemical indices were almost restored by the regeneration of hepatocytes.
...
PMID:Studies on the hepatotoxicity induced by bis (tributyltin) oxide. 149 81
A weak anion-exchange high-performance liquid chromatographic procedure with post-column reaction detection for simultaneous determination of
alkaline phosphatase
(
EC 3.1.3.1
,
ALP
) isoenzymes is described. We identified six peaks with
ALP
isoenzyme activity in normal serum. The peaks were, in order of elution, one intestinal/bone, two bone and three liver
ALP
isoenzymes. This new assay with automatic injection, on-line post-column reaction detection and powerful integration data system could be of significant value in the routine clinical biochemistry laboratory. The advantages include improved sensitivity and selectivity over previous methods for the determination of
ALP
isoenzymes.
...
PMID:Determination of alkaline phosphatase isoenzymes in serum by high-performance liquid chromatography with post-column reaction detection. 150 Apr 60
A canine blood group antigen, QN, which was detected by a naturally occurring alloantibody in the antiglobulin test, was shown to be antigenically related to the human A and cattle J antigens by absorption experiments. Family studies supported a dominant mode of inheritance with the gene controlling the production of QN being dominant to the gene responsible for its absence. Frequencies of the QN and Tr antigens and serological data strongly suggested that the two antigens are identical. Two canine plasma
alkaline phosphatase
variants, F and S, were detected by starch gel electrophoresis, pH 8.65. Assuming genetic control of two codominant alleles, ALPF and ALPS, the distributions of types in families differed significantly from expectation. A relationship between the
ALP
and Tr(QN) systems was demonstrated with Tr-positive animals having a significant deficiency of S
alkaline phosphatase
types.
...
PMID:Canine plasma alkaline phosphatase polymorphism and its relationship with the canine Tr blood group system. 150 70
We report a case of recurrent transient hyperphosphatasemia in a 29-year-old man with immune deficiency. He had serum
alkaline phosphatase
(
ALP
;
EC 3.1.3.1
) activity 16.9- and 4.8-fold greater than the upper reference limit on two occasions; the activity returned to normal within 2 months on the first and within 1 month on the second. On both occasions we observed the typical electrophoretic pattern for
ALP
isoenzymes seen in transient hyperphosphatasemia of infancy. We noted no evidence of liver or bone disease. Recognition of the occurrence of transient hyperphosphatasemia of infancy in adults, although rare (it is the fifth case reported), seems as important as in children so that unnecessary extensive investigations are avoided.
...
PMID:Recurrent transient hyperphosphatasemia of infancy in an adult. 152 34
We investigated the prevalence and characteristics of intestinal alkaline phosphatase (
ALP
;
EC 3.1.3.1
) identified in human serum by cellulose acetate electrophoresis in 8% of fasting serum samples from hospital patients (n = 500) and in 35% of fasting serum samples from patients with diabetes mellitus (n = 106; not differentiated between types 1 and 2). The intestinal
ALP
electrophoretic band was usually heterogeneous and contained two major subtypes of
ALP
. Isoelectric focusing of intestinal-
ALP
-positive serum treated with levamisole and neuraminidase (EC 3.2.1.18) revealed two distinct regions of enzymatic activity that comigrated with
ALP
extracted from small intestinal and colonic mucosa. Anodic intestinal
ALP
was resistant to treatment with levamisole and neuraminidase and comigrated with
ALP
from small intestinal mucosa. The more-cathodic intestinal
ALP
, which comigrated with
ALP
from colonic mucosa, was completely inhibited by levamisole and converted by neuraminidase to a species with a more basic pI than that of neuraminidase-digested tissue-nonspecific form. This component of intestinal
ALP
may be of vascular origin.
...
PMID:Prevalence and properties of the intestinal alkaline phosphatase identified in serum by cellulose acetate electrophoresis. 156 15
This modified lectin affinity electrophoresis method is suitable for simultaneous measurement of liver, bone, and high-molecular-mass (high-Mr) isoforms of
alkaline phosphatase
(
ALP
;
EC 3.1.3.1
) in children. Age-related isoform reference ranges were derived for 247 children, ages 0-13 years. Liver
ALP
did not appear in plasma until after six months of age, and remained constant after one year of age. Bone
ALP
was highest in the youngest age group, and declined to relatively constant activities thereafter. High-MrALP was not detected in normal children. In bone disease, the bone isoform was increased in all age groups. In liver disease, only 5 of 30 infants younger than six months had detectable liver
ALP
, although half had increased bone
ALP
. Among children older than six months, 5 patients with biliary atresia and 15 patients with hepatitis A all had increased liver isoform activity. Liver
ALP
was also a sensitive index of early hepatobiliary complications in 27 nonjaundiced children with cystic fibrosis. Measurement of
ALP
isoforms therefore yields useful clinical information in children older than six months but is of doubtful value in younger infants.
...
PMID:Wheat-germ lectin affinity electrophoresis for alkaline phosphatase isoforms in children: age-dependent reference ranges and changes in liver and bone disease. 158 17
In patients with pancreatitis an increase of the total amount of
alkaline phosphatase
(
ALP
;
EC 3.1.3.1
) and the appearance of its macro isoenzyme which parallels the decrease of bone isoenzyme was found. This isoenzymatic profile suggests that the increase of
ALP
in pancreatitis is due to the concomitant hepatobiliary disorder. Moderate increases of
ALP
didn't appear to be related to the existence of gallstones.
...
PMID:[Isoenzyme profile of alkaline phosphatase in patients with pancreatitis]. 159 67
The diagnostic values of CA 19-9 and CEA were evaluated in 187 cases (including 31 gastric, 41 colorectal, 12 pancreatic, 7 hepatobiliar and 5 hepatocellular carcinomas). These tumor markers were compared to the other laboratory parameters [hemoglobin, erythrocyte sedimentation rate, serum bilirubin, ASAT (aspartate amino transferase), ALAT (alanine amino transferase) GGT (gamma glutamil transpeptidase),
ALP
(
alkaline phosphatase
)]. The specificity of CA 19-9 was 89.5%, while the sensitivity of this tumor markers was 91.7% in pancreatic carcinoma, 54.8% in gastric carcinoma and 43.9% in colorectal carcinoma. The sensitivity of CEA only in colorectal patients was higher than that of CA 19-9 (specificity 73.9%, sensitivity 64.5%). Although the CA 19-9 and CEA are not known to give any cross-reaction with each other, simultaneous measurement and evaluation of these two tumor antigens did not result in a better diagnostic sensitivity. After undergoing a gastrointestinal carcinoma operation, CA 19-9 indicated the appearance of tumor recidiva with a 62% sensitivity. Calculated together with CEA the sensitivity elevated to 88.9%. In most of the patient with benign cholostasis, the CA 19-9 and CEA values were out of the normal range (53.3% and 36.4% respectively), so these tumor markers are not suitable to differentiate between benign and malign cholostasis. According to the authors, CA 19-9 is the most useful diagnostic tool to differentiate between pancreatic carcinoma and pancreatitis chronica (both group without cholostasis), as well as for monitoring the patients after surgery of a gastrointestinal cancer.
...
PMID:[Diagnostic value of CA 19-9 and CEA in gastrointestinal pathology]. 160 81
Urinary enzyme activities (N-acetyl-beta-D-glucosaminidase [NAG],
alkaline phosphatase
[
ALP
], leucine aminopeptidase [LAP], gamma-glutamyl transpeptidase [gamma-GTP]) were investigated to determine their clinical significance in diabetic nephropathy. There were correlations among
ALP
, LAP, and gamma-GTP, though no correlation existed between NAG and the other three enzymes. Activities of NAG isozymes (both A and B) were higher than in normal controls. It has been reported that NAG isozyme A might be associated with glomerular diseases, and isozyme B might be associated with proximal tubular damage. The results of our study suggest that NAG reflects lysosomal dysfunction of both glomerular and proximal tubular epithelial cells, which may be caused by poor glycemic control, and that
ALP
, LAP, and gamma-GTP reflect brush border damage of proximal tubules, which may be caused by diabetic nephropathy.
...
PMID:Clinical significance of urinary enzymes in diabetic nephropathy. 168 60
Seventy-four patients' sera containing macroenzymes or other uncommon enzyme forms were analyzed for total creatine kinase, lactate dehydrogenase,
alkaline phosphatase
, or amylase activity on an Ektachem 700XR analyzer. The Ektachem test results correlated well with activities obtained by means of liquid reagents on RA-1000. For each enzyme tested, linear-regression analysis yielded data comparable with those for sera containing exclusively the more common isoenzymes. Increased concentrations of intestinal
ALP
, however, resulted in higher activities of total
ALP
being reported for the Ektachem.
...
PMID:Effect of isoenzyme composition on Kodak Ektachem test results for creatine kinase, lactate dehydrogenase, alkaline phosphatase, and amylase. 172 39
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