Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:3.2.1.31 (
beta-glucuronidase
)
7,680
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
During the acute renal tubular dysfunction of Fanconi syndrome and type 2
renal tubular acidosis
(FS/RTA2) induced by maleic acid in the unanesthetized dog, we observed: 30 minutes after the onset of FS/RTA2, the urinary excretion of lysosomal enzymes, N-acetyl-beta-glucosaminidase (NAG),
beta-glucuronidase
(beta-gluc) and beta-galactosidase (beta-galac), increased simultaneously with the anticipated increase in renal clearance of lysozyme; the severities of all these hyperenzymurias increased rapidly, progressively, and in parallel, all reaching a peak some 60 to 80 minutes after their onset; thereafter, while the FS/RTA2 continued undiminished in severity, the severity of the hyperenzymurias decreased rapidly, greatly, progressively, and in parallel; and sodium phosphate loading strikingly attenuated the FS/RTA2 and the hyperenzymurias. Thus, the maleic acid-induced FS/RTA2 is attended by an acute reversible-complex derangement in the renal tubular processing of proteins that: affects not only lysozyme which is normally filtered, but also NAG and other lysosomal enzymes, which are not; and is to some extent functionally separable from that of FS/RTA2. The findings suggest that the derangements in renal processing of lysozyme and lysosomal enzymes are linked, and that a phosphate-dependent metabolic abnormality in the proximal tubule can participate in the pathogenesis of both these derangements and the FS/RTA2.
...
PMID:Coordinately increased lysozymuria and lysosomal enzymuria induced by maleic acid. 310 28
We used the A-chain of the toxin ricin (
RTA
) as a toxin specific to Kupffer cells in mice.
RTA
is specifically taken up by the mannose receptor present exclusively in macrophages. Kupffer cells were quantitated by shifts in
beta-glucuronidase
clearance and microscopic counts of cells which phagocytosed India ink. When compared to saline controls, 20 mg/kg of
RTA
intraperitoneally (divided over 4 days) or intraportally (single doses) significantly prolonged the t 1/2 half-life of
beta-glucuronidase
by 270 +/- 37 and 210 +/- 8%, respectively. Kupffer cell numbers were significantly decreased by 27 +/- 8 and 33 +/- 16%. This effect persisted for at least 3 days after toxin administration. Despite effects on Kupffer cell number, minimal histological damage to liver, spleen, lung, and heart was noted. Higher doses of
RTA
or doses potentiated by ureteral ligation to prevent renal clearance resulted in prohibitive mortalities and histologic liver damage. Doses of Hura crepitans inhibitor, a toxin similar to
RTA
but not mannose-receptor specific, did not affect Kupffer cell numbers. We conclude that
RTA
given both intraperitoneally and intraportally at low doses is toxic specifically to Kupffer cells. Kupffer cell numbers can be indirectly measured by
beta-glucuronidase
clearance.
...
PMID:Use of ricin A-chain to selectively deplete Kupffer cells. 339 96
