To investigate useful biomarkers associated with proximal tubular injury, we assessed
changes in levels of a focused set of biomarkers in urine and blood. Male rats
administered a single dose or four doses of gentamicin (GM, 240 mg/kg/day) or a single
dose of cisplatin (CDDP, 5 mg/kg) were euthanized on days 2 (the day after initial dosing)
5, or 12. At each time point, histopathological examination of the kidney and
immunohistochemistry for biomarkers, kidney injury molecule-1 (Kim-1), lipocalin (NGAL),
clusterin (CLU), cystatin C (CysC) and β2-microglobulin (β2M) were performed. Biomarker
levels were measured in urine and blood. In both treatment groups, degenerated/necrotic
proximal tubules and regenerated tubules were mainly observed on days 5 and 12,
respectively. At the same time as these tubular injuries, urinary Kim-1, CysC and β2M
levels were increased. Moreover, urinary levels of CysC and β2M in GM-treated animals and
Kim-1 in CDDP-treated animals increased (on day 2) prior to tubular injury on day 5. This
was considered to reflect the characteristics of drug toxicity. Although almost all of the
biomarkers in blood were not sufficiently sensitive to detect proximal tubular injury,
urinary and plasma β2M levels simultaneously increased. Therefore, in addition to urinary
Kim-1, CysC and β2M levels, plasma β2M levels were also considered useful for detecting
proximal tubular injury.
To investigate the effect of enzymatically modified isoquercitrin (EMIQ) on hepatocellular tumor promotion induced by phenobarbital (PB), male rats were administered a single intraperitoneal injection of 200 mg/kg N-diethylnitrosamine (DEN) and then fed with a diet containing PB (500 ppm) for 8 weeks, with or without EMIQ (2,000 ppm) in the drinking water. One week after PB administration, rats underwent a two-thirds partial hepatectomy. The PB-induced increase in the number and area of glutathione S-transferase placental form-positive foci and the proliferating cell nuclear antigen-positive ratio was significantly suppressed by EMIQ. Real-time reverse transcription-polymerase chain reaction analysis revealed increases in mRNA expression levels of Cyp2b2 and Mrp2 in the DEN-PB and DEN-PB-EMIQ groups compared with the DEN-alone group, while the level of Mrp2 decreased in the DEN-PB-EMIQ group compared with the DEN-PB group. There were no significant changes in microsomal reactive oxygen species (ROS) production and oxidative stress markers between the DEN-PB and DEN-PB-EMIQ groups. Immunohistochemically, the constitutive active/androstane receptor (CAR) in the DEN-PB group was clearly localized in the nuclei, but its immunoreactive intensity was decreased in the DEN-PB-EMIQ group. These results indicate that EMIQ suppressed the liver tumor-promoting activity of PB by inhibiting nuclear translocation of CAR, and not by suppression of oxidative stress.
Acifluorfen (ACI), a protoporphyrinogen oxidase (PROTOX) inhibitor herbicide, promotes the accumulation of protoporphyrin IX (PPIX), and induces tumors in the rodent liver. Porphyria is a risk factor for liver tumors in humans; however, the specific mechanisms through which ACI induces hepatocarcinogenesis in rodents are unclear. Here, we investigated the mode of action of ACI-induced hepatocarcinogenesis, focusing on constitutive androstane receptor (CAR, NR1I3), which is essential for the development of rodent liver tumors in response to certain cytochrome P450 (CYP) 2B inducers. Dietary treatment with 2500 ppm ACI for up to 13 weeks increased Cyp2b10 expression in the livers of wild-type (WT) mice, but not in CAR-knockout (CARKO) mice. Microscopically, ACI treatment-induced cytotoxic changes, including hepatocellular necrosis and inflammation, and caused regenerative changes accompanied by prolonged increases in the numbers of proliferating cell nuclear antigen-positive hepatocytes in WT mice. In contrast, these cytotoxic and regenerative changes in hepatocytes were significantly attenuated, but still observed, in CARKO mice. ACI treatment also increased liver PPIX levels similarly in both genotypes; however, no morphological evidence of porphyrin deposition was found in hepatocytes from either genotype. Treatment with 2500 ppm ACI for 26 weeks after initiation with diethylnitrosamine increased the incidence and multiplicities of altered foci and adenomas in hepatocytes from WT mice; these effects were significantly reduced in CARKO mice. These results indicated that prolonged cytotoxicity in the liver was a key factor for ACI-induced hepatocarcinogenesis, and that CAR played an important role in ACI-induced liver injury and tumor development in mice.
A 10-year-old female miniature poodle had a mass in its carpal joint of the left
forelimb. The tumor was divided into small multiple lobules by delicate
connective tissues, and necroses were found in some of the central lobules. In
some connective stromal areas, chondroid and osteoid tissues were formed. The
tumor cells were similar to the structure of apocrine gland epithelial cells
with apical blebs resembling apocrine secretion and eosinophilic secretary
materials within the luminal space, and spindle cells were sometimes found in
the basal area of the glandular structure. In some areas, tumor cells invaded in
the blood vessels, bone and bone marrow. Immunohistochemically, the tumor cells
forming tubulo-acinar to solid structures were intensely positive for
cytokeratin and keratin K8/K18, and the spindle cells were positive for vimentin
and alpha-smooth muscle actin. This case was diagnosed as a malignant mixed
apocrine gland tumor with metastases to the bone and bone marrow.
In this report, we describe a case of neuroendocrine carcinoma of undetermined
origin in a dog. Necropsy revealed scattered small neoplastic nodules in the
bilateral lungs and a small nodule in the parapancreatic lymph node.
Histopathologically, both pulmonary and lymph nodal nodules showed a similar
histologic pattern, with neoplastic cells being arranged in diffusely
proliferating sheet-like cellular nests separated by variable amounts of fibrous
septa, sometimes forming rosettes and duct-like structures. Scattered small
necrotic foci and invasion to fibrous septa were typically observed. Neoplastic
cells showed round to oval-shaped nuclei with prominent nucleoli and abundant
eosinophilic cytoplasm that were positive for Grimelius’ silver impregnation
staining and immunostaining with cytokeratin, synaptophysin, vasoactive
intestinal peptide and chromogranin A, indicative of the development of a
neuroendocrine carcinoma. However, judging from the distribution of tumors
lacking the portion suggestive of the primary site in any organ examined, as
well as no further indication of differentiation potential of neoplastic cells,
this tumor has so far been diagnosed as neuroendocrine carcinoma of undetermined
origin.
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