The influence of phenethyl isothiocyanate (PEITC) on cell kinetics in the target organs of N-nitrosobis(2-oxopropy1)amine (BOP) tumorigenicity and on xenohiotic-metabolizing enzymes was investigated in hamsters. Female 5-week-old Syrian hamsters were given a single S.C. dose of 0,20 or 50 mg/ kg of BOP 2 b after receiving PEITC by gavage at a dose of 0, 100 or 250 pmol/animal (0, 16.3 or 40.8 mg/animal). Six and 22 h after the BOP administration, hamsters were killed and tissues were sampled. Proliferating cell nuclear antigen immunohistochemistry demonstrated significant reduction (P
In this study, we investigated the sequential changes in the development of renal tubular cysts in newborn rats treated with p-cumylphenol (PCP). Fifteen animals per sex were treated orally with 300 mg/kg/day of PCP for up to 18 days from postnatal day (PND) 4 and were sacrificed on PNDs 8, 12, 19 and 22 and after a 7 day recovery period. On PNDs 8 and 12, slight dilatation of the collecting ducts was frequently observed in the medulla and slight papillary necrosis was also noted in some cases. These dilated collecting ducts were lined with slightly hyperplastic epithelial cells. On PNDs 19 and 22, multiple large cystic changes arising from the collecting ducts in the outer medulla were seen. These cystically dilated ducts were also lined with hyperplastic epithelial cells. During the dosing period, the labeling index of proliferating cell nuclear antigen in the collecting duct epithelium was higher in the PCP-treated group than in the control group at all time points. After a 7 day recovery period, the cystic change still remained, although the cell density was decreased and the epithelial cells became flattened. On the other hand, basophilic tubules with peritubular lymphoid cell infiltration were multifocally observed in the cortex. In conclusion, PCP induced multiple renal cysts that developed in the collecting ducts of the outer medulla in neonatal rats, and it is suggested that epithelial cell proliferation may play some roles in the induction of cystic lesions.
Biological background data up to 11 weeks of age and tumorigenic susceptibility to
xenotransplantation with HeLa cells were compared between severely immuno-deficient NOG
and NSG mice. The body weight was lower in NOG mice than in NSG mice. Severe depletion of
peripheral blood lymphocytes and lymphoid hypoplasia that are well-known characteristics
of these mice were equally observed. No lymphoproliferative lesions developed in any mouse
of either strain. The occurrence of ectopic exocrine gland and cyst was a common finding
in the thymus of both strains. In addition, minimal spongiotic change was observed in the
medulla oblongata and spinal cord in both strains, and its incidence in female NOG mice
was a little higher than that in NSG mice. In the adrenal, subcapsular cell hyperplasia
that is known as an age-related change in non-genetically modified mice developed earlier
and its incidence was higher in NSG mice than in NOG mice. The development of female
genital organs of NOG mice was slightly retarded in comparison with that of NSG mice. To
evaluate tumorigenic susceptibility to xenotransplantation, female mice were implanted in
the dorsal subcutis with 1×103 to 1×106 cells/head of HeLa cells,
and were checked up to 16 weeks after implantation. As a result, there was no significant
strain difference on tumor formation rate and tumor volume. In conclusion, the present
study clearly demonstrated that NOG and NSG mice showed no distinct strain differences in
either biological features or biological disadvantages.
-To obtain background data of NOD/Shi-scid IL-2Rγ null (NOG) mice, severely immunedeficient mice, a total of 120 animals were examined at 7, 26 and 52 weeks-old (20 mice/sex/group). The survival rate at 52 weeks-old was 95% (19/20) in both sexes. Clinically, circling behavior in one direction along the cage wall was observed in males after 8 weeks and females after 47 weeks-old, and hunchback position was found in males after 32 weeks-old. Hematologically, lymphocyte count markedly decreased at all ages, while white blood cell count increased in several mice at 52 weeks-old. Blood chemistry results revealed high values of aspartate aminotransferase, lactate dehydrogenase and creatine phosphokinase in some females at 26 weeks-old, without any related histological change. Histologically, lymphoid hypoplasia characterized by severe lymphocyte depletion with poorly developed tissue architectures was observed. In addition, spongiotic change in the nerve tissue was observed in both sexes at 7 and 26 weeks-old, and intracytoplasmic materials known as tubular aggregates in the skeletal muscles were found in males terminated at 26 and 52 weeks-old and in females at 52 weeks-old. Malignant lymphoma was found in one female euthanized at 20 weeks-old. Further, small intestinal adenoma, hepatocellular adenoma, leukemia, cerebral lipomatous hamartoma, Harderian gland adenoma and uterine polyp were also observed, and their incidences were low except for that of uterine polyp. This study provided detailed background data on NOG mice up to 52 weeks-old and provided information on appropriate use of NOG mice in the various research fields.
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