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Strain differences of cerebral ventricles in mice: Can the MRL/MpJ mouse be a model for hydrocephalus?
2009
Hino, K.(Hokkaido Univ., Sapporo (Japan)) | Otsuka, S. | Ichii, O. | Hashimoto, Y. | Kon, Y.
Hydrocephalus is an intractable disease characterized by the excessive accumulation of cerebrospinal fluid (CSF) in the cerebral ventricles. There are many cases in both human and animals; however, the cause and mechanism of its development is not clearly understood. In this study, differences of cerebral ventricles in 5 inbred mice strains (MRL/MpJ, C57BL/6, C3H/He, DBA/2 and BALB/c) were investigated by histological techniques to determine the possibility of a new animal model for hydrocephalus. Our analysis showed that significant differences in the volume and the surface area of lateral ventricles in the 5 inbred strains, with MRL/MpJ mice having the largest lateral, third, aqueduct and fourth ventricles. In addition, when MRL/MpJ mice were compared to BALB/c mice on 0 day after birth, the former already had larger lateral ventricles than the latter. Although there was no significant difference in the ratios of ependymal cell types in MRL/MpJ mice and BALB/c mice, the number and the diameter of lipid droplets in MRL/MpJ mice were, interestingly, smaller than those in BALB/c mice. It is well known that ependymal cells absorb nutritional substances in CSF by endocytosis, suggesting the possibility that their decrease may relate to the larger cerebral ventricles in MRL/MpJ. In conclusion, MRL/ MpJ mice have greater volumes in cerebral ventricles than other strains and may be useful for a model showing high susceptibility to hydrocephalus.
Mostrar más [+] Menos [-]Preliminary studies on the effects of orally-administered transforming growth factor-beta on protozoan diseases in mice
2009
Namangala, B.(Obihiro Univ. of Agriculture and Veterinary Medicine, Hokkaido (Japan)) | Inoue, N. | Sugimoto, C.
Transforming growth factor beta-1 (TGF-beta1) is a pleiotropic cytokine with both pro- and antiinflammatory properties, depending on its environment and concentration. The present study evaluated the effects of orally-delivered TGF-beta1 on mice parenterally-infected with various protozoan parasites. We report that while orally-administered TGF-beta1 seems to confer partial protection against murine chronic babesiosis and acute trypanosomosis, no beneficial clinical effects were observed against acute babesiosis, malaria or toxoplasmosis. Taken together, these preliminary data suggest that the systemic effects conferred by exogenous TGF-beta1 could be parasite species-specific. The variations in different parasitic infections could be due to (i) intrinsic differences between parasite species and/or strains in their ability to induce production of immunosuppressive molecules and/or (ii) differences in mechanisms governing host protection against different parasitic infections.
Mostrar más [+] Menos [-]Exon skipping of exonuclease 1 in MRL/MpJ mice is caused by a nucleotide substitution of the branchpoint sequence in intron eight
2004
Namiki, Y. (Hokkaido Univ., Sapporo (Japan)) | Kon, Y. | Sasaki, N. | Agui, T. | Endoh, D.
In MRJ/MpJ mice, there is a genetic mutation of exonuclease 1 (Exol), in which the exon 9 is sometimes deleted. In the present study, to check the gen-eration of the spliced exons, exon 8-intron 8-exon 9 (pCX/Ex/EIE/B and pCX/ Ex/EIE/M) plasmids were temporally transfected in vitro into BALB 3T3 cells, and RT-PCR using appropriate primer pair was carried out 1 day after transfection. In these constructions, pCX/Ex/EIE/B was derived from genomic sequence of C57BL/6 mice, and pCX/Ex/EIE/M was from MRL/MpJ. A spliced band was detected in pCX/Ex/EIE/B , but was present little or very weakly in pCX/Ex/EIE/M . Next, the same spliced band was demonstrated in pCX/Ex/EIE/M(T) plasmid, in which the branchpoint sequence (BPS) of pCX/Ex/EIE/M including the exon 9 was changed into that of pCX/Ex/EIE/B. The splicing did not occur in the del1/B mutant, in which 1960 nucleotides of the intron 8 were deleted, whereas it was detected in the del2/B plasmid deleted 1036 nucleotides in its middle region. These results suggest that the nucleotide T to A mutation of the BPS in the intron 8 is at least a sufficient for generation of splice variants (tr-l and tr-2 Exol).
Mostrar más [+] Menos [-]Passive immunization with monoclonal antibodies: Effects on Haemaphysalis longicornis tick infestation of BALB/c mice
2003
Nakajima, M. (Hokkaido Univ., Sapporo (Japan)) | Yanase, H. | Iwanaga, T. | Kodama, M. | Ohashi, K. | Onuma, M.
Taenia taeniaeformis larval product induces gastric mucosal hyperplasia in SCID mice
2002
Lagapa, J.T.G. (Hokkaido Univ., Sapporo (Japan)) | Oku, Y. | Nonaka, N. | Kamiya, M.
The effects of intraperitoneal implantation of Taenia taeniaeformis larvae and inoculation of in vitro larval products on gastric mucosa of SCID mice were investigated in this study. Mice surgically implanted with T, taeniaeformis larvae developed slight and moderate gastric hyperplasia. When in vitro cultured T. taeniaeformis larval excretory-secretory (TtLES) products containing 1 mg of protein were injected daily into mice, they caused gastropathy after 5-7 days. Mice injected daily with 0.5 mg of TtLES products also showed slight gastric hyperplasia after day 14 and 28. The gastropathy was characterized by reduction of both parietal and zymogenic cell number and increased number of alcian blue-periodic acid Schiff (AB-PAS)-positive cells and by two-fold extension of proliferative zone of gastric units. Larval implantation demonstrated a more potent effect in inducing gastropathy than did in vitro larval culture products. Significant decrease in number of parietal cells with con-comitant increase of tive zone and AB-PAS-positive cell number indicated their important roles in inducing the hyperplastic lesion. Similarities with other gastropathies indicated that there is a common fundamental regulatory mechanism involved, and that the host response may not be specific to parasites. Present study validated the induction of gastric mucosal hyperplasia by larval ES products of T. taeniaeformis. This proved the hypothesis of previous studies suggesting the role of larvae-derived products in inducing gastric mucosal hyperplasia in T. taeniaeformis-infected rats.
Mostrar más [+] Menos [-]Relationship among growth, steroid production and immunolocalization of transforming growth factor-beta1 in the normally developing mouse follicles cultured in vitro
2001
Bishonga, C. (Hokkaido Univ., Sapporo (Japan)) | Takahashi, Y. | Katagiri, S. | Nagano, M. | Ishikawa, A.
Protective effects of intranasal vaccination with plasmid encoding pseudorabies virus glycoprotein B in mice
1999
Takada, A. (Hokkaido Univ., Sapporo (Japan)) | Okazaki, K. | Kida, H.
Intranasal administration of plasmid DNA encoding glycoprotein B of pseudorabies virus into mice induced both serum and secretory antibody responses. These mice resisted intranasal challenge with lethal dose of the virus, but did not intraperitoneal challenge. On the other hand, intramuscular injection of the plasmid induced less secretory and higher serum antibody responses than those of intranasally vaccinated mice. None of them was protected from virus challenge. The present results suggest that administration of plasmid DNA encoding glycoprotein B by respiratory mucosal route generates local secretory antibodies which serve to protect animals from pseudorabies virus infection
Mostrar más [+] Menos [-]Development of single blastomeres from 4-cell stage embryos after aggregation with parthenogenones in mice
1994
Pinyopummin, A. (Hokkaido Univ., Sapporo (Japan). Faculty of Veterinary Medicine) | Takahashi, Y. | Hishinuma, M. | Kanagawa, H.
Effects of various cryoprotectants on the survival of mouse embryos cryopreserved by the quick freezing method
1989
Mazni, O.A. (Yokohama Univ. (Japan). Faculty of Engineering) | Takahashi, Y. | Valdez, C.A. | Nishinuma, M. | Kanagawa, H.
Effect of phytosin on mouse embryo survival after short-term storage
1987
Valdez, C.A. (Hokkaido Univ., Sapporo (Japan). Faculty of Veterinary Medicine) | Mazni, O.A. | Kanagawa, H.