Noriaki Kamikaidou scite author profile

Noriaki Kamikaidou

5Publications

32Citation Statements Received

19Citation Statements Given

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Affiliations

Nara Medical University

Publications

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Contribution of interferon γ and membrane-associated interleukin 1 to the resistance to murine typhoid of Ityr mice

Kita

Emoto

Oku

et al. 1992

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Resistance of mice to Salmonella typhimurium in the early phase of infection is known to be controlled by the expression of chromosome 1 locus Ity. To clarify the mechanism by which the genetically resistant (Ityr) mice can overcome the first phase of salmonellosis, the early response in DBA/2 (Ityr) and BALB/c (Itys) mice was compared after a subcutaneous injection of S. typhimurium. In both strains, the growth of S. typhimurium was controlled in livers and Kupffer cells until day 3, but thereafter the bacteria multiplied rapidly in BALB/c mice. Over the first 2 days nonspecific responses (changes in levels of blood leukocytes, plasma iron, and alpha 1-antitrypsin) were not significantly different between the strains, and the capacity of Kupffer cells isolated from infected mice of both strains to produce interleukin 1 (IL-1) and tumor necrosis factor alpha (TNF-alpha) was of the same degree. Thereafter, only DBA/2 Kupffer cells were able to produce membrane-associated IL-1 (ma IL-1) as well as TNF-alpha. Moreover, only DBA/2 splenocytes were able to produce interferon gamma (IFN-gamma) upon stimulation with Salmonella antigens, although concanavalin A-stimulated splenocytes of both strains produced the same level of interleukin 2. Furthermore, administration of recombinant murine IFN-gamma and DBA/2 Kupffer cells of day 6 to BALB/c mice 3 days after infection resulted in a significant level of protection, whereas neither of these materials alone induced protection. Injection of anti-TNF-alpha antibodies did not affect the resistance of DBA/2 mice. Thus, these findings suggest that the early resistance of Ityr mice is partly attributable to their capacity to produce IFN-gamma and ma IL-1 after infection.

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Mononuclear cell response in the liver of mice infected with hepatotoxigenic Campylobacter jejuni

Kita

Nishikawa²,

Kamikaidou³

et al. 1992

Journal of Medical Microbiology

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Mechanism of the protective immunity against murine typhoid: persistence of salmonella L forms in the liver after immunization with live-cell vaccines

Kita

Nishikawa

Kamikaidou

et al. 1992

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Live‐cell vaccines of Salmonella typhimurium, either a sub‐lethal dose of a wild‐type (strain LT2) or a high dose of its two‐heptose Rd1 mutant (strain SL1004), induced acquired resistance to murine typhoid, which remained 180 days after immunozation. Growth of S. typhimurium as a bacillary form ceased between days 30 and 60 of immunization, but L forms of this bacterium colonized the liver (the mean number of L forms in the liver: 600 L‐forming units) even at 180 days post‐immunization. In contrast, a high inoculum of either a Ra mutant (strain TV148) of strain LT2 or S. schottmülleri 8006 sharing the same O antigenic components with those of S. typhimurium induced only a short‐lived protection in proportion to the number of L forms in the liver, and the protective immunity was lost before day 180. However, there was no significant difference in the salmonella‐specific T‐cell responses among groups of immunized mice on day 180 of immunization. A lethal infection with strain LT2 in mice which had been immunized 75 days previously with living cells of strain SL1004 resulted in a rapid clearance of the challenge inoculum, together with a rapid elevation of anti‐S. typhimurium antibody responses. Thus, the present data suggest that the long‐lived immunity conferred upon live S. typhimurium vaccines is attributable to the colonization of this bacterium in the liver as L forms and the ability to colonize the liver as L forms is independent of the brain length of salmonella O‐antigens.

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Liposarcoma of the cheek: Report of a case

Kamikaidou¹,

Kirita²,

Mishima³

et al. 1998

Journal of Oral and Maxillofacial Surgery

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Clinical study of oral manifestations in patients with HIV infection. Relationship of clinical stage based on CD 4+ cell counts with oral manifestations.

Kamikaidou

Morimoto

Yamamoto

et al. 1998

Jpn. J. Oral Maxillofac. Surg.

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