Journal of the Japan Society of Blood Transfusion
Online ISSN : 1883-8383
Print ISSN : 0546-1448
ISSN-L : 0546-1448
PREVENTION OF ALLOIMMUNIZATION BY ULTRAVIOLET-B IRRADIATION
INACTIVATION OF LEUKOCYTES AND THE GENERATION OF ACTIVE OXYGEN AND RADICALS
Tsuneo TakahashiJunichi AkasakaYuko MogiNaoki KamoMikinori KuwabaraSadayoshi Sekiguchi
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JOURNAL FREE ACCESS

1994 Volume 40 Issue 5 Pages 702-710

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Abstract

UV-B irradiation of platelet concentrates (PC) has been tried in several institutes to inactivate leukocytes in PC and prevent alloimmunization on platelet transfusion. However, the mechanism of inactivation of leukocytes contaminating PC has not been fully understood.
It is known that UV-B light is absorbed by photosensitizers in cells and produces active oxygen and radicals, such as singlet oxygen, superioxide anions and hydroxyl radicals. These active oxygen or radicals should injure cellular components and this could cause the suppression of cellular functions.
In this study, we investigated the relationships among UV-B irradiation, free radical generation and leukocyte inactivation. We found the evidence that active oxygen and radicals were produced in peripheral blood mononuclear cells by UV-B irradiation. UV-B irradiation suppressed the stimulatory function of leukocytes in a mixed lymphocyte reaction (MLR), and the suppression depended on the dosage of UV-B. Even a low dosage of UV-B, 10J/m2, could inhibit the MLR if the irradiated cells were incubated at 37°C for 24 hours before co-culture with responder cells. Treatments of cells with the exogenous singlet oxygen or superoxide anions also caused suppression of the stimulatory function in the MLR, inhibition of capping formation of HLA-DR antigens, and an increase of intracellular free Ca2+ levels as did the UV-B treatment.
These results indicate that the active oxygen or radicals generated in UV-B-irradiated leukocytes could be one of the causes of leukocyte inactivation.

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© The Japan Society of Transfusion Medicine and Cell Therapy
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