Journal
RADIATION RESEARCH
Volume 171, Issue 2, Pages 180-187Publisher
RADIATION RESEARCH SOC
DOI: 10.1667/RR1241.1
Keywords
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Funding
- Bhabha Atomic Research Centre, Government of India
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Shukla, J., Chatterjee, S., Thakur, V. S., Premachandran, S., Checker, R. and Poduval, T. B. L-Arginine Reverses Radiation-Induced Immune Dysfunction: The Need for Optimum Treatment Window. Radiat. Res. 171, 180-187 (2009). The aim of the present study was to investigate the protective efficacy of L-arginine in mitigating the injury induced by 2 Gy of total-body gamma radiation (TBI). Mice exposed to radiation (TBI group) had significantly decreased spleen weight, splenocyte numbers and bone marrow cellularity. Administration Of L-arginine 2 h after TBI (TBI + L-arginine group) was effective in reducing the radiation-induced depletion of spleen and bone marrow cellularity but was not effective when administered before TBI (L-arginine + TBI group). The radiation-induced decrease in Con A-induced spleen cell proliferation, specific antibody response of spleen B cells to sheep red blood cells, and spleen RNA content was reversed in mice in the TBI + L-arginine group. The radiation-induced increase in serum TNF-alpha levels, serum nitrate/nitrite (NOx) levels, spleen DNA fragmentation, spleen nitric oxide synthase (NOS) activity, spleen inducible NOS (iNOS) activity, and hepatic iNOS activity was reversed in mice in the TBI + L-arginine group. L-Arginine administered before TBI could not reverse these changes. Mice in the TBI + L-arginine group had significantly increased spleen arginase activity compared to mice from either the TBI or (L-arginine + TBI group). The results suggest the importance of the time of administration of L-arginine and the L-arginine pathway in mitigating the radiation-induced host immune dysfunction. (C) 2009 by Radiation Research Society
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