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MOUSE POPLITEAL LYMPH NODE ASSAY FOR ASSESSMENT OF ALLERGIC AND AUTOIMMUNITY-INDUCING POTENTIALS OF LOW-MOLECULAR-WEIGHT DRUGS

In the present collaborative study, popliteal lymph node (PLN) responses to penicillin G (an allergenic chemical), D-penicillamine (an autoimmunity-inducing chemical), and barbital (a negative reference chemical) were investigated in three different mouse strains by ten pharmaceutical companies. Two...

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Published in:Journal of toxicological sciences 1999/05/10, Vol.24(2), pp.95-102
Main Authors: SHINKAI, Kenkichi, NAKAMURA, Kazuichi, TSUTSUI, Naohisa, KUNINISHI, Yoshiharu, WAKI, Yoshinobu, NISHIDA, Hitoshi, SUZUKI, Ritsuyoshi, VOHR, Hans-Wemer, TAKAHASHI, Miharu, TAKAHASHI, Kenji, KAMIMURA, Yasuhiro, MAKI, Eiji
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Language:English
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Summary:In the present collaborative study, popliteal lymph node (PLN) responses to penicillin G (an allergenic chemical), D-penicillamine (an autoimmunity-inducing chemical), and barbital (a negative reference chemical) were investigated in three different mouse strains by ten pharmaceutical companies. Two inbred mouse strains (BALB/c and A/J) and one outbred strain (ICR) were subcutaneously injected with saline solutions containing penicillin G (1.25, 2.5 and 5 mg/mouse), D-penicillamine (0.5, 1 and 2 mg/mouse), or barbital (2 mg/mouse) into one hind footpad and saline only was injected into the contralateral footpad. PLN cellularity indices were determined on day 7. In the three strains tested, the penicillin G and D-penicillamine injections resulted in approximately dose-dependent responses. In contrast, barbital failed to generate a significant PLN reaction. In the typical data from one of the participating laboratories, the PLN responses of A/J, BALB/c, and ICR to penicillin G were high, intermediate and low, respectively, while their PLN responses to D-penicillamine were all high. Some variation in PLN cellularity indices was observed among the participating laboratories, but reproducibility of the popliteal lymph node assay (PLNA) evaluation was partly confirmed. Although the appropriate selection of mouse strains and drug dosage levels has to be considered, these results suggest that the PLNA may be an appropriate screening system for prediction of the allergic or autoimmunity-inducing potentials of low-molecular-weight drugs.
ISSN:0388-1350
1880-3989
DOI:10.2131/jts.24.95