Immunity to Babesia in mice I. Adoptive transfer of immunity to Babesia rodhaini with immune spleen cells and the effect of irradiation on the protection of immune mice
Publication date
1984
Authors
Kuil, H.
Zivkovic, D.
Seinen, W.
Albers-van Bemmel, C.M.G.
Speksnijder, J.E.
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Document Type
Article
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Abstract
Immunisation of Balb/c mice against Babesia rodhaini by an amicarbalide-
controlled infection resulted in a solid immunity which
lasted for 216 days. With spleen cells of immune mice protection
could be transferred both to naive mice pretreated with cyclophosphamide.
Treatment of naive mice with cyclophosphamide (300 mg/kg)
five days before a lethal B.rodhaini inoculation resulted in over
50% survival. This protective effect of cyclophosphamide is explained
by its inhibiting effect on suppressor T-cells.
The protection against B.rodhaini challenge infection afforded
to immune Balb/c mice was completely resistant to a sublethal irradiation
of 400 tad. Since B-lymphocyte function in antibody production
is suppressed by this dose, the role of antibodies in the
effector phase of the immunity appears to be of minor if any importance.
A considerable degree of protection was still preserved after
irradiation of immune animals with 875 rad. Sensitivity to this
irradiation dose of all immunocompetent cells except macrophages
and a small fraction of T-lymphocytes indicates the involvement
of these cell types in the effector phase of the specific immunity.
Highly radioresistant macrophages are therefore considered to play
the major role but T-lymphocytes are also required for complete
protection.