Adoptive Transfer of Antiviral Resistance by Lymphoid Cells from Mice Protected against Friend Leukemia Virus-induced Disease by Passive Serum Therapy1
نویسندگان
چکیده
Spleen and bone marrow cells from DBA/2 mice protected against infection with a leukemogenic dose of Friend leukemia virus (FLV) by passive therapy with chimpanzee anti-FLV serum were shown to be able to adoptively transfer antiviral resistance to unimmunized irradiated syngeneic recipients. Similar to the results obtained with donor mice immunized against a synge neic FLV erythroleukemia cell line, spleen cells from serumprotected donor mice were more effective in transferring anti viral resistance than were the corresponding bone marrow cells. In contrast to the previously demonstrated close corre lation between passive serum therapy protection and the de velopment of a host antiviral humoral response, adoptive cell transfer-mediated resistance to FLV challenge was not accom panied by the presence of detectable antiviral antibodies. While the cell type(s) responsible for transfer of antiviral resistance have not been conclusively identified, studies presented in this report indicate that elimination of T-cells by treatment with antiThy 1.2 antibodies plus complement does not affect the ability of spleen cells from serum-protected mice to adoptively trans fer antiviral resistance. Furthermore, the idea that mature Tcells do not play a critical role in the FLV serum protection mechanism is further supported by the fact that the serum therapy protocol operates effectively in nude athymic mice. In the course of the adoptive transfer studies, it was observed that sublethal irradiation of DBA/2 mice prevented the devel opment of FLV-induced splenomegaly (which reflects the activ ity of the defective spleen focus-forming virus component) without affecting the replication of the helper nondefective lymphatic leukemia virus. This irradiation effect could be re versed by reconstituting the mice with spleen or bone marrow cells from normal or FLV-infected syngeneic mice, suggesting that the irradiation effect is due to the inactivation of a spleen focus-forming virus target cell, presumably of an erythroid stem cell nature, which can be replaced by normal or leukemic spleen or bone marrow cells.
منابع مشابه
Adoptive transfer of antiviral resistance by lymphoid cells from mice protected against Friend leukemia virus-induced disease by passive serum therapy.
Spleen and bone marrow cells from DBA/2 mice protected against infection with a leukemogenic dose of Friend leukemia virus (FLV) by passive therapy with chimpanzee anti-FLV serum were shown to be able to adoptively transfer antiviral resistance to unimmunized irradiated syngeneic recipients. Similar to the results obtained with donor mice immunized against a synge neic FLV erythroleukemia cell ...
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Previous studies have demonstrated that spleen cells from DBA/2 mice protected against challenge with a leukemogenic dose of Friend leukemia virus (FLV) by passive administration of xenogeneic antiviral or anti-FLV Mr 71,000 viral envelope glycoprotein antisera can adoptively transfer antiviral resistance to unimmunized irradiated syngeneic recipients. In addition, elimination of T-cells by tre...
متن کاملUse of Adoptive Transfer and Winn Assay Procedures in the Further Analysis of Antiviral Acquired Immunity in Mice Protected against Friend Leukemia Virus-induced Disease by Passive Serum Therapy1
Previous studies have demonstrated that spleen cells from DBA/2 mice protected against challenge with a leukemogenic dose of Friend leukemia virus (FLV) by passive administration of xenogeneic antiviral or anti-FLV M, 71,000 viral envelope glycoprotein antisera can adoptively transfer antiviral resistance to unimmunized irradiated syngeneic recipients. In addition, elimi nation of T-cells by tr...
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