Immunological disease induced by injecting F1 lymphoid cells into certain parental strains.

1 December 1974

journal article

Vol. 27 (6) , 989-1007

Abstract

Injection of neonatal Balb/c or C57Bl/6 mice with C57Bl/6 x Balb/c)F1 lymphoid cells leads to transient chimerism and runting, and to splenomegaly, deficient T-cell function and a gradual replacement of lymphoid organs with abnormal reticular cells. Activated MuLV can be isolated from such mice. It is proposed that either graft-versus-host or host-versus-graft allogeneic reactivity activates endogenous MuLV virus, which then causes functional and morphological abnormalities in the lymphoid organs.

This publication has 19 references indexed in Scilit:

TUMOR INDUCTION BY IMMUNOLOGICALLY ACTIVATED MURINE LEUKEMIA VIRUS
The Journal of Experimental Medicine, 1973
Transient Appearance of PHA-Reactive Thymocytes in the Foetal Mouse
Nature New Biology, 1973
GENETIC FACTORS INFLUENCING C-TYPE RNA VIRUS INDUCTION
The Journal of Experimental Medicine, 1972
Life‐long tolerance and chimerism in parental mice induced with F₁ hybrid cells
European Journal of Immunology, 1971
Leukemia Virus Activation in Chronic Allogeneic Disease
Proceedings of the National Academy of Sciences, 1970
Plaque assay techniques for murine leukemia viruses
Virology, 1970
SYNERGY AMONG LYMPHOID CELLS MEDIATING THE GRAFT-VERSUS-HOST RESPONSE
The Journal of Experimental Medicine, 1970
F1 Hybrid Animals: Reactivity Against Recognition Structures of Parental Strain Lymphoid Cells
Pathobiology, 1969
IMMUNIZATION OF DISSOCIATED SPLEEN CELL CULTURES FROM NORMAL MICE
The Journal of Experimental Medicine, 1967
Malignant Lymphomas Following Allogenic Disease: Transition from an Immunological to a Neoplastic Disorder
Science, 1965