Chronic suppression of immunoglobulin allotype production in adult congenic mice

Abstract

MOUSE allotypes refer to the inheritance of antigenic differences on the constant region of immunoglobulin (Ig) heavy chains (C_H). As such, allotypes are used as genetic markers to distinguish allelic C_H genes, the expression of which is codominant in heterozygous mice^1,2. The expression of a paternal C^H gene, however, can be suppressed in heterozygote offspring if the mother has previously been made immune to the allotype encoded by the paternal gene³. Neonatally induced suppression of this sort is known to lead to (or result in) the generation of allotype-specific suppressor T lymphocytes which directly or indirectly prevent allotype production by B lymphocytes^4–6. In contrast to this we have shown that allotype suppression can also be initiated in adult mice, that is in BALB/c mice that are congenic for the C57BL allotype (C.B-17 mice)¹. When X-irradiated C.B-17 mice (550 r.) are injected with thymocytes from BALB/c donors immune to the C57BL allotype, IgG_2a allotype production in the C.B-17 recipients becomes chronically suppressed⁷. We now report that allotype suppression in C.B-17 mice is mediated by T cells; that production of only the IgG_2a class allotype (G²) is suppressed, presumably as a result of direct interaction between specific T and B cells, and that the capacity of spleen cells to suppress host allotype production can be transferred serially from one C.B-17 mouse to another and as yet without obvious limit.