Dominant nonresponsiveness in the induction of autoimmunity to liver-specific F antigen.

Silver, Donald M.; Lane, David P.

doi:10.1084/jem.142.6.1455

Cited by 32 publications

(7 citation statements)

References 10 publications

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“…I t has previously been reported that BIO.A mice, in response to low doses of C3H liver extract, are also able to produce precipitating antibodies against a non-Fantigen component of liver, but when these sera were tested against the DBA/1 serum, lines of nonidentity were seen (Silver & Lane 1979). In this study, none of the DBA/1 mice responded to multiple immunizations with C3H liver extract ( + Mice were immunized on days 0 and 28 then weekly thereafter with the liver extract in CFA.Titer taken as the reciprocal of the highest dilution of serum that bound specifically 50% of the bindable F-antigen in the radioimmunoassay described by Silver & Lane (1975). Gel1 diffusion + refers to line of identity against control anti-F serum unless nonidentity is designated.…”

Section: Resultsmentioning

confidence: 72%

“…In a similar vein the question can be posed as to why only DBA/1 mice responded to this antigen when previous studies with F-antigen (Silver & Lane 1975) have involved cross immunizing a variety of inbred strains with liver extracts from every other strain without any anti-Ll being detected. The simplest explanation would be that all mice possess and are tolerant to this antigen except DBA/1 which lacks the antigen.…”

Section: Discussionmentioning

confidence: 99%

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Identification of an Antigen Shared by Mouse Liver and Lung

Silver

1979

Tissue Antigens

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In response to multiple injections of liver extract from Balb/c mice, DBA/1 mice produce antibodies against a component of the liver preparation which is not F‐antigen, but which is able to precipitate in gel diffusion tests. This antigen is also found in extracts of Balb/c lung, but not in a variety of other organs tested. Liver extracts from all of the inbred strains studied contain the antigen, except extracts from DBA/1 mice. Furthermore, this antigen was not found in the liver or lungs of other vertebrates tested. The antigen has been designated antigen‐L1.

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Section: Resultsmentioning

confidence: 72%

Section: Discussionmentioning

confidence: 99%

Identification of an Antigen Shared by Mouse Liver and Lung

Silver

1979

Tissue Antigens

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“…F antigen is a cytoplasmic water soluble liver-specific antigen which elicits an interesting immunological response in mice: thus immunization with allogeneic, but not autologous, liver leads to production of autoantibody to F antigen (anti-F-antibody). There are two isoforms of F antigen in the liver of mice (Silver & Lane 1975, Utzinger 1975 and inbred strains possessing one isoform will produce anti-F antibody in response to immunization with the other isoform from another strain, but do not respond to antigen from strains containing the same isoform (Silver & Lane 1975); however not all strains are responders to the alternate isoform. The response to F antigen is T cell dependent, and F antigen, as a hapten, may become associated with an alloantigen acting as a carrier moiety (Iverson & Lindenmann 1972).…”

mentioning

confidence: 99%

Localization of Genetic Control in Mice over Response to Liver‐Specific F Antigen

et al. 1978

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“…the F 1 immune response corresponds to that of the LR parent. 2,3 The pertinent genes were mapped to the H2A 4±6 or H2E loci, 7,8 but the role of H2 adjacent regions 9±11 and non-H2 genes 12 has also been reported.…”

Section: Introductionmentioning

confidence: 99%

Recessive expression of the H2A‐controlled immune response phenotype depends critically on antigen dose

et al. 2000

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SUMMARYMajor histocompatibility complex (MHC) alleles acting as immune response genes are coexpressed in heterozygous individuals and therefore control of immune responses is usually codominant. As an exception to this rule, however, several examples of recessive immune responses have been ascribed to regulatory, e.g. suppressive, interactions. We report here that the recessive phenotype of both antibody and T-cell responses to the mycobacterial 16 000-MW antigen depends critically on a low antigen dose for immunization. On the basis of similar responses in hemi-and heterozygous mice, we suggest that the mechanism of recessive MHC control does not involve regulation by the low-responder allele. We also demonstrated mixed haplotype restriction of peptide recognition for a signi®cant fraction of high-antigen-dose primed T cells. Their paucity under limiting antigen dose conditions may lead to the recessive expression of MHC control. In conclusion, our results suggest that recessive MHC control can be explained as a simple gene dosage effect under conditions where antigen is limiting, without a need for regulatory mechanisms.

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Dominant nonresponsiveness in the induction of autoimmunity to liver-specific F antigen.

Cited by 32 publications

References 10 publications

Identification of an Antigen Shared by Mouse Liver and Lung

Identification of an Antigen Shared by Mouse Liver and Lung

Localization of Genetic Control in Mice over Response to Liver‐Specific F Antigen

Recessive expression of the H2A‐controlled immune response phenotype depends critically on antigen dose

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