Abstract
Peripheral tolerance is essential for silencing weakly autoreactive B cells that have escaped central tolerance, but it is unclear why these potentially pathogenic B cells are retained rather than being eliminated entirely. Release from peripheral tolerance restraint can occur under certain circumstances (i.e., strong TLR stimulus), that are present during infection. In this regard, we hypothesized that autoreactive B cells could function as a reserve population that can be activated to contribute to the humoral immune response, particularly with pathogens, such as HIV-1, that exploit immune tolerance to avoid host defense. In this study, we identify a population of autoreactive B cells with the potential to neutralize HIV-1 and experimentally release them from the functional restrictions of peripheral tolerance. We have previously identified murine monoclonal antibodies that displayed autoreactivity against histone H2A and neutralized HIV-1 in vitro. Here, we identify additional H2A-reactive IgM monoclonal antibodies and demonstrate that they are both autoreactive and polyreactive with self and foreign antigens and are able to neutralize multiple clades of tier 2 HIV-1. Flow cytometric analysis of H2A-reactive B cells in naïve wildtype mice revealed that these B cells are present in peripheral B cell populations and we further document that murine H2A-reactive B cells are restrained by peripheral tolerance mechanisms. Specifically, we show endogenous H2A-reactive B cells display increased expression of the inhibitory mediators CD5 and phosphatase and tensin homolog (PTEN) phosphatase and fail to mobilize calcium upon immunoreceptor stimulation; all characterized markers of anergy. Moreover, we show that toll-like receptor stimulation or provision of CD4 T cell help induces the in vitro production of H2A-reactive antibodies, breaking tolerance. Thus, we have identified a novel poly/autoreactive B cell population that has the potential to neutralize HIV-1 but is silenced by immune tolerance.
Highlights
Immunological tolerance functions to remove or functionally silence autoreactive specificities from lymphocyte populations
We argue that many of these autoreactive B cells whose B cell receptor (BCR) display polyreactivity may be retained to increase the diversity of the primary B cell repertoire and enhance the detection of pathogen epitopes
We identify and characterize within a wild type, polyclonal repertoire of B cells a population of histone H2A-specific autoreactive B cells with potential to neutralize human immunodeficiency virus 1 (HIV-1) but that are silenced by immune tolerance
Summary
Immunological tolerance functions to remove or functionally silence autoreactive specificities from lymphocyte populations. 20–35% of the B cells exiting the bone marrow maintain some level of autoreactivity [2, 5] These cells migrate to secondary lymphoid organs where they are rendered tolerant by mechanisms of peripheral tolerance including exclusion from the B cell follicles, lack of T cell help, and induction of a functionally inert state known as anergy [6,7,8,9]. These autoreactive B cells are silenced by peripheral tolerance, the question remains— why retain a considerable frequency of potentially pathogenic B cells in the periphery? Do these autoreactive B cells serve a beneficial purpose in healthy individuals?
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