Humoral autoimmunity as a mediator of CNS repair.

A. J. Bieber; A. Warrington; L. R. Pease; M. Rodriguez

doi:10.1016/s0166-2236(00)01991-3

Humoral autoimmunity as a mediator of CNS repair.

A. J. Bieber, A. Warrington, L. R. Pease, M. Rodriguez

Research output: Contribution to journal › Review article › peer-review

52 Scopus citations

Abstract

Autoimmune responses directed against the central nervous system (CNS) have generally been considered pathogenic in nature. Although there are several well understood conditions in which this is the case, there is also a growing body of experimental evidence to show that both the cellular and humoral immune responses can promote tissue repair following CNS injury and disease. Our laboratory has used a mouse model of chronic demyelinating disease to characterize a class of polyreactive IgM autoantibodies that react with oligodendrocyte surface antigens and promote myelin repair. By screening a large number of human monoclonal antibodies, we have found that IgM antibodies that react with CNS tissue are relatively common. Autoreactive IgM antibodies might constitute an endogenous system for tissue repair, and therefore these antibodies could be of value as therapeutic reagents.

Original language	English (US)
Pages (from-to)	S39-44
Journal	Trends in neurosciences
Volume	24
Issue number	11 Suppl
DOIs	https://doi.org/10.1016/s0166-2236(00)01991-3
State	Published - Nov 2001

ASJC Scopus subject areas

General Neuroscience

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10.1016/s0166-2236(00)01991-3

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title = "Humoral autoimmunity as a mediator of CNS repair.",

abstract = "Autoimmune responses directed against the central nervous system (CNS) have generally been considered pathogenic in nature. Although there are several well understood conditions in which this is the case, there is also a growing body of experimental evidence to show that both the cellular and humoral immune responses can promote tissue repair following CNS injury and disease. Our laboratory has used a mouse model of chronic demyelinating disease to characterize a class of polyreactive IgM autoantibodies that react with oligodendrocyte surface antigens and promote myelin repair. By screening a large number of human monoclonal antibodies, we have found that IgM antibodies that react with CNS tissue are relatively common. Autoreactive IgM antibodies might constitute an endogenous system for tissue repair, and therefore these antibodies could be of value as therapeutic reagents.",

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AU - Warrington, A.

AU - Pease, L. R.

AU - Rodriguez, M.

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AB - Autoimmune responses directed against the central nervous system (CNS) have generally been considered pathogenic in nature. Although there are several well understood conditions in which this is the case, there is also a growing body of experimental evidence to show that both the cellular and humoral immune responses can promote tissue repair following CNS injury and disease. Our laboratory has used a mouse model of chronic demyelinating disease to characterize a class of polyreactive IgM autoantibodies that react with oligodendrocyte surface antigens and promote myelin repair. By screening a large number of human monoclonal antibodies, we have found that IgM antibodies that react with CNS tissue are relatively common. Autoreactive IgM antibodies might constitute an endogenous system for tissue repair, and therefore these antibodies could be of value as therapeutic reagents.

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Humoral autoimmunity as a mediator of CNS repair.

Abstract

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