Mice Deficient in Complement Receptors 1 and 2 Lack a Tissue Injury-Inducing Subset of the Natural Antibody Repertoire

Fleming, Sherry D.; Shea‐Donohue, Terez; Guthridge, Joel M.; Kulik, Liudmila; Waldschmidt, Thomas J.; Gipson, Matthew G.; Tsokos, George C.; Holers, V. Michael

doi:10.4049/jimmunol.169.4.2126

Cited by 167 publications

(169 citation statements)

References 59 publications

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“…Of interest, transferred IgM and IgG each contributed to different aspects of tissue injury but together allowed the development of a complete injury phenotype (6). These findings demonstrated a previously unrecognized role for complement receptors in the development within the natural antibody repertoire of a tissue injury-inducing subset of antibodies.…”

Section: Complement In Tissue Injurymentioning

confidence: 79%

“…The exact mechanism of complement activation during intestinal IR remains unclear as there is evidence that more than one complement pathway (classical, alternative or lectin) may become activated and enhance tissue injury (1,5,6). However, two observations have strongly implicated the classical pathway in this process.…”

Section: Complement In Tissue Injurymentioning

confidence: 99%

“…CR2-/-mice demonstrate a substantial defect in the generation of IgG switched isotype responses (12, 13) as well as impaired B cell memory following immunization with T-dependent antigens (13,14). To determine if CR2 plays a role in mesenteric IR, Cr2-/-mice were subjected to intestinal IR injury and were shown to be protected from the induction of tissue injury (6). Because the levels of complement molecules and complement activation are normal in Cr2-/-mice, other factors were considered to be responsible for this protection.…”

Section: Complement In Tissue Injurymentioning

confidence: 99%

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Complement, natural antibodies, autoantibodies and tissue injury

Fleming

Tsokos

2006

Autoimmunity Reviews

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Activation of the classical complement pathway represents an effector mechanism of intestinal ischemia/reperfusion injury. Mice deficient in complement receptors 1 and 2 fail to produce a component of the natural antibody repertoire that binds to ischemiaconditioned tissues and activate complement. In contrast, mice prone to autoimmunity display accelerated and enhanced tissue injury that results from the binding of autoantibodies to injured tissues. Our experiments demonstrate that naturally occurring antibodies and autoantibodies mediate tissue injury only after an organ has been subjected to a stressor such as ischemia.

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Section: Complement In Tissue Injurymentioning

confidence: 79%

Section: Complement In Tissue Injurymentioning

confidence: 99%

Section: Complement In Tissue Injurymentioning

confidence: 99%

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Complement, natural antibodies, autoantibodies and tissue injury

Fleming

Tsokos

2006

Autoimmunity Reviews

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“…The major function of complement traditionally has been thought to be recognition and elimination of pathogens through direct killing (3) and/or stimulation of phagocytosis (4,5). However, over the last decade the complement system has also been shown to play central immunoregulatory roles such as enhancing humoral immunity (6), modifying T cell immunity (7), shaping the development of the natural Ab repertoire (8), and regulating tolerance to nuclear self Ags such as DNA and chromatin (9,10). In addition to its immunoregulatory functions, many studies have also elaborated on the pathogenic role of complement during ischemic, inflammatory, and autoimmune diseases (reviewed in Ref.…”

Section: Overview Of Complement and Its Biologic Rolesmentioning

confidence: 99%

The Central Role of the Alternative Complement Pathway in Human Disease

Thurman

Holers

2006

The Journal of Immunology

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389

350

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The complement system is increasingly recognized as important in the pathogenesis of tissue injury in vivo following immune, ischemic, or infectious insults. Within the complement system, three pathways are capable of initiating the processes that result in C3 activation: classical, alternative, and lectin. Although the roles that proinflammatory peptides and complexes generated during complement activation play in mediating disease processes have been studied extensively, the relative contributions of the three activating pathways is less well understood. Herein we examine recent evidence that the alternative complement pathway plays a key and, in most instances, obligate role in generating proinflammatory complement activation products in vivo. In addition, we discuss new concepts regarding the mechanisms by which the alternative pathway is activated in vivo, as recent clinical findings and experimental results have provided evidence that continuous active control of this pathway is necessary to prevent unintended targeting and injury to self tissues.

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“…The mechanism of activation in the latter condition involves natural Abs (3,4) as well as the acute phase protein C-reactive protein (CRP) 4 (5-7). These molecules bind to newly exposed epitopes or ligands present on ischemic and/or apoptotic cells (8 -10).…”

mentioning

confidence: 99%

Evidence That Complement Protein C1q Interacts with C-Reactive Protein through Its Globular Head Region

McGrath

Brouwer

Arlaud

et al. 2006

The Journal of Immunology

118

101

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C1q acts as the recognition unit of the first complement component, C1, and binds to immunoglobulins IgG and IgM, as well as to non-Ig ligands, such as C-reactive protein (CRP). IgG and IgM are recognized via the globular head regions of C1q (C1qGR), whereas CRP has been postulated to interact with the collagen-like region (C1qCLR). In the present study, we used a series of nine mAbs to C1q, five directed against C1qGR and four against C1qCLR, to inhibit the interaction of C1q with CRP. The F(ab′)2 of each of the five mAbs directed against C1qGR inhibited binding of C1q to polymerized IgG. These five mAbs also successfully inhibited the interaction of C1q with CRP. Moreover, these five mAbs inhibited C1 activation by CRP as well as by polymerized IgG in vitro. In contrast, none of the four mAbs against C1qCLR inhibited C1q interaction with CRP or IgG, or could reduce activation of complement by CRP or polymerized IgG. These results provide the first evidence that the interaction of C1q with CRP or IgG involves sites located in the C1qGR, whereas sites in the CLR do not seem to be involved in the physiological interaction of C1q with CRP.

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Mice Deficient in Complement Receptors 1 and 2 Lack a Tissue Injury-Inducing Subset of the Natural Antibody Repertoire

Cited by 167 publications

References 59 publications

Complement, natural antibodies, autoantibodies and tissue injury

Complement, natural antibodies, autoantibodies and tissue injury

The Central Role of the Alternative Complement Pathway in Human Disease

Evidence That Complement Protein C1q Interacts with C-Reactive Protein through Its Globular Head Region

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