In Vivo Characterization and Therapeutic Efficacy of a C5-specific Inhibitor from the Soft Tick Ornithodoros moubata

Hepburn, Natalie J.; Williams, Anwen Siân; Nunn, Miles A.; Chamberlain-Banoub, Jayne C.; Hamer, John; Morgan, B. Paul; Harris, Claire L.

doi:10.1074/jbc.m609858200

Cited by 78 publications

(88 citation statements)

References 29 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…3E). OmCI (0.6 μM; gift from Varleigh, London, United Kingdom) was used to block terminal pathway activation as described previously (29,49). ShEA-C3b cells were resuspended in AP buffer at 2% (vol/vol).…”

Section: Methodsmentioning

confidence: 99%

Common polymorphisms in C3, factor B, and factor H collaborate to determine systemic complement activity and disease risk

Heurich

Martı́nez-Barricarte

Francis

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

198

180

View full text Add to dashboard Cite

show abstract

Section: Methodsmentioning

confidence: 99%

Common polymorphisms in C3, factor B, and factor H collaborate to determine systemic complement activity and disease risk

Heurich

Martı́nez-Barricarte

Francis

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

198

180

View full text Add to dashboard Cite

show abstract

“…Investigations have included studies on anti‐tumoral effects (Chudzinski‐Tavassi et al ., 2010; Abreu et al ., 2014; Sousa et al ., 2015), applications against inflammatory diseases like myasthenia gravis (Hepburn et al ., 2007), new anticoagulants (Koh et al ., 2011) and the treatment of asthma (Horka et al ., 2012). …”

Section: Tick Saliva As a Source Of Toxins Tick‐borne Pathogens And mentioning

confidence: 99%

Tick attachment cement – reviewing the mysteries of a biological skin plug system

et al. 2017

View full text Add to dashboard Cite

The majority of ticks in the family Ixodidae secrete a substance anchoring their mouthparts to the host skin. This substance is termed cement. It has adhesive properties and seals the lesion during feeding. The particular chemical composition and the curing process of the cement are unclear. This review summarizes the literature, starting with a historical overview, briefly introducing the different hypotheses on the origin of the adhesive and how the tick salivary glands have been identified as its source. Details on the sequence of cement deposition, the curing process and detachment are provided. Other possible functions of the cement, such as protection from the host immune system and antimicrobial properties, are presented. Histochemical and ultrastructural data of the intracellular granules in the salivary gland cells, as well as the secreted cement, suggest that proteins constitute the main material, with biochemical data revealing glycine to be the dominant amino acid. Applied methods and their restrictions are discussed. Tick cement is compared with adhesives of other animals such as barnacles, mussels and sea urchins. Finally, we address the potential of tick cement for the field of biomaterial research and in particular for medical applications in future.

show abstract

“…For rat and pig sera, rabbit erythrocytes in AP buffer were used and the serum doses selected (just sufficient to cause 100% lysis) were 7.5% (rat) and 10% (pig). For mouse serum, Ab-sensitized rabbit erythrocytes in CP buffer were used as described (20) with a selected serum dose of 4%. Dose of mAb was varied as described.…”

Section: Hemolysis Assaysmentioning

confidence: 99%

A Novel Antibody against Human Factor B that Blocks Formation of the C3bB Proconvertase and Inhibits Complement Activation in Disease Models

Subias

Tortajada

Gastoldi

et al. 2014

The Journal of Immunology

Self Cite

View full text Add to dashboard Cite

The alternative pathway (AP) is critical for the efficient activation of complement regardless of the trigger. It is also a major player in pathogenesis, as illustrated by the long list of diseases in which AP activation contributes to pathology. Its relevance to human disease is further emphasized by the high prevalence of pathogenic inherited defects and acquired autoantibodies disrupting components and regulators of the AP C3-convertase. Because pharmacological downmodulation of the AP emerges as a broad-spectrum treatment alternative, there is a powerful interest in developing new molecules to block formation and/or activity of the AP C3-convertase. In this paper, we describe the generation of a novel mAb targeting human factor B (FB). mAb FB48.4.2, recognizing with high affinity an evolutionary-conserved epitope in the Ba fragment of FB, very efficiently inhibited formation of the AP C3-proconvertase by blocking the interaction between FB and C3b. In vitro assays using rabbit and sheep erythrocytes demonstrated that FB28.4.2 was a potent AP inhibitor that blocked complement-mediated hemolysis in several species. Using ex vivo models of disease we demonstrated that FB28.4.2 protected paroxysmal nocturnal hemoglobinuria erythrocytes from complement-mediated hemolysis and inhibited both C3 fragment and C5b-9 deposition on ADP-activated HMEC-1 cells, an experimental model for atypical hemolytic uremic syndrome. Moreover, i.v. injection of FB28.4.2 in rats blocked complement activation in rat serum and prevented the passive induction of experimental autoimmune Myasthenia gravis. As a whole, these data demonstrate the potential value of FB28.4.2 for the treatment of disorders associated with AP complement dysregulation in man and animal models.

show abstract

In Vivo Characterization and Therapeutic Efficacy of a C5-specific Inhibitor from the Soft Tick Ornithodoros moubata

Cited by 78 publications

References 29 publications

Common polymorphisms in C3, factor B, and factor H collaborate to determine systemic complement activity and disease risk

Common polymorphisms in C3, factor B, and factor H collaborate to determine systemic complement activity and disease risk

Tick attachment cement – reviewing the mysteries of a biological skin plug system

A Novel Antibody against Human Factor B that Blocks Formation of the C3bB Proconvertase and Inhibits Complement Activation in Disease Models

Contact Info

Product

Resources

About