Naseem Mushtaq scite author profile

In this study we have shown that activation of arthritogenic splenocytes with antigen and agonistic anti-CD40 gives raise to a B cell population that produce high levels of interleukin (IL)-10 and low levels of interferon (IFN)-γ. Transfer of these B cells into DBA/1-TcR-β-Tg mice, immunized with bovine collagen (CII) emulsified in complete Freund's adjuvant inhibited T helper type 1 differentiation, prevented arthritis development, and was also effective in ameliorating established disease. IL-10 is essential for the regulatory function of this subset of B cells, as the B cells population isolated from IL-10 knockout mice failed to mediate this protective function. Furthermore, B cells isolated from arthritogenic splenocytes treated in vitro with anti–IL-10/anti–IL-10R were unable to protect recipient mice from developing arthritis. Our results suggest a new role of a subset of B cells in controlling T cell differentiation and autoimmune disorders.

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Prevention and Cure of Systemic Escherichia coli K1 Infection by Modification of the Bacterial Phenotype

Mushtaq¹,

Redpath²,

Luzio

et al. 2004

Antimicrob Agents Chemother

102

121

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Escherichia coli is a common cause of meningitis and sepsis in the newborn infant, and the large majority of isolates from these infections produce a polysialic acid (PSA) capsular polysaccharide, the K1 antigen, that protects the bacterial cell from immune attack. We determined whether a capsule-depolymerizing enzyme, by removing this protective barrier, could alter the outcome of systemic infection in an animal model. Bacteriophage-derived endosialidase E (endoE) selectively degrades the PSA capsule on the surface of E. coli K1 strains. Intraperitoneal administration of small quantities of recombinant endoE (20 g) to 3-day-old rats, colonized with a virulent strain of K1, prevented bacteremia and death from systemic infection. The enzyme had no effect on the viability of E. coli strains but sensitized strains expressing PSA to killing by the complement system. This study demonstrates the potential therapeutic efficacy of agents that cure infections by modification of the bacterial phenotype rather than by killing or inhibition of growth of the pathogen.

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Cigarette smoke and platelet-activating factor receptor dependent adhesion ofStreptococcus pneumoniaeto lower airway cells

Grigg

Walters

Sohal

et al. 2012

Thorax

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Treatment of experimental Escherichia coli infection with recombinant bacteriophage-derived capsule depolymerase

Mushtaq¹,

Redpath²,

Luzio³

et al. 2005

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A small single dose of capsule-depolymerizing enzyme has therapeutic utility in lethal systemic infection in a non-invasive model that has characteristics of the infectious process in humans. We propose that the enzyme reduces the virulence of E. coli K1 by rapid removal of the protective capsular polysaccharide, sensitizing the pathogen to host defences such as phagocytosis by macrophages. Thus, whilst endoE-mediated therapy may not be a viable approach to the treatment of systemic infection in humans, it does support the concept that alteration of the cell wall phenotype is a valid therapeutic strategy.

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Adhesion of Streptococcus pneumoniae to human airway epithelial cells exposed to urban particulate matter

Mushtaq

Ezzati

Hall

et al. 2011

Journal of Allergy and Clinical Immunology

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Naseem Mushtaq

Prevention of Arthritis by Interleukin 10–producing B Cells

Prevention and Cure of Systemic Escherichia coli K1 Infection by Modification of the Bacterial Phenotype

Cigarette smoke and platelet-activating factor receptor dependent adhesion ofStreptococcus pneumoniaeto lower airway cells

Treatment of experimental Escherichia coli infection with recombinant bacteriophage-derived capsule depolymerase

Adhesion of Streptococcus pneumoniae to human airway epithelial cells exposed to urban particulate matter

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