Statins protect against fulminant pneumococcal infection and cytolysin toxicity in a mouse model of sickle cell disease
Jason W. Rosch, … , Carlos J. Orihuela, Elaine I. Tuomanen
Jason W. Rosch, … , Carlos J. Orihuela, Elaine I. Tuomanen
Published January 19, 2010
Citation Information: J Clin Invest. 2010;120(2):627-635. https://doi.org/10.1172/JCI39843.
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Statins protect against fulminant pneumococcal infection and cytolysin toxicity in a mouse model of sickle cell disease

Abstract

Sickle cell disease (SCD) is characterized by intravascular hemolysis and inflammation coupled to a 400-fold greater incidence of invasive pneumococcal infection resulting in fulminant, lethal pneumococcal sepsis. Mechanistically, invasive infection is facilitated by a proinflammatory state that enhances receptor-mediated endocytosis of pneumococci into epithelial and endothelial cells. As statins reduce chronic inflammation, in addition to their serum cholesterol-lowering effects, we hypothesized that statin therapy might improve the outcome of pneumococcal infection in SCD. In this study, we tested this hypothesis in an experimental SCD mouse model and found that statin therapy prolonged survival following pneumococcal challenge. The protective effect resulted in part from decreased platelet-activating factor receptor expression on endothelia and epithelia, which led to reduced bacterial invasion. An additional protective effect resulted from inhibition of host cell lysis by pneumococcal cholesterol-dependent cytotoxins (CDCs), including pneumolysin. We conclude therefore that statins may be of prophylactic benefit against invasive pneumococcal disease in patients with SCD and, more broadly, in settings of bacterial pathogenesis driven by receptor-mediated endocytosis and the CDC class of toxins produced by Gram-positive invasive bacteria.

Authors

Jason W. Rosch, Angela R. Boyd, Ernesto Hinojosa, Tamara Pestina, Yunming Hu, Derek A. Persons, Carlos J. Orihuela, Elaine I. Tuomanen

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Figure 3

Effect of statin treatment on TNF-α–induced upregulation of PAFr on endothelial cells in vitro.

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Effect of statin treatment on TNF-α–induced upregulation of PAFr on endo...
(A) Immunohistochemical detection (purple) of PAFr expression on HBMECs activated with TNF-α with or without simvastatin. Original magnification, ×200. (B) Relative bacterial adhesion to activated HBMECs with or without pretreatment with simvastatin, and reversal by mevalonate. *P < 0.01 versus no treatment; P < 0.01 versus statin; P < 0.01 versus TNF plus statin. Error bars represent SD. (C) Detection of PAFr by Western blot analysis in activated HBMEC lysates and infected lung homogenates of SCD mice with or without simvastatin treatment. β-Actin served as the loading control. (D) Uninfected lung sections of SCD (with or without simvastatin), WT, and SCD Ptafr–/– mice showing bronchial epithelium stained for PAFr (purple). Arrowheads indicate staining in sections showing patchy expression. Original magnification, ×100.