Overexpression of the Natural Inhibitor of Cysteine Peptidases in Leishmania mexicana Leads to Reduced Virulence and a Th1 Response

doi:10.1128/IAI.00558-08

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Infection and Immunity, July 2009, p. 2971-2978, Vol. 77, No. 7
0019-9567/09/$08.00+0 doi:10.1128/IAI.00558-08
Copyright © 2009, American Society for Microbiology. All Rights Reserved.

Overexpression of the Natural Inhibitor of Cysteine Peptidases in Leishmania mexicana Leads to Reduced Virulence and a Th1 Response

Karen Bryson,¹^, Sébastien Besteiro,²^,^, H. Adrienne McGachy,¹ Graham H. Coombs,¹ Jeremy C. Mottram,² and James Alexander¹^*

Strathclyde Institute of Pharmacy and Biomedical Sciences, University of Strathclyde, The John Arbuthnott Building, 27 Taylor St., Glasgow G4 ONR, United Kingdom,¹ Wellcome Centre for Molecular Parasitology and Division of Infection and Immunity, Glasgow Biomedical Research Centre, University of Glasgow, 120 University Place, Glasgow G12 8TA, United Kingdom²

Received 7 May 2008/ Returned for modification 19 June 2008/ Accepted 23 April 2009

Leishmania mexicana cysteine peptidases (CPs) have been identifiedas important parasite virulence factors. More recently, a naturalinhibitor of CPs (ICP) from L. mexicana has been characterized,and ICP mutants have been created. Infection of BALB/c micewith ICP null mutants or ICP reexpressing mutants resulted innonhealing, progressively growing lesions albeit slightly attenuatedcompared with the growth of lesions produced by wild-type parasites.In contrast, BALB/c mice infected with mutants overexpressingICP were able to significantly control lesion growth or heal.While BALB/c mice infected with wild-type parasites, ICP nullmutants, or ICP reexpressing mutants produced significant antibodyresponses, including immunoglobulin E (IgE), no Th1 response,as indicated by antigen-induced splenocyte gamma interferon(IFN- ${gamma}$ ) production, could be demonstrated. In contrast, BALB/cmice infected with mutants overexpressing ICP produced significantlyless antibody, particularly IgE, as well as significantly reducedsplenocyte interleukin-4 and enhanced IFN- ${gamma}$ production. BALB/cmice were able to resolve infection following infection withone ICP overexpressing clone, which was subsequently used forvaccination studies with BALB/c mice. However, no protectionwas afforded these mice when they were challenged with wild-typeparasites. Nevertheless, two other mouse strains susceptibleto L. mexicana, C3H and C57BL/6, vaccinated with overexpressingICP mutants were able to control challenge infection associatedwith an enhanced Th1 response. This study confirms that L. mexicanaCPs are virulence factors and that ICPs have therapeutic potential.

* Corresponding author. Mailing address: Strathclyde Institute of Pharmacy and Biomedical Sciences, University of Strathclyde, The John Arbuthnott Building, 27 Taylor St., Glasgow G4 ONR, United Kingdom. Phone: 44 141 548 3925. Fax: 44 141 552 3562. E-mail: j.alexander{at}strath.ac.uk

Published ahead of print on 11 May 2009.

Editor: J. F. Urban, Jr.

Both authors contributed equally to the study.

Present address: UMR CNRS 5235, Université de Montpellier2, Montpellier F-34095, France.