Reduced Expression of CD45 Protein-tyrosine Phosphatase Provides Protection against Anthrax Pathogenesis

doi:10.1074/jbc.M809633200

Reduced Expression of CD45 Protein-tyrosine Phosphatase Provides Protection against Anthrax Pathogenesis^*

^‡United States Army Medical Research Institute of Infectious Diseases, Frederick, Maryland 21702-5011, ^§Target Structure Based Drug Discovery Group, SAIC-Frederick, Inc., NCI-Frederick, National Institutes of Health, Frederick, Maryland, 21702-1201, ^¶AVI BioPharma Inc., Corvallis, Oregon 97333, ^∥Target Structure Based Drug Discovery Group, Information Technology Branch, Developmental Therapeutic Program, NCI, National Institutes of Health, Frederick, Maryland 21702-1201, ^**Sidney Kimmel Cancer Center, San Diego, California 92121, and ^‡‡Virogenics, Inc., Del Mar, California 92014

¹ To whom correspondence may be addressed: 1425 Porter St., USAMRIID, Frederick, MD 21702. Tel.: 301-619-4985; Fax: 301-619-2348; E-mail: rekha.panchal{at}amedd.army.mil. ² To whom correspondence may be addressed: 1425 Porter St., USAMRIID, Frederick, MD 21702. Tel.: 301-619-4246; Fax: 301-619-2348; E-mail: sina.bavari{at}amedd.army.mil.

Abstract

The modulation of cellular processes by small molecule inhibitors, gene inactivation, or targeted knockdown strategies combined with phenotypic screens are powerful approaches to delineate complex cellular pathways and to identify key players involved in disease pathogenesis. Using chemical genetic screening, we tested a library of known phosphatase inhibitors and identified several compounds that protected Bacillus anthracis infected macrophages from cell death. The most potent compound was assayed against a panel of sixteen different phosphatases of which CD45 was found to be most sensitive to inhibition. Testing of a known CD45 inhibitor and antisense phosphorodiamidate morpholino oligomers targeting CD45 also protected B. anthracis-infected macrophages from cell death. However, reduced CD45 expression did not protect anthrax lethal toxin (LT) treated macrophages, suggesting that the pathogen and independently added LT may signal through distinct pathways. Subsequent, in vivo studies with both gene-targeted knockdown of CD45 and genetically engineered mice expressing reduced levels of CD45 resulted in protection of mice after infection with the virulent Ames B. anthracis. Intermediate levels of CD45 expression were critical for the protection, as mice expressing normal levels of CD45 or disrupted CD45 phosphatase activity or no CD45 all succumbed to this pathogen. Mechanism-based studies suggest that the protection provided by reduced CD45 levels results from regulated immune cell homeostasis that may diminish the impact of apoptosis during the infection. To date, this is the first report demonstrating that reduced levels of host phosphatase CD45 modulate anthrax pathogenesis.

Footnotes

↵3 The abbreviations used are: PTP, protein-tyrosine phosphatase; PMO, phosphorodiamidate morpholino oligomers; LF, lethal factor; MAPKK/MEK, mitogen-activated protein kinase kinase; LT, lethal toxin; DiFMUP, 6,8-difluoro-4-methylumbelliferyl phosphate; PA, protective antigen; CFU, colony-forming units; m.o.i., multiplicity of infection; PBS, phosphate-buffered saline.
↵4 E. L. Virts, N. Raschke, R. G. Panchal, S. Bavari and W. C. Raschke, manuscript in preparation.
↵* This work was supported, in whole or in part, by National Institutes of Health Grant N01-CO-12400, by the Defense Threat Reduction Agency (to S. B. and R. G. P.), the NIAID, National Institutes of Health Grant R43 A1055102 (to W. C. R.), and by the Developmental Therapeutics Program in the Division of Cancer Treatment and Diagnosis of the NCI, National Institutes of Health.
↵ The on-line version of this article (available at http://www.jbc.org) contains supplemental Figs. 1–8 and Tables 1 and 2.
- Received December 22, 2008.
- Revision received February 25, 2009.
The American Society for Biochemistry and Molecular Biology, Inc.