Abstract

Mucosal and cutaneous epithelial surfaces act as a barrier to microbial infection. For decades, this barrier was thought to represent only a physical impediment to microbial colonization, dependent upon innate cellular and adaptive immunity to recognize and eliminate foreign antigens. Recently, work from our laboratory and others have identified additional components of the mucosal defense system used to resist infection and respond to injury. These """"""""antimicrobial peptides"""""""" consist of diverse gene families and protein structures and can be found in plants, insects, amphibians, and mammals. At least three families of antimicrobial peptides are produced in human mucosal epithelium: alpha-defensins, beta-defensins, and the more recently discovered cathelicidins. Cathelicidins represent a unique family of mucosal antimicrobial peptides that do not undergo the extensive posttranslational modifications necessary for production of active defensins. This proposal seeks to exploit this fundamental advantage of the cathelicidins and use a bacterial genetic approach to overexpress these peptides and understand their mechanism(s) of action. Specifically, this investigation proposes to: (1) determine the antimicrobial activity of cathelicidins against important human mucosal pathogens and prevalent commensal microflora; (2) investigate mechanisms of microbial sensitivity and resistance to cathelicidins by bacterial mutagenesis and cloning strategies. Clone and characterize bacterial genes conferring resistance or susceptibility to cathelicidins; and (3) express a functional mammalian cathelicidin in a prokaryotic background as a first step toward development of a novel antimicrobial peptide delivery system for therapy of human mucosal infections. This exploratory project, bringing together investigators with complementary expertise, may enhance our understanding of the role of cathelicidins in mucosal immunity, and potentially establish new therapeutic targets and strategies to combat human mucosal pathogens.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Exploratory/Developmental Grants (R21)
Project #
5R21AI048176-02
Application #
6374629
Study Section
Special Emphasis Panel (ZAI1-NN-I (M1))
Program Officer
Ridge, John P
Project Start
2000-09-01
Project End
2002-08-31
Budget Start
2001-09-01
Budget End
2002-08-31
Support Year
2
Fiscal Year
2001
Total Cost
$210,000
Indirect Cost

  Institution

Name
Veterans Medical Research Fdn/San Diego
Department
Type
DUNS #
933863508
City
San Diego
State
CA
Country
United States
Zip Code
92161

  Publications

Henningham, Anna; Döhrmann, Simon; Nizet, Victor et al. (2015) Mechanisms of group A Streptococcus resistance to reactive oxygen species. FEMS Microbiol Rev 39:488-508
Henningham, Anna; Yamaguchi, Masaya; Aziz, Ramy K et al. (2014) Mutual exclusivity of hyaluronan and hyaluronidase in invasive group A Streptococcus. J Biol Chem 289:32303-15
Cole, Jason N; Aziz, Ramy K; Kuipers, Kirsten et al. (2012) A conserved UDP-glucose dehydrogenase encoded outside the hasABC operon contributes to capsule biogenesis in group A Streptococcus. J Bacteriol 194:6154-61
Dahesh, Samira; Nizet, Victor; Cole, Jason N (2012) Study of streptococcal hemoprotein receptor (Shr) in iron acquisition and virulence of M1T1 group A streptococcus. Virulence 3:566-75
Pence, Morgan A; Rooijakkers, Suzan H M; Cogen, Anna L et al. (2010) Streptococcal inhibitor of complement promotes innate immune resistance phenotypes of invasive M1T1 group A Streptococcus. J Innate Immun 2:587-95
Cole, Jason N; Pence, Morgan A; von Köckritz-Blickwede, Maren et al. (2010) M protein and hyaluronic acid capsule are essential for in vivo selection of covRS mutations characteristic of invasive serotype M1T1 group A Streptococcus. MBio 1:
Pinheiro da Silva, Fabiano; Gallo, Richard L; Nizet, Victor (2009) Differing effects of exogenous or endogenous cathelicidin on macrophage toll-like receptor signaling. Immunol Cell Biol 87:496-500
Lauth, Xavier; von Köckritz-Blickwede, Maren; McNamara, Case W et al. (2009) M1 protein allows Group A streptococcal survival in phagocyte extracellular traps through cathelicidin inhibition. J Innate Immun 1:202-14
Di Nardo, Anna; Braff, Marissa H; Taylor, Kristen R et al. (2007) Cathelicidin antimicrobial peptides block dendritic cell TLR4 activation and allergic contact sensitization. J Immunol 178:1829-34
Nizet, Victor (2007) Understanding how leading bacterial pathogens subvert innate immunity to reveal novel therapeutic targets. J Allergy Clin Immunol 120:13-22

Showing the most recent 10 out of 30 publications