Abstract |
Oropharyngeal candidiasis (OPC) is caused by the opportunistic fungi Candida albicans and is prevalent in immunocompromised patients, individuals with dry mouth, or patients with prolonged antibiotic therapies that reduce oral commensal bacteria. Human salivary histatins, including histatin 5 (Hst 5), are small cationic proteins that are the major source of fungicidal activity of saliva. However, Hsts are rapidly degraded in vivo, limiting their usefulness as therapeutic agents despite their lack of toxicity. We constructed a conjugate peptide using spermidine (Spd) linked to the active fragment of Hst 5 (Hst 54-15), based upon our findings that C. albicans spermidine transporters are required for Hst 5 uptake and fungicidal activity. We found that Hst 54-15-Spd was significantly more effective in killing C. albicans and Candida glabrata than Hst 5 alone in both planktonic and biofilm growth and that Hst 54-15-Spd retained high activity in both serum and saliva. Hst 54-15-Spd was not bactericidal against streptococcal oral commensal bacteria and had no hemolytic activity. We tested the effectiveness of Hst 54-15-Spd in vivo by topical application to tongue surfaces of immunocompromised mice with OPC. Mice treated with Hst 54-15-Spd had significant clearance of candidal tongue lesions macroscopically, which was confirmed by a 3- to 5-log fold reduction of C. albicans colonies recovered from tongue tissues. Hst 54-15-Spd conjugates are a new class of peptide-based drugs with high selectivity for fungi and potential as topical therapeutic agents for oral candidiasis.
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Authors | Swetha Tati, Rui Li, Sumant Puri, Rohitashw Kumar, Peter Davidow, Mira Edgerton |
Journal | Antimicrobial agents and chemotherapy
(Antimicrob Agents Chemother)
Vol. 58
Issue 2
Pg. 756-66
( 2014)
ISSN: 1098-6596 [Electronic] United States |
PMID | 24247141
(Publication Type: Journal Article, Research Support, N.I.H., Extramural)
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Chemical References |
- Antifungal Agents
- HTN3 protein, human
- Histatins
- Oligopeptides
- Spermidine
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Topics |
- Administration, Mucosal
- Animals
- Antifungal Agents
(chemistry, pharmacology)
- Biofilms
(drug effects, growth & development)
- Biological Transport
- Candida albicans
(drug effects, growth & development)
- Candida glabrata
(drug effects, growth & development)
- Candidiasis, Oral
(drug therapy, immunology, microbiology)
- Female
- Histatins
(chemistry, pharmacology)
- Humans
- Immunocompromised Host
- Mice
- Mouth Mucosa
(drug effects, immunology, microbiology)
- Oligopeptides
(chemistry)
- Plankton
(drug effects, growth & development)
- Spermidine
(chemistry)
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