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Wiley InterScience | ||
![]() FEMS Immunology & Medical MicrobiologyVolume 41 Issue 3, Pages 249 - 258 Published Online: 9 Jan 2006 © 2009 Federation of European Microbiological Societies. Published by Blackwell Publishing Ltd. All rights reserved Published on behalf of the Federation of European Microbiological Societies
Abstract | References | Full Text: HTML, PDF (Size: 298K) | Related Articles | Citation Tracking Co-administration of immunomodulator tuftsin and liposomised nystatin can combat less susceptible Candida albicans infection in temporarily neutropenic mice 1Interdisciplinary Biotechnology Unit, AMU, Aligarh, India. 2ICGEB, Shaheed Jeet Singh Marg, New Delhi, India. 3Central Drug Research Institute, Lko, India. 4Jamia Hamdard, New Delhi-62, India. Copyright 2004 Federation of European Microbiological Societies KEYWORDS Candidiasis • Immunomodulator • Liposome • Nystatin • Tuftsin ABSTRACTIn order to develop a prospective chemotherapeutic agent against opportunistic infections, it is important to know that host factors such as degree of immunological debility as well as recovery of immune functions to normality may contribute significantly to a successful elimination of the pathogens. We demonstrated previously that concomitant delivery of antimicrobial agents and immunomodulators to the pathogen harbouring-host contributes to the complete elimination of the deep-seated fungal infections (aspergillosis and candidiasis) in animals with normal immune status. Considering that neutropenic hosts are the main targets of such infections, it can be argued about the potential of the immunomodulator-based therapy in subjects with non-functional immune system. To resolve the hypothesis, we studied the role of immunomodulator tuftsin against experimental murine candidiasis in temporarily neutropenic Balb/c mice. The neutropenic mice were challenged with an isolate of Candida albicans that was showing less susceptibility to both free and liposomised-amphotericin B. The co-administration of tuftsin increased the efficiency of liposomised-polyene antibiotics (nystatin and amphotericin B) against experimental murine candidiasis in immunocompromised Balb/c mice. Pretreatment with liposomised tuftsin prior to C. albicans infection clearly enhanced protection against candidiasis, suggesting a prophylactic role of tuftsin in normal and temporarily neutropenic animals. Received 6 February 2004, Revised 20 March 2004, Accepted 22 March 2004 |