The Nature of Extracellular Iron Influences Iron Acquisition by Mycobacterium tuberculosis Residing within Human Macrophages

doi:10.1128/IAI.72.4.2022-2028.2004

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Infection and Immunity, April 2004, p. 2022-2028, Vol. 72, No. 4
0019-9567/04/$08.00+0 DOI: 10.1128/IAI.72.4.2022-2028.2004
Copyright © 2004, American Society for Microbiology. All Rights Reserved.

The Nature of Extracellular Iron Influences Iron Acquisition by Mycobacterium tuberculosis Residing within Human Macrophages

Oyebode Olakanmi,¹^,2 Larry S. Schlesinger,³ Ambar Ahmed,¹ and Bradley E. Britigan¹^,2^,4^*

Department of Internal Medicine and Research Service, VA Medical Center—Iowa City, Iowa City, Iowa 52246,¹ Departments of Internal Medicine,² The Free Radical and Radiation Biology Program, Roy G. and Lucille A. Carver College of Medicine, The University of Iowa, Iowa City, Iowa 52242,⁴ Departments of Internal Medicine and Molecular Virology, Immunology, and Medical Genetics and The Center for Microbial Interface Biology, The Ohio State University, Columbus, Ohio 43210³

Received 29 October 2003/ Returned for modification 5 December 2003/ Accepted 16 December 2003

We have reported that Mycobacterium tuberculosis residing withinthe phagosomes of human monocyte-derived macrophages (MDM) canacquire Fe from extracellular transferrin (TF) and sources withinthe MDM. In the lung, Fe is also bound to lactoferrin (LF) andlow-molecular-weight chelates. We therefore investigated theability of intraphagosomal M. tuberculosis to acquire Fe fromthese sources. M. tuberculosis acquired 30-fold and 3-fold moreFe from LF and citrate, respectively, compared to TF, in spiteof similar MDM-associated Fe. M. tuberculosis infection decreasedMDM-associated Fe relative to uninfected MDM as follows: TF(38.7%), citrate (21.1%), and LF (15.3%). M. tuberculosis Feacquisition from extracellular chelates (exogenous source) andfrom endogenous MDM Fe initially acquired from the three chelates(endogenous source) was compared. M. tuberculosis Fe acquisitionwas similar from exogenous and endogenous sources supplied asFe-TF. In contrast, there was much greater intracellular M.tuberculosis Fe uptake from LF and citrate from the exogenousthan endogenous source. Gamma interferon (IFN- ${gamma}$ ) reduced MDMFe uptake from each chelate by $~$ 50% and augmented the M. tuberculosis-induceddecrease in MDM Fe uptake from exogenous TF, but not from LFor citrate. IFN- ${gamma}$ minimally decreased intracellular M. tuberculosisFe acquisition from exogenous Fe-TF but significantly increasedFe uptake from LF and citrate. Intraphagosomal M. tuberculosisFe acquisition from both exogenous and endogenous MDM sources,and the effect of IFN- ${gamma}$ on this process, is influenced by thenature of the extracellular Fe chelate. M. tuberculosis hasdeveloped efficient mechanisms of acquiring Fe from a varietyof Fe chelates that it likely encounters within the human lung.

* Correpsonding author. Mailing address: University of Iowa Hospitals and Clinics, Department of Internal Medicine, SW54, GH, Iowa City, IA 52242. Phone: (319) 356-3674. Fax: (319) 356-4600. E-mail: bradley-britigan{at}uiowa.edu.

Editor: F. C. Fang

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