Oxidant regulation of the bivalent cation transporter Nramp1
Oxidant regulation of the bivalent cation transporter Nramp1
Nramp1 (murine natural resistance-associated macrophage protein 1 gene)/Slc11a1 (solute carrier family 11 member a1 gene) encodes a bivalent-metal/iron transporter that is expressed within late endosomes/lysosomes of macrophages. A functionally null Nramp1 allele that exhibits impaired bivalent cation transport enables excessive growth of intracellular pathogens. Iron is important for many cellular activities, including defence against pathogens; however, redox-active/free iron can participate in Fenton chemistry that generates reactive oxygen species. Using Raw264.7 cells, non-functional for Nramp1, and stable Nramp1 transfectants, we have examined the effects of impaired bivalent cation transport on macrophage function using glutathione depletion as OS (oxidant stress). Our results demonstrate that OS itself is a signal for increasing Nramp1 transcription and that Nramp1 expression protects against OS. We suggest that OS-mediated protection by Nramp1 function may arise from direct removal of redox-active bivalent cations from a cytosolic pool. We show that OS transcriptional responses are probably mediated by the Sp1 transcription factor.
Nramp1, oxidant stress, specificity protein 1 (Sp1), transcriptional regulation
1008-1010
Yeung, I.Y.L.
3f27b5c7-072c-44cc-9666-6324cd63e764
Phillips, E.
16ee48e2-0cca-478b-b233-28aca3957406
Mann, D.A.
54e772bb-f94f-4485-98c8-b2339a929d86
Barton, C.H.
f0d39d0b-5a75-48ca-86cc-a7b3aba8b6b5
2004
Yeung, I.Y.L.
3f27b5c7-072c-44cc-9666-6324cd63e764
Phillips, E.
16ee48e2-0cca-478b-b233-28aca3957406
Mann, D.A.
54e772bb-f94f-4485-98c8-b2339a929d86
Barton, C.H.
f0d39d0b-5a75-48ca-86cc-a7b3aba8b6b5
Yeung, I.Y.L., Phillips, E., Mann, D.A. and Barton, C.H.
(2004)
Oxidant regulation of the bivalent cation transporter Nramp1.
Biochemical Society Transactions, 32 (6), .
Abstract
Nramp1 (murine natural resistance-associated macrophage protein 1 gene)/Slc11a1 (solute carrier family 11 member a1 gene) encodes a bivalent-metal/iron transporter that is expressed within late endosomes/lysosomes of macrophages. A functionally null Nramp1 allele that exhibits impaired bivalent cation transport enables excessive growth of intracellular pathogens. Iron is important for many cellular activities, including defence against pathogens; however, redox-active/free iron can participate in Fenton chemistry that generates reactive oxygen species. Using Raw264.7 cells, non-functional for Nramp1, and stable Nramp1 transfectants, we have examined the effects of impaired bivalent cation transport on macrophage function using glutathione depletion as OS (oxidant stress). Our results demonstrate that OS itself is a signal for increasing Nramp1 transcription and that Nramp1 expression protects against OS. We suggest that OS-mediated protection by Nramp1 function may arise from direct removal of redox-active bivalent cations from a cytosolic pool. We show that OS transcriptional responses are probably mediated by the Sp1 transcription factor.
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Published date: 2004
Keywords:
Nramp1, oxidant stress, specificity protein 1 (Sp1), transcriptional regulation
Identifiers
Local EPrints ID: 27504
URI: http://eprints.soton.ac.uk/id/eprint/27504
ISSN: 0300-5127
PURE UUID: f879f9fb-8d24-4a1b-bd32-7d0a71c1c6e2
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Date deposited: 26 Apr 2006
Last modified: 08 Jan 2022 12:54
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Contributors
Author:
I.Y.L. Yeung
Author:
E. Phillips
Author:
D.A. Mann
Author:
C.H. Barton
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