Can iron depletion inside macrophages serve to prolong HIV disease progression?

Esaki Muthu Shankar , Ramachandran Vignesh , Vijayakumar Velu , Esakimuthu Ponmalar , Kailapuri G. Murugavel , Muthu Sundaram , Pachamuthu Balakrishnan , Suniti Solomon
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引用次数: 1

Abstract

Studies have shown that the more iron in a given population, the more that population is vulnerable to intracellular opportunistic infections (OIs) in AIDS, mainly because these microbes make use of the intracellular iron to proliferate, and could render infections deadly. In contrast, macrophages that lack iron are effective in preventing an establishment of infection. We propose that reduction in total body iron could be a valuable treatment option for some intracellular infections, including OIs. We suggest two options to deprive pathogens of using intracellular iron (i) to practice regular blood-letting, an ancient treatment option, and (ii) to down-regulate hepcidin, the key hormone involved in the regulation of iron balance and recycling. This could also deprive transformed cells of metabolizing iron for survival. Whether or these methods serve to curb the onset of OIs/cancers to prolong HIV disease progression remains to be investigated.

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巨噬细胞内的铁耗尽是否有助于延长HIV疾病的进展?
研究表明,特定人群中的铁含量越高,该人群就越容易受到艾滋病细胞内机会性感染(oi)的影响,这主要是因为这些微生物利用细胞内的铁进行增殖,并可能使感染致命。相反,缺乏铁的巨噬细胞在预防感染方面是有效的。我们建议减少体内总铁可能是一些细胞内感染(包括oi)的一种有价值的治疗选择。我们建议两种方法来阻止病原体利用细胞内铁(i)进行常规放血,这是一种古老的治疗方法;(ii)下调hepcidin,一种参与铁平衡和循环调节的关键激素。这也可能剥夺转化细胞代谢铁的生存能力。这些方法是否有助于抑制OIs/癌症的发生以延长HIV疾病进展仍有待研究。
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