The utility of iron chelators in the management of inflammatory disorders

C. Lehmann; S. Islam; S. Jarosch; J. Zhou; D. Hoskin; A. Greenshields; N. Al-Banna; N. Sharawy; A. Sczcesniak; M. Kelly; K. Wafa; W. Cheliak; B. Holbein

doi:10.1155/2015/516740

The utility of iron chelators in the management of inflammatory disorders

C. Lehmann, S. Islam, S. Jarosch, J. Zhou, D. Hoskin, A. Greenshields, N. Al-Banna, N. Sharawy, A. Sczcesniak, M. Kelly, K. Wafa, W. Cheliak, B. Holbein

Producción científica: Contribución a una revista › Artículo de revisión › revisión exhaustiva

47 Citas (Scopus)

Resumen

Since iron can contribute to detrimental radical generating processes through the Fenton and Haber-Weiss reactions, it seems to be a reasonable approach to modulate iron-related pathways in inflammation. In the human organism a counterregulatory reduction in iron availability is observed during inflammatory diseases. Under pathological conditions with reduced or increased baseline iron levels different consequences regarding protection or susceptibility to inflammation have to be considered. Given the role of iron in development of inflammatory diseases, pharmaceutical agents targeting this pathway promise to improve the clinical outcome. The objective of this review is to highlight the mechanisms of iron regulation and iron chelation, and to demonstrate the potential impact of this strategy in the management of several acute and chronic inflammatory diseases, including cancer.

Idioma original	English
Número de artículo	516740
Publicación	Mediators of Inflammation
Volumen	2015
DOI	https://doi.org/10.1155/2015/516740
Estado	Published - 2015

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Publisher Copyright:
© 2015 C. Lehmann et al.

ASJC Scopus Subject Areas

Immunology
Cell Biology

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title = "The utility of iron chelators in the management of inflammatory disorders",

abstract = "Since iron can contribute to detrimental radical generating processes through the Fenton and Haber-Weiss reactions, it seems to be a reasonable approach to modulate iron-related pathways in inflammation. In the human organism a counterregulatory reduction in iron availability is observed during inflammatory diseases. Under pathological conditions with reduced or increased baseline iron levels different consequences regarding protection or susceptibility to inflammation have to be considered. Given the role of iron in development of inflammatory diseases, pharmaceutical agents targeting this pathway promise to improve the clinical outcome. The objective of this review is to highlight the mechanisms of iron regulation and iron chelation, and to demonstrate the potential impact of this strategy in the management of several acute and chronic inflammatory diseases, including cancer.",

author = "C. Lehmann and S. Islam and S. Jarosch and J. Zhou and D. Hoskin and A. Greenshields and N. Al-Banna and N. Sharawy and A. Sczcesniak and M. Kelly and K. Wafa and W. Cheliak and B. Holbein",

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AU - Lehmann, C.

AU - Islam, S.

AU - Jarosch, S.

AU - Zhou, J.

AU - Hoskin, D.

AU - Greenshields, A.

AU - Al-Banna, N.

AU - Sharawy, N.

AU - Sczcesniak, A.

AU - Kelly, M.

AU - Wafa, K.

AU - Cheliak, W.

AU - Holbein, B.

PY - 2015

Y1 - 2015

N2 - Since iron can contribute to detrimental radical generating processes through the Fenton and Haber-Weiss reactions, it seems to be a reasonable approach to modulate iron-related pathways in inflammation. In the human organism a counterregulatory reduction in iron availability is observed during inflammatory diseases. Under pathological conditions with reduced or increased baseline iron levels different consequences regarding protection or susceptibility to inflammation have to be considered. Given the role of iron in development of inflammatory diseases, pharmaceutical agents targeting this pathway promise to improve the clinical outcome. The objective of this review is to highlight the mechanisms of iron regulation and iron chelation, and to demonstrate the potential impact of this strategy in the management of several acute and chronic inflammatory diseases, including cancer.

AB - Since iron can contribute to detrimental radical generating processes through the Fenton and Haber-Weiss reactions, it seems to be a reasonable approach to modulate iron-related pathways in inflammation. In the human organism a counterregulatory reduction in iron availability is observed during inflammatory diseases. Under pathological conditions with reduced or increased baseline iron levels different consequences regarding protection or susceptibility to inflammation have to be considered. Given the role of iron in development of inflammatory diseases, pharmaceutical agents targeting this pathway promise to improve the clinical outcome. The objective of this review is to highlight the mechanisms of iron regulation and iron chelation, and to demonstrate the potential impact of this strategy in the management of several acute and chronic inflammatory diseases, including cancer.

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The utility of iron chelators in the management of inflammatory disorders

Resumen

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ASJC Scopus Subject Areas

ODS de las Naciones Unidas

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