4.5 Review

The role of disrupted iron homeostasis in the development and progression of arthropathy

Journal

JOURNAL OF ORTHOPAEDIC RESEARCH
Volume 40, Issue 6, Pages 1243-1250

Publisher

WILEY
DOI: 10.1002/jor.25323

Keywords

cartilage degeneration; hereditary hemochromatosis; iron; osteoarthritis; oxidative stress

Categories

Funding

  1. University of Sharjah [1901050144, 2101090196, 2001090180]

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Arthropathy or joint disease is closely associated with iron overload, but there are still some mysteries in the pathogenesis. This review focuses on the interaction between iron accumulation in the joints and cartilage homeostasis, and explores the mechanisms and pathways of iron-induced cartilage degeneration.
Arthropathy or joint disease leads to significant pain and disability irrespective of etiology. Clinical and experimental evidence point to the presence of considerable links between arthropathy and iron overload. Previous work has suggested that iron accumulation in the joints is often associated with increased oxidative stress, disrupted matrix metabolism, and cartilage degeneration. However, key issues regarding the role of iron overload in the pathogenesis of arthropathy remain ambiguous. For example, significant gaps in our knowledge of the primary cellular targets of iron overload-induced damage and the exact molecular mechanism through which disrupted iron homeostasis leads to joint damage still exist. The exact signaling pathway that links iron metabolism and cellular damage in arthropathy also remains largely unmapped. In this review, we focus on the relationship between iron overload and arthropathy with special emphasis on the adversarial relationship between iron that accumulates in the joints over time and cartilage homeostasis. A better understanding of the mechanisms and pathways underlying iron-induced cartilage degeneration may help in defining new prognostic markers and therapeutic targets in arthropathy.

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