Abstract
Alkaptonuria (AKU) is characterised by increased circulating homogentisic acid and deposition of ochronotic pigment in collagen-rich connective tissues (ochronosis), stiffening the tissue. This process over many years leads to a painful and severe osteoarthropathy, particularly affecting the cartilage of the spine and large weight bearing joints. Evidence in human AKU tissue suggests that pigment binds to collagen. The exposed collagen hypothesis suggests that collagen is initially protected from ochronosis, and that ageing and mechanical loading causes loss of protective molecules, allowing pigment binding. Schmorl’s staining has previously demonstrated knee joint ochronosis in AKU mice. This study documents more comprehensively the anatomical distribution of ochronosis in two AKU mouse models (BALB/c Hgd−/−, Hgd tm1a−/−), using Schmorl’s staining. Progression of knee joint pigmentation with age in the two AKU mouse models was comparable. Within the knee, hip, shoulder, elbow and wrist joints, pigmentation was associated with chondrons of calcified cartilage. Pigmented chondrons were identified in calcified endplates of intervertebral discs and the calcified knee joint meniscus, suggesting that calcified tissues are more susceptible to pigmentation. There were significantly more pigmented chondrons in lumbar versus tail intervertebral disc endplates (p = 0.002) and clusters of pigmented chondrons were observed at the insertions of ligaments and tendons. These observations suggest that loading/strain may be associated with increased pigmentation but needs further experimental investigation. The calcified cartilage may be the first joint tissue to acquire matrix damage, most likely to collagen, through normal ageing and physiological loading, as it is the first to become susceptible to pigmentation.
Highlights
Alkaptonuria (AKU; OMIM #203500) is a rare inherited metabolic bone disease caused by deficiency of homogentisate 1,2-dioxygenase (HGD; EC 1.13.11.5) [1]
Ochronotic pigment was visible without staining in chondrons of the articular calcified cartilage (ACC) in the knee joint of a 65.7-week-old BALB/c Hgd−/− AKU mouse, which can be seen as both intracellular and extracellular yellow-brown pigment (Fig. 1b, arrowed)
Ochronotic pigmentation in AKU mice has only been reported in the ACC of the knee joint
Summary
Alkaptonuria (AKU; OMIM #203500) is a rare inherited metabolic bone disease caused by deficiency of homogentisate 1,2-dioxygenase (HGD; EC 1.13.11.5) [1]. Most HGA is excreted but over time some is deposited as a dark pigment in connective tissues, primarily the cartilage of loaded joints. This formation of pigment, probably through oxidation of HGA, is termed ochronosis and causes tissues to become dark in appearance and brittle [2, 4, 5]. In cartilage this leads to the early-onset and severe debilitating osteoarthropathy that characterises AKU. Pigmentation has been identified in heart valves, chordae tendineae and the roots and walls of major arteries such as the aorta, where pigmentation was present in the intima and adventitia of the arterial wall [6, 7, 9, 13]
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