Increased osteoclastic activity in acute Charcot’s osteoarthopathy: the role of receptor activator of nuclear factor-kappaB ligand

A Gough; A Sabokbar; A Sabokbar; A. Sabokbar; AM Flanagan; E Grimaud; G. Mabilleau; H Yasuda; IE Adamopoulos; JF Baumhauer; JR Edwards; K Kobayashi; K Motoyoshi; LC Hofbauer; LJ Sanders; M. E. Edmonds; MS Bendre; N. L. Petrova; O Kudo; O Kudo; SL Teitelbaum; T Hirayama; W Jeffcoate; W Zou; WJ Jeffcoate; Y Fujikawa

Increased osteoclastic activity in acute Charcot’s osteoarthopathy: the role of receptor activator of nuclear factor-kappaB ligand

Authors: A Gough
A Sabokbar
A Sabokbar
A. Sabokbar
AM Flanagan
E Grimaud
G. Mabilleau
H Yasuda
IE Adamopoulos
JF Baumhauer
JR Edwards
K Kobayashi
K Motoyoshi
LC Hofbauer
LJ Sanders
M. E. Edmonds
MS Bendre
N. L. Petrova
O Kudo
O Kudo
SL Teitelbaum
T Hirayama
W Jeffcoate
W Zou
WJ Jeffcoate
Y Fujikawa
Publication date: 1 January 2008
Publisher: Springer-Verlag
Doi

Abstract

Aims/hypothesis: Our aims were to compare osteoclastic activity between patients with acute Charcot's osteoarthropathy and diabetic and healthy controls, and to determine the effect of the receptor activator of nuclear factor-kappaB ligand (RANKL) and its decoy receptor osteoprotegerin (OPG). Methods: Peripheral blood monocytes isolated from nine diabetic Charcot patients, eight diabetic control and eight healthy control participants were cultured in the presence of macrophage-colony stimulating factor (M-CSF) alone, M-CSF and RANKL, and also M-CSF and RANKL with excess concentrations of OPG. Osteoclast formation was assessed by expression of tartrate-resistant acid phosphatase on glass coverslips and resorption on dentine slices. Results: In cultures with M-CSF, there was a significant increase in osteoclast formation in Charcot patients compared with healthy and diabetic control participants (p=0.008). A significant increase in bone resorption was also seen in the former, compared with healthy and diabetic control participants (p<0.0001). The addition of RANKL to the cultures with M-CSF led to marked increase in osteoclastic resorption in Charcot (from 0.264±0.06% to 41.6±8.1%, p<0.0001) and diabetic control (0.000±0.00% to 14.2±16.5%, p<0.0001) patients, and also in healthy control participants (0.004±0.01% to 10.5±1.9%, p0.0001). Although the addition of OPG to cultures with M-CSF and RANKL led to a marked reduction of resorption in Charcot patients (41.6±8.1% to 5.9±2.4%, p=0.001), this suppression was not as complete as in diabetic control patients (14.2±16.5% to 0.45±0.31%, p=0.001) and in healthy control participants (from 10.5±1/9% to 0.00±0.00%, p<0.0001). Conclusions/interpretation: These results indicate that RANKL-mediated osteoclastic resorption occurs in acute Charcot's osteoarthropathy. However, the incomplete inhibition of RANKL after addition of OPG also suggests the existence of a RANKL-independent pathway