Thus, TWEAK levels may serve as an indication of LN presence and activity.

Methods: Multicenter cohorts of systemic lupus erythematosus (SLE) patients and controls were recruited for cross-sectional and longitudinal analysis of urinary TWEAK (uTWEAK) and/or serum TWEAK (sTWEAK) levels as potential biomarkers of LN. The performance of TWEAK as a biomarker for nephritis was compared to routinely used laboratory tests in lupus patients, including anti-double stranded DNA antibodies and levels of C3 and C4.

Results: uTWEAK levels were significantly higher in LN patients than in non-LN SLE patients and other disease control groups (P=0.039).

Furthermore, uTWEAK was better at distinguishing between LN and non-LN SLE patients than anti-DNA antibodies and complement levels, while high uTWEAK levels predicted LN in SLE patients with odds ratio of 7.36 (95% CI: 2.25 to 24.07; P=0.001). uTWEAK levels peaked during LN flares, and were significantly higher during the flare than at 4 and 6 months prior or following the flare event.

A linear mixed-effects model showed a significant association between uTWEAK levels in SLE patients and their disease activity over time (P=0.008). sTWEAK levels, however, were not found to correlate with the presence of LN or the degree of nephritis activity.

Conclusions: High uTWEAK levels are indicative of LN, as opposed to non-LN SLE and other healthy and disease control populations, and reflect renal disease activity in longitudinal followup.

Thus, our study further supports a role for TWEAK in the pathogenesis of LN, and provides strong evidence for uTWEAK as a candidate clinical biomarker for LN.

Author: Noa SchwartzTamar RubinsteinLinda BurklyChristopher CollinsIrene BlancoLihe SuBernard HojailiMeggan MackayCynthia AranowWilliam StohlBrad RovinJennifer MichaelsonChaim Putterman
Credits/Source: Arthritis Research &Therapy 2009, 11:R143