RT Journal Article
SR Electronic
T1 Serum total renin, an independent marker of the activity and severity of retinopathy in patients with IDDM
JF British Journal of Ophthalmology
JO Br J Ophthalmol
FD BMJ Publishing Group Ltd.
SP 939
OP 944
DO 10.1136/bjo.82.8.939
VO 82
IS 8
A1 Sari Mäkimattila
A1 Paula Summanen
A1 Irma Matinlauri
A1 Matti Mäntysaari
A1 Anna Schlenzka
A1 Maija Aalto
A1 Kerttu Irjala
A1 Hannele Yki-Järvinen
YR 1998
UL http://bjo.bmj.com/content/82/8/939.abstract
AB BACKGROUND/AIMS Recent studies have demonstrated marked renin and prorenin concentration gradients between ocular tissues and blood, and local expression of the renin-angiotensin system (RAS) in the eye. The authors determined whether serum total renin, which mostly consists of prorenin, is a marker of the activity and severity of diabetic retinopathy independent of other microvascular complications. METHODS Total renin concentrations (TRC) were measured with a time resolved immunofluorometric assay in 38 patients with IDDM (age 34 (SD 7) years, duration of disease 22 (7) years, serum creatinine 95 (15) μmol/l, urinary albumin excretion rate (UAER) 207 (829) μg/min, HbA1c 8.5% (1.2%)), and in 13 matched normal subjects. All subjects were carefully characterised with respect to the presence and severity of retinopathy (RP score), nephropathy, and neuropathy using seven different tests of autonomic neuropathy. RESULTS Serum TRC was on average twofold higher in IDDM (396 (SE 211) ng/l) than in normal subjects (201 (88) ng/l, p&lt;0.001). It was nearly twofold higher in patients with preproliferative or active proliferative retinopathy requiring careful follow up or therapy (TRC 596 (268) ng/l, n=11) compared with those with quiescent proliferative retinopathy after laser treatment (TRC 338 (183) ng/l, p&lt;0.01, n=5); moderately severe non-proliferative retinopathy (337 (106) ng/l, p&lt;0.01, n=13), no retinopathy, or only minimal non-proliferative retinopathy (270 (43) ng/l, p&lt;0.001, n=9). In multiple linear regression analysis, RP score (p&lt;0.01), but not the UAER or any index of autonomic neuropathy, was an independent determinant of serum TRC, and explained 32% of its variation (R=0.57, p&lt;0.005). CONCLUSIONS Serum TRC in patients with diabetic retinopathy is increased independent of renal function and autonomic neuropathy, especially in those with severe active changes requiring careful follow up or treatment. These findings support the idea that diabetic retinopathy is the most important determinant of serum TRC in patients with IDDM, and that TRC is produced when retinopathy is active.