Water-soluble C-60 fullerene ameliorates astroglial reactivity and TNFa production in retina of diabetic rats
Tarih
2019Yazar
Nedzvetsky, V. S. and Sukharenko, V, E. and Baydas, G. and Andrievsky,
V, G.
Üst veri
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The complications of both first and second types of diabetes mellitus
patients are important cause of decline in quality of life and mortality
worldwide. Diabetic retinopathy (DR) is a widespread complication that
affects almost 60\% of patients with prolonged (at least 10-15 years)
diabetes. The critical role of glial cells has been shown in retinopathy
initiation in the last decades. Furthermore, glial reactivity and
inflammation could be key players in early pathogenesis of DR. Despite
the large amount of research data, the approaches of effective DR
therapy remain unclear. The progress of DR is accompanied by
pro-inflammatory and pro-oxidative changes in retinal cells including
astrocytes and Muller cells. Glial reactivity is a key pathogenetic
factor of various disorders in neural tissue. Fullerene C-60
nanoparticles were confirmed for both antioxidant and anti-inflammatory
capability. In the presented study glioprotective efficacy of
water-soluble hydrated fullerene C-60 (C(60)HyFn) was tested in a
STZ-diabetes model during 12 weeks. Exposure of the STZ-diabetic rat
group to C(60)HyFn ameliorated the astrocyte reactivity which was
determined via S100 beta and PARP1 overexpression. Moreover, C(60)HyFn
induced the decrease of TNF alpha production in the retina of
STZ-diabetic rats. By contrast, the treatment with C(60)HyFn of the
normal control rat group didn't change the content of all abovementioned
markers of astrogliosis and inflammation. Thus, diabetes-induced
abnormalities in the retina were suppressed via the anti-oxidant,
anti-inflammatory and glioprotective effects of C(60)HyFn at low doses.
The presented results demonstrate that C(60)HyFn can ensure viability of
retinal cells viability through glioprotective effect and could be a new
therapeutic nano-strategy of DR treatment.
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