Atıf İçin Kopyala
Demirci T., Orbak Z., Öztürk N., Kaygisiz M. D., Nalcı K. A., Polat Z. B.
HORMONE RESEARCH IN PAEDIATRICS, cilt.91, ss.345-346, 2019 (SCI-Expanded)
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Yayın Türü:
Makale / Özet
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Cilt numarası:
91
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Basım Tarihi:
2019
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Dergi Adı:
HORMONE RESEARCH IN PAEDIATRICS
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Derginin Tarandığı İndeksler:
Science Citation Index Expanded (SCI-EXPANDED)
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Sayfa Sayıları:
ss.345-346
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Atatürk Üniversitesi Adresli:
Evet
Özet
bring many metabolic diseases, especially obesity and diabetes. Re�cent years, more scientific interest in how can diet effect on brain
function has emerged. We aimed to investigate the effect of high
fructose and high-fat diet on the brain, and whether the presence
of relationship with advanced glycation end products histologi�cally, in rat model.
Materials & Methods: Twenty-four Sprague Dawley rats were
used and divided into 3 groups as control group, high fructose
group and high fatty group. During 12 weeks, while the rats in the
control group were given standard rat chow, those of in the high
fructose and high fatty group were fed with %60 high fructose diet
and %45 high fat diet, respectively. At the end of the experiment,
their brains were removed. AGE and R-AGE expression were eval�uated by immunohistochemistry and biochemically.
Results: In the H-E stained sections, the control group rat
brains showed healthy histological appearance. The brain sections
of the high fructose group showed that histological structure was
deteriorated. There was a significant increase in glial cells, espe�cially in the mediobasal hypothalamus. Shrinkage and eosinophilic
staining of the neurons were noticed, chromatin condensation in
the nucleus was prominent. Also, pericellular edema was present
in neurons and glial cells. Similar findings were observed in the
high-fat group. Glial cells were increased compared to the control
group but were less than the high fructose group. There was dilated
blood vessels and pericellular edema. Small eosinophilic neurons
with shrunken nuclei and with condensed chromatin were also
abundantly observed in the high-fat group. In the control group,
no AGE immunostaining was observed in the axonal structures,
whereas immunopositive staining was observed in neural cells.
When the brain sections of high fructose group were examined,
it was observed that AGE immunostaining positivity was more
significant than the control and high-fat group. R-AGE immu�nostaining intensity in hypothalamus of both high fructose and
high-fat groups was higher than in the control group. Biochemical
results are given in Table 1.
Conclusions: The feeding with both high fructose and high�fat diet might cause the deterioration in the brain mainly the hy�pothalamus, and increased advanced glycation end products may
play an essential role in the development of damage.
Control
Brain
High fructose
Brain
High fat
Brain
Glucose
µmol/L
25,86 25,09 19,42
Insulin
ng/mL
17,93 16,25 17,09
R-AGE pg/mL 93,24 169,42 163,78
GEs ng/mL 132,73 86,85 100,36