This
study compared the effects of the nonacylated and acylated
anthocyanin-rich extracts on plasma metabolic profiles of Zucker diabetic
fatty rats. The rats were fed with the nonacylated anthocyanin extract
from bilberries (NAAB) or the acylated anthocyanin extract from purple
potatoes (AAPP) at daily doses of 25 and 50 mg/kg body weight for
8 weeks.
1
H NMR metabolomics was used to study the changes
in plasma metabolites. A reduced fasting plasma glucose level was
seen in all anthocyanin-fed groups, especially in the groups fed with
NAAB. Both NAAB and AAPP decreased the levels of branched-chain amino
acids and improved lipid profiles. AAPP increased the glutamine/glutamate
ratio and decreased the levels of glycerol and metabolites involved
in glycolysis, suggesting improved insulin sensitivity, gluconeogenesis,
and glycolysis. AAPP decreased the hepatic
TBC1D1
and
G6PC
messenger RNA level, suggesting regulation
of gluconeogenesis and lipogenesis. This study indicated that AAPP
and NAAB affected the plasma metabolic profile of diabetic rats differently.
Anthocyanins have
been reported to possess antidiabetic effects.
Recent studies indicate acylated anthocyanins have better stability
and antioxidative activity compared to their nonacylated counterparts.
This study compared the effects of nonacylated and acylated anthocyanins
on hepatic gene expression and metabolic profile in diabetic rats,
using full-length transcriptomics and
1
H NMR metabolomics.
Zucker diabetic fatty (ZDF) rats were fed with nonacylated anthocyanin
extract from bilberries (NAAB) or acylated anthocyanin extract from
purple potatoes (AAPP) at daily doses of 25 and 50 mg/kg body weight
for 8 weeks. Both anthocyanin extracts restored the levels of multiple
metabolites (glucose, lactate, alanine, and pyruvate) and expression
of genes (
G6pac
,
Pck1
,
Pklr
, and
Gck
) involved in glycolysis and gluconeogenesis.
AAPP decreased the hepatic glutamine level. NAAB regulated the expression
of
Mgat4a
,
Gstm6
, and
Lpl
, whereas AAPP modified the expression of
Mgat4a
,
Jun
,
Fos
, and
Egr1
. This study indicated different effects of AAPP and NAAB on the
hepatic transcriptomic and metabolic profiles of diabetic rats.
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