Application of a kind of genistein benzylpiperazine derivative in the field of diabetes
A technology of vegetarian benzylpiperazine and its derivatives, applied in related product fields
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Embodiment 1
[0013] Establish a diabetic mouse model by injecting streptozotocin (STZ), wherein the injection dose of STZ is 50 mg / d / kg body weight, and the injection lasts for 5 days. L is the criterion for successful modeling. A genistein benzylpiperazine derivative 3.5 mg / kg body weight was administered orally for 30 consecutive days. At the end of the experiment, fasting blood glucose, AMPK, and NF-κB were measured. Compared with the diabetic model group, a genistein benzylpiperazine derivative had a 40.2% activation rate of AMPK and a 16.1% inhibition rate of NF-κB. Significantly reduce the fasting blood glucose level to normal level, the reduction rate reaches 20.1%. Therefore, the application mechanism or pathway of genistein benzylpiperazine derivatives in the field of diabetes is: by activating AMPK and inhibiting NF-κB pathway, thereby significantly reducing fasting blood sugar to normal levels.
Embodiment 2
[0015] Establish a diabetic mouse model by injecting streptozotocin (STZ), wherein the injection dose of STZ is 50 mg / d / kg body weight, and the injection lasts for 5 days. L is the criterion for successful modeling. A genistein benzylpiperazine derivative was administered 5.5 mg / kg body weight for 30 consecutive days. At the end of the experiment, fasting blood glucose, AMPK, and NF-κB were measured. Compared with the diabetic model group, a genistein benzylpiperazine derivative had a 71.2% activation rate of AMPK and a 30.7% inhibition rate of NF-κB. Significantly reduce the fasting blood sugar level to normal level, the reduction rate reaches 26.8%. Therefore, the application mechanism or pathway of genistein benzylpiperazine derivatives in the field of diabetes is: by activating AMPK and inhibiting NF-κB pathway, thereby significantly reducing fasting blood sugar to normal levels.
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