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¡¶Î÷²¿ÖÐÒ½Ò©¡·[ISSN:2096-9600/CN:62-1204/R]

¾í:

35

ÆÚÊý:

2022Äê12ÆÚ

Ò³Âë:

35-38

À¸Ä¿:

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2022-12-15

ÎÄÕÂÐÅÏ¢/Info

Title:

Study on the Mechanism of Soft Capsules of Compound Oil of Jujube, Arboruitae and Gardenia Improving the Intelligence of GPR40

×÷Õß:

Ãç÷¾²¹, ËÕÅô·É², ÁõÉú÷¹

1.ÑÓ°²´óѧҽѧԺ£¬ÉÂÎ÷ ÑÓ°² 716000
2.ÑÓ°²´óѧ

Author(s):

MIAO Meijing¹, SU Pengfei², LIU Shengmei¹

1.Medical School of Yan'an University, Yan'an 716000, China
2.Yan'an University

¹Ø¼ü´Ê:

ѧϰ¼ÇÒäÕÏ°­; Ëá°ØèÙÓÍÈí½ºÄÒ; ÐÐΪѧ; GPR40; Ð¡Êó; ¶¯ÎïʵÑé

Keywords:

learning and memory disorders; soft capsules of compound oil of jujube;  arboruitae and gardenia; ethology; GPR40; mice; animal experiment

·ÖÀàºÅ:

R285

DOI:

10.12174/j.issn.2096-9600.2022.12.08

ÎÄÏ×±êÖ¾Âë:

A

ÕªÒª:

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Abstract:

ObjectiveTo observe the effects of soft capsules of compound oil of jujube, arboruitae and gardenia (COJAG) on the intelligence of memory acquisition impairment mice models, and analyze the specific mechanism of COJAG improving the brain of GPR40. MethodsAll 152 Kunming male mice were chosen, after one week of adaptive feeding, 24 ones were selected as blank control group, the remaining 128 mice were established into memory acquisition impairment models, and 120 successful mice models were randomized into five groups, 24 ones in each group, that is, the model group, Naofukang group, low, moderate and high dosages groups of COJAG. All the groups were drenched with the medicine in the set dose, once each day, for 40 days consecutively. By the end of the experiment, Morris water mase was used to detect the mice's behaviors, immuno-fluorescence and immunohistochemistry were applied to detect the expressions and distribution of GPR40 in central nervous system. ResultsFrom the first day to the fifth day, the latency and path of finding platform in the model group were higher than these in the other groups (P<0.05); after the medication, the latency and path of finding platform in COJAG group and Naofukang group were reduced compared with these of the model group (P<0.05); the latency and path of finding platform in high dose group of COJAG were the shortest, the difference was statistically significant compared with low dose group (P<0.05), the difference had no statistical meaning compared with moderate dose group (P>0.05); Compared with blank control group, the length of stay at the third quadrant prolonged, the percentage of the journey at the third quadrant lowered and the times of crossing the platform reduced in the mice of the model group (P<0.05); after the medication, the length of stay at the third quadrant shortened, the length of stay at the third quadrant increased and the times of crossing the platform added in COJAG group and Naofukang group (P<0.05); in high dose group of COJAG, the length of stay at the third quadrant was the shortest, the percentage of the journey at the third quadrant the highest and the times of crossing the platform were the most, the difference had statistical meaning when high dose group was compared with low dose group (P<0.05), while there was no significant difference when it was compared with moderate dose group (P>0.05). Compared with other groups, the expressions of GPR40 were the highest in the control group, the expressions ranked from high to low in the other groups: Naofukang group, high dose group, moderate dose group, low dose group, and the expressions in the model group were the lowest. ConclusionThe application of COJAG could elevate the expressions of GPR40 in cerebral tissue, promote the proliferation of neural precursor cells and synaptic growth of neuronal cells, and this might be the main mechanism of COJAG improving learning ability in memory impairment mice.

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