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¡¶ÐÄÔàÔÓÖ¾¡·[ISSN:1009-7236/CN:61-1268/R]

ÆÚÊý:

2013ÄêµÚ1ÆÚ

Ò³Âë:

22-027

À¸Ä¿:

»ù´¡Ñо¿

³ö°æÈÕÆÚ:

2013-02-25

ÎÄÕÂÐÅÏ¢/Info

Title:

Empirical study of bionomical effect of mice mesenchymal stem cells preconditioned by endothelial cellª²specific moleculeª²1

×÷Õß:

Öì×ڳɹ; »Ý ½Ü²; ÉòÕñÑDz; Ê¢Ïþ¶«¹; Öܽ¨Áú¹; ·¶èº¹; ½ðæççù¹

(1.³£ÊìÊеڶþÈËÃñÒ½ÔºÐÄÄÚ¿Æ£¬½­ËÕ ³£Êì 215500£»2.ËÕÖÝ´óѧ¸½ÊôµÚÒ»ÈËÃñÒ½ÔºÐÄÄÚ¿Æ£¬½­ËÕ ËÕÖÝ 215006)

Author(s):

ZHU Zong cheng¹;  HUI Jie²;  SHEN Zhenª²ya²;  SHENG Xiaoª²dong¹;  ZHOU Jianª²long¹;  FAN Tao¹;  JIN Xiaoª²qi¹

(1.Department of Cardiology, Changshu Second People¡¯s Hospital, Suzhou 215006, Jiangsu, China; 2.Department of Cardiology, First Hospital Affiliated to Suzhou University, Suzhou 215006, Jiangsu, China)

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ÄÚƤϸ°ûÌØÒìÐÔ·Ö×Óª²1; ¹ÇËè¼ä³äÖʸÉϸ°û; Ðļ¡¹£ËÀ; Ð¡Êó

Keywords:

endothelial cellª²specific moleculeª²1;  bone marrow mesenchymal stem cells;  myocardial infarction;  mouse

·ÖÀàºÅ:

R542.2

DOI:

-

ÎÄÏ×±êʶÂë:

A

ÕªÒª:

Ä¿µÄ:̽ÌÖÄÚƤϸ°ûÌØÒìÐÔ·Ö×Óª²1£¨ESMª²1£©·õÓýÔ¤´¦Àí¶ÔСÊó¹ÇËè¼ä³äÖʸÉϸ°ûÉúÎïѧÌØÐÔµÄÓ°Ï죬Ϊ¸Éϸ°ûÒÆÖ²ÌṩʵÑéÒÀ¾Ý¡£·½·¨£º ÅàÑø¼°¼ø¶¨¹ÇËè¼ä³äÖʸÉϸ°û¡£Ìáȡϸ°ûÊý¼°Å¨¶È¹Ì¶¨µÄ³õ¼¶ÅàÑøÒºÖеĹÇËè¼ä³äÖʸÉϸ°û£¬²¢·ÖΪÁ½×飺¶ÔÕÕ×飨²»½øÐÐÔ¤´¦Àí£©¼°3¸öŨ¶È£¨0ª±05 ¦Ìg/ml¡¢0ª±1 ¦Ìg/ml¡¢0ª±15 ¦Ìg/ml£©µÄESMª²1Ô¤´¦Àí×顣ÿ×éÉè4¸ö¸´¿×£¬Ã¿¿×¾ù´¦Àí60 min¡£ÊÕ¼¯Ã¿¿×ÖеÄÌõ¼þÅàÑøÒº£¬¼ì²âÔ¤´¦Àí¶Ô¹ÇËè¼ä³äÖʸÉϸ°û·ÖÃÚѪ¹ÜÄÚƤÉú³¤Òò×Ó(VEGF)¼°¼îÐÔÁ×Ëáø(ALP)µÄÓ°Ïì¡£½á¹û£º ESMª²1·õÓýÔ¤´¦Àí¹ÇËè¼ä³äÖʸÉϸ°ûºó£¬Æä´æ»îÂÊÃ÷ÏÔÔö¼Ó£¬¶øµòÍöÂÊÏÔÖøϽµ£¬ÇÒ¹ÇËè¼ä³äÖʸÉϸ°ûÔöÖ³ÄÜÁ¦Ëæ×ÅESMª²1Ô¤´¦ÀíŨ¶ÈµÄÔö¼Ó¶øÖð½¥Éý¸ß£¬µòÍöÂÊÈ´³ÊÏà·´µÄϽµÇ÷ÊÆ¡£ESMª²1Ô¤´¦Àíºó£¬¹ÇËè¼ä³äÖʸÉϸ°û·ÖÃÚVEGF¡¢ALPµÄˮƽÃ÷ÏÔÉý¸ß£¬ÇÒËæ×ÅESMª²1Ũ¶ÈµÄÔö¼Ó£¬¹ÇËè¼ä³äÖʸÉϸ°û·ÖÃÚVEGF¡¢ALPµÄˮƽҲÏàÓ¦Ôö¼Ó¡£ESMª²1·õÓýÔ¤´¦ÀíºóµÄ¹ÇËè¼ä³äÖʸÉϸ°û£¬Ï¸°ûÐÎ̬һÖ£¬Éú³¤¼°·Ö»¯Ëٶȼӿ졣½áÂÛ£º ESMª²1·õÓýÔ¤´¦Àí¹ÇËè¼ä³äÖʸÉϸ°û²»½ö´Ù½ø¹ÇËè¼ä³äÖʸÉϸ°ûÔöÖ³¼°½µµÍÆäµòÍö£¬¶øÇÒ¿ÉÔö¼ÓVEGF¡¢ALPµÄ·ÖÃÚ¡£ESMª²1ͨ¹ý»î»¯¹ÇËè¼ä³äÖʸÉϸ°û£¬Ìá¸ßϸ°û±¾ÉíµÄDZÄÜ£¬¼Ì¶øÌá¸ßÆä´æ»î¡¢ÔöÖ³µÄÄÜÁ¦, ΪÁÙ´²¼±ÐÔÐļ¡¹£ËÀµÄÖÎÁÆÌṩÁ˹㷺µÄÓ¦ÓÃÇ°¾°¡£

Abstract:

AIM:To investigate the endothelial cellª²specific moleculeª²1 (ESMª²1) after incubation with pretreatment on mouse bone marrow mesenchymal stem cells (BMª²MSCs). We studied the biological characteristic influence in order to provide an experimental basis for stem cell transplantation. METHODS: For cultivation and identification of BMª²MSCs, extraction of cell number and concentration of fixed primary cultured BMª²MSCs were divided into two groups: control group (no pretreatment) and three concentrations (0ª±05 ¦Ìg/ml, 0ª±1 ¦Ìg/ml, 0ª±15 ¦Ìg/ml) of ESMª²1 pretreatment group. Each group has four complex holes. Each hole was preconditioned for 60 min. Every hole was collected in the conditioned medium, and effect of pretreatment on BMª²MSCs on secretion of vascular endothelial growth factor (VEGF) and alkaline phosphatase (ALP) was shown. RESULTS: After incubation of ESMª²1 preconditioned BMª²MSCs, the survival rate increased significantly, whereas apoptosis rate decreased significantly and proliferation of BMª²MSCs with increasing concentrations of ESMª²1 pretreatment increased, but the apoptosis rate showed the opposite decreasing trend. ESMª²1 after pretreatment showed BMª²MSCs secreted VEGF, ALP levels increased, and with increasing the concentration of ESMª²1, BMª²MSCs secreted VEGF. ALP levels also increased accordingly. Incubation of ESMª²1 preconditioned BMª²MSCs, cell morphology, and growth and differentiation is accelerated. CONCLUSION: ESMª²1 incubated with preconditioned BMª²MSCs promote the proliferation of BMª²MSCs and reduce apoptosis and can increase VEGF and ALP secretion. ESMª²1 through the activation of BMª²MSCs improves the cell potential itself and then improves survival and proliferation. The prospect exists for clinical treatment of acute myocardial infarction with wide application.

²Î¿¼ÎÄÏ×/References

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¸üÐÂÈÕÆÚ/Last Update: 2013-03-20