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

ÆÚÊý:

2005ÄêµÚ6ÆÚ

Ò³Âë:

524-527,541

À¸Ä¿:

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2005-12-05

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Title:

Phenotypic modulation of vascular smooth muscle cells and change of mitogenª²activated protein kinase phosphataseª²1(MKPª²1) after intimal injury

×÷Õß:

ÕÅÐÂƽ¹;  ÅÓÔ»ª²;  ·ëÒå²®¹;  ¹ÈÏè¹;  ÀèÃ÷¹ ;  ¸¶×÷ÁÖ¹;  Ê·´ºÖ¾¹

1.»ªÖпƼ¼´óѧͬ¼ÃҽѧԺ¸½ÊôЭºÍÒ½ÔºÐÄÄÚ¿Æ, ºþ±± Î人 430022; 2.ÎÚ³ľÆëÊÐÓÑÒêÒ½Ôº, н® ÎÚ³ľÆë 830049

Author(s):

ZHANG Xinª²ping; PANG Yueª²hua; FENG Yiª²bai;  GU Xiang; LI Ming;  FU Zuoª²lin;  SHI Chunª²zhi

1. Department of Cardiology, Union Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, Hubei 430022, China; 2. Friendship Hospital of Urumchi, Urumchi, Xinjiang 830049, China

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ÄÚĤËðÉË; Ñª¹Üƽ»¬¼¡Ï¸°û; ±íÐÍת»¯; Ë¿ÁÑÔ­¼¤»îµ°°×¼¤Ã¸Á×Ëáøª²1

Keywords:

intimal injury;  vascular smooth muscle cells;  phenotypic modulation;  MKPª²1

·ÖÀàºÅ:

R543.5

DOI:

-

ÎÄÏ×±êʶÂë:

A

ÕªÒª:

Ä¿µÄ ¹Û²ì¶¯ÂöÄÚĤËðÉ˺óѪ¹Üƽ»¬¼¡Ï¸°û(vascular smooth muscle cells,VSMC)±íÐÍת»¯ºÍË¿ÁÑÔ­¼¤»îµ°°×¼¤Ã¸Á×Ëáø-1(mitogenª²activated protein kinase phosphataseª²1,MKPª²1)±í´ïµÄ¶¯Ì¬±ä»¯¡£·½·¨ ·Ö±ðÓÃHEȾɫ¡¢ÃâÒß×黯ºÍÄæת¼ª²¾ÛºÏøÁ´(RTª²PCR)·½·¨¼ì²â¼ÙËðÉË×é(S×é)ºÍËðÉ˺ó²»Í¬Ê±¼äµãѪ¹ÜÐÎ̬ѧ¸Ä±ä¼°Ñª¹Ü±ÚÖÐÔöֳϸ°ûºË¿¹Ô­(PCNA)¡¢Æ½»¬¼¡¦Á¼¡¶¯µ°°×(SM¦Áª²actin)ºÍMKPª²1 mRNA¼°µ°°×±í´ïµÄ±ä»¯¡£½á¹û ¢ÙËðÉ˺ó1 dÖÐĤǻ²à¡¢3 d¹ÜÇ»ÄÚ±íÃæ¿É¼ûÔöÖ³µÄVSMC,5~7 dÐÂÉúÄÚĤ(neointima, NI)Ðγɲ¢Öð½¥Ôöºñ,14~35 d NI½øÐÐÐÔÔöºñ;¸÷×éÖÐĤ¾ùÓÐÔöÖ³µÄVSMCÏòÇ»Ã漯¾Û¡£¢ÚS×éÖÐĤVSMC¼°ÄÚƤϸ°ûPCNAΪÒõÐÔ;ÖÐĤÓÚËðÉ˺ó1~14 d, NIÓÚ5~14 d PCNAÑôÐÔϸ°ûÂÊÖð½¥Ôö¶à,14 d´ï¸ß·å,28 dºó¿ªÊ¼Öð½¥¼õÉÙ,µ«NIÑôÐÔÂʶàÓÚÖÐĤ¡£¢ÛS×éÖÐĤSM¦Áª²actin±í´ïΪÑôÐÔ,ÄÚƤΪÒõÐÔ;ÖÐĤÑôÐÔÃæ»ýÓÚËðÉ˺ó1 d¿ªÊ¼¼õÉÙ,3 d×îΪÃ÷ÏÔ,5 dºó¿ªÊ¼Öð½¥Ôö¼Ó,NIÑôÐÔ±í´ïÈõÓÚÖÐĤ¡£¢ÜS×éÖÐĤMKPª²1³ÊÈõÑôÐÔ»òÑôÐÔ±í´ï,ËðÉ˺ó1d¼´¿ªÊ¼Ï½µ,5~7 d´ï×îµÍ, 14 d ÉÔÓлØÉý,ÖÁ35 dÈÔδ»Øµ½¼ÙËðÉË×éˮƽ; NIÑôÐÔ±í´ïÈõÓÚÖÐĤ¡£MKPª²1±í´ï±ä»¯ÓëPCNA±í´ï±ä»¯³Ê¸ºÏà¹Ø¡£½áÂÛ VSMCÔöÖ³ÄÜÁ¦ÓëÆä±íÐÍת»¯ÃÜÇÐÏà¹Ø, MKPª²1²ÎÓëÁËËðÉ˺óVSMC±íÐÍת»¯µÄµ÷½Ú¡£

Abstract:

AIM To explore phenotypic modulation of vascular smooth muscle cells (VSMC) and change of MKPª²1 expression after intimal injury of rabbit carotid arteries. METHODS The model of vascular restenosis established by balloon injury of rabbit carotid arteries was used. HE staining, immunohistochemistry and reverse transcriptaseª²polymerase chain reaction (RTª²PCR) were used to detect the change of proliferation cell nuclear antigen (PCNA),smooth muscle ¦Áª²actin (SM¦Áª²actin), MKPª²1 mRNA and protein expression, and morphology of shamª²injured group and injury groups at different time. RESULTS The proliferation of VSMC was observed on the side of the medium lumen at 1 d and on the surface of vascular lumen at 3 d after injury. The neointima was formed and gradually getting thickening at 5-7 d, and thickening was more obvious and rapid at 14-35 d. The expression of PCNA was negative in the medium and endothelium in shamª²injured group. Positive cell rate of PCNA was gradually increased at 1-14 d in the medium and at 5-14 d in the neointima, reaching maximum at 14 d and declining gradually at 28 d. Positive cell rate of PCNA in the neointima was higher than that in the medium. Expression of SM¦Áª²actin was positive in the medium, negative in the endothelium in shamª²injured group. Positive cell area of SM¦Áª²actin began to decrease at 1 d in the medium, getting to the minimum at 3 d and started to increase at 5 d. Expression of SM¦Áª²actin in the neointima was lower than in the medium. Expression of MKPª²1 was feeble positive or positive in shamª²injured group. Expression of MKPª²1 initially decreased at 1 d, reaching lowest value at 5-7 d, increased gradually from 14 d. MKPª²1 was negatively correlated with PCNA in the vascular wall after injury. CONCLUSION There is a close relationship between phenotypic modulation and proliferation ability of VSMC. MKPª²1 participates in regulation of phenotypic modulation of VSMC after intimal injury.

²Î¿¼ÎÄÏ×/References

£Û1£Ý Lavigne MC, Ramwell PW, Clarker P. Growth and phenotypic characterization of porcine coronary artery smooth muscle cells£ÛJ£Ý. In Vitro Cell Dev Biol Anim, 1999, 35:136-143.

£Û2£Ý Regan CP, Adam PJ, Madsen CS, et al. Molecular mechanisms of decreased smooth muscle differentiation marker expression after vascular injury £ÛJ£Ý. J Clin Invest, 2000, 106(9): 1139-1147.

£Û3£Ý Haapasalo HK, Sallinen PK, Helen PT, et al. Comparison of three quantitation methods for PCNA immunostaining:applicability and relation to survival in 83 astrocytic neoplasms£ÛJ£Ý. J Patho, 1993, 171:207-214.

£Û4£Ý Metzler B, Li CH, Hu YH, et al. LDL stimulates mitogenª²activated protein kinase phosphataseª²1 expression, independent of LDL receptors, in vascular smooth muscle ce11s£ÛJ£Ý. Arterioscler Thromb Vasc Biol,1999,19:1862-1871.

£Û5£Ý Mark F, Steve B, David J, et al. Cellular senescence after single and repeated balloon catheter denudations of rabbit carotid arteries£ÛJ£Ý. Arteriosclerosis, Thrombosis Vascular Biology, 2001, 21:220-226.

£Û6£Ý Meena SK, Gary KO. Combinatorial control of smooth muscle specific gene expression £ÛJ£Ý. Arteriosclerosis, Thrombosis,Vascular Biology, 2003, 23:737-747.

£Û7£Ý Hungerford JE. Developmental biology of the vascular smooth muscle cell: building a multilayered vessel wall £ÛJ£Ý. J Vasc Res, 1999, 36(1):2-27.

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¸üÐÂÈÕÆÚ/Last Update: 2010-01-06