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

ÆÚÊý:

2005ÄêµÚ1ÆÚ

Ò³Âë:

4-7

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³ö°æÈÕÆÚ:

2005-01-05

ÎÄÕÂÐÅÏ¢/Info

Title:

An experimental study on the survival and differentiation of transplanted bone marrow mesenchymal stem cells in rats with cardiomyopathy

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½­µÂÇÚ; Ìï½Ü; °×ÓÀºç; ÕÅÎÄ; ÕÅÀÙ; Öì¾²; ³Âãä

ÖØÇìÒ½¿Æ´óѧ¸½Êô¶ùͯҽԺ£¬ÖØÇì 400014

Author(s):

JIANG Deª²qin;  TIAN Jie;  BAI Yongª²hong;  ZHANG Wen;  ZHANG Lei;  ZHU Jing;  CHEN Yuan

Children's Hospital, Chongqing University of Medical Sciences, Chongqin 400014

¹Ø¼ü´Ê:

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Keywords:

bone marrow mesenchymal stem cells (MSCs);  transplantation;  differentiation;  cardiomyopathy;  experimental study

·ÖÀàºÅ:

R542.2

DOI:

-

ÎÄÏ×±êʶÂë:

A

ÕªÒª:

Ä¿µÄ Ñо¿¹ÇËè¼ä³äÖʸÉϸ°û£¨MSCs£©ÒÆÖ²ÔÚÐļ¡²¡´óÊóÌåÄÚ´æ»î¡¢·Ö»¯µÄÇé¿ö¡£·½·¨ ½«´ÆÐÔWistar´óÊó30Ö»¾­¸¹Ç»×¢É䰢ùËØ6´Î£¨×ܼÁÁ¿15 mg/kg£©£¬½¨Á¢Ðļ¡²¡µÄ¶¯ÎïÄ£ÐÍ£¬ÔÚ´ËÄ£Ð͵Ä×óÊÒÇ°±Ú²ÉÓÃ΢¾²Âö×¢Éä·¨Ö²ÈëMSCs¡£8Öܺó´¦ËÀ´óÊó£¬È¡³öÐÄÔà±ê±¾£¬×ö±ù¶³ÇÐƬ½øÐÐHEȾɫ£¬¹Û²ìÖ²ÈëµÄMSCsÔÚ²¡ËðÐļ¡×éÖ¯Öеı仯¼°ÃâÒßÓ«¹â¼ì²é¹Û²ìÖ²ÈëMSCsÐļ¡¼¡Çòµ°°×ÖØÁ´£¨MHC£©¼°Ðļ¡ÌØÓеÄÁ¬½Óµ°°×£¨CX43£©±í´ïÇé¿ö¡£½á¹û HEȾɫ¼ì²éÏÔʾ£¬Ö²ÈëµÄMSCs´æ»î²¢ÓÐÐÂÉúѪ¹ÜÐγɣ»ÃâÒßÓ«¹â¼ì²éÏÔʾֲÈëµÄMSCs£¬±í´ïMHC¼°CX43£¬µ«½ÏËÞÖ÷±í´ïÈõ¡£½áÂÛ MSCsÒÆÖ²ÔÚÐļ¡²¡´óÊóÌåÄÚÐļ¡Î¢»·¾³ÖÐÄÜ´æ»î£¬²¢ÏòÐļ¡Ï¸°û·Ö»¯¡£

Abstract:

AIM To study bone marrow mesenchymal stem cells (MSCs) transplanted to global myocardium in rats with doxorubicinª²induced cardiomyopathy and to observe their survival and differentiation in damaged host myocardium. METHODS Cardiomyopathy was induced by intraperitoneal injection of doxorubicin (total dose 15 mg/kg for six times) in thirty female Wistar rats. MSCs were intravenously injected into the left ventricular myocardium. Eight weeks later, the hearts were excised for histological analysis to observe morphological changes in the injured myocardium and for immunohistochemical analysis to investigate the expressions of sarcomeric myosin heavy chain (MHC) and connexin 43(CX43) of MSCs. RESULTS HE staining showed that the implanted MSCs labeled with DAPI survived and angiogenesis was identified at the implantation site. Eight weeks after the transplantation, immunohistochemical analysis showed the expression of MHC and CX43 in the implanted MSCs. CONCLUSION Implanted MSCs could survive in damaged myocardium and differentiate into cardiomyocytes.

²Î¿¼ÎÄÏ×/References

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£Û2£Ý ´Þ¼Ì¸£, ÕÔѧ, Îâ×Ú¹í,µÈ. ¹·¹ÇËè¼ä³äÖʸÉϸ°ûÌåÍâ·Ö»¯Îª¼¡Ô´ÐÔϸ°ûµÄ³õ²½¹Û²ì£ÛJ£Ý. ½â·Å¾üҽѧÔÓÖ¾, 2003£¬28£¨5£©£º436-437.

£Û3£Ý ÂÀÌúΰ, Ìï½Ü, Öì¾²,µÈ. ¹ÇËè¼ä³äÖʸÉϸ°ûÌåÄÚÓÕµ¼·Ö»¯ÎªÐļ¡Ï¸°ûµÄ³õ²½ÊµÑé¹Û²ì£ÛJ£Ý.ÖØÇìÒ½¿Æ´óѧѧ±¨, 2003£¬28£¨4£©:463-466.

£Û4£Ý Pittenger MF, Mackay AM, Beck SC, et al. Multilineage potential of adult human mesenchymal stem cells£ÛJ£Ý. Science, 1999, 284: 143-147.

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£Û8£Ý Li RK, Jia ZQ, Weisel RD, et al. Cardiomyocyte transplantation improves heart function £ÛJ£Ý. Ann Thorac Surg, 1996, 62:654-661.

£Û9£Ý Taylor D, Atkins B, Hungspreungs P, et al. Regenerating functional myocardium: improve performance after skeletal myoblasts transplantation£ÛJ£Ý. Nat Med, 1998, 4:929-933.

£Û10£ÝTomita S, Nakatani T, Fukuhara S, et al.Bone marrow stromal cells contract synchronously with cardiomyocytes in a coculture system£ÛJ£Ý. Jpn J Thorac Cardiovasc Surg, 2002,50(8):321-324.

£Û11£ÝTomita S, Li RK, Weisel RD, et al. Autologous transplantation of bone marrow cells improves damaged heart function£ÛJ£Ý. Circulation, 1999, 100(19 Suppl):II247-II256.

£Û12£ÝKocher AA, Schuster MD, Szabolcs MJ, et al. Neovascularization of ischemic myocardium by human boneª²marrowª²derived angioblasts prevents cardiomyocyte apoptosis, reduces remodeling and improves cardiac function£ÛJ£Ý. Nat Med, 2001, 7:430-436.

£Û13£ÝOrlic D, Kajstura J, Chimenti S, et al. Mobilized bone marrow cells repair the infarcted heart, improving function and survival£ÛJ£Ý. Proc Natl Acad Sci U S A, 2001, 98(18):10344-10349.

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