«ÉÏһƪ/Previous Article|±¾ÆÚĿ¼/Table of Contents|ÏÂһƪ/Next Article»

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

ÆÚÊý:

2006ÄêµÚ4ÆÚ

Ò³Âë:

400-403

À¸Ä¿:

»ù´¡Ñо¿

³ö°æÈÕÆÚ:

2006-08-25

ÎÄÕÂÐÅÏ¢/Info

Title:

Experimental study of engineered cardiac patch in vitro

×÷Õß:

³£º£Ï¼; Ö£Ç¿Ý¥

µÚËľüÒ½´óѧÌƶ¼Ò½ÔºÐÄÄÚ¿Æ£¬ÉÂÎ÷ Î÷°² 710038

Author(s):

CHANG Hai-xia;  ZHENG Qiang-sun

Department of Cardiology, Tangdu Hospital, Fourth Military Medical University, Xi¡äan£¬Shaanxi 710038, China

¹Ø¼ü´Ê:

Ô­´úÐļ¡Ï¸°û; ÒºÌ¬¢ñÐͽºÔ­; ¹¤³Ì»¯Ðļ¡Æ¬²ã

Keywords:

primary cardiomyocyte;  liquid collagen type I;  engineered cardiac patch

·ÖÀàºÅ:

R540.27

DOI:

-

ÎÄÏ×±êʶÂë:

A

ÕªÒª:

Ä¿µÄ ̽Ë÷ÔÚÌåÍâ¹¹½¨¹¤³Ì»¯Ðļ¡Æ¬²ãµÄ·½·¨¡£·½·¨ ÓýºÔ­¡¢Matrigel¡¢2±¶DMEM·Ö±ðÓëÖƱ¸µÄÈéÊóÔ­´úÐļ¡Ï¸°û»ìºÏ£¬×¢Èë·½ÐβÛÄÚÐγÉÐļ¡Æ¬²ã£¬5 dºóÐж¯Ì¬Á¦Ñ§À­Éì¼ÌÐøÅàÑø1ÖÜ¡£³£¹æHEȾɫ¡¢ÃâÒß×黯ȾɫµÈ¶Ô×éÖ¯¹¤³Ì»¯Ðļ¡×éÖ¯£¬¼´Ðļ¡Æ¬²ã½øÐÐÆÀ¼Û¡£½á¹û Ðļ¡Æ¬²ãÔÚÅàÑø1 d³öÏÖµã×´×Ô·¢ÐÔÌø¶¯£¬Ëæʱ¼äµÄÑÓ³¤Ìø¶¯µÄÇøÓòÖð½¥Ôö¶à,Ç¿¶ÈÖð½¥Ôö´ó,3 d³öÏÖ²»Ò»Öµľֲ¿Ìø¶¯£¬À­Éì2 d³öÏÖÈâÑۿɼûÕû¸öƬ²ãµÄÒ»ÖÂÐԵĽÚÂÉÐÔÌø¶¯¡£HEȾɫÏÔʾƬ²ãÖÐϸ°ûÅÅÁÐÕûÆëÓëÕý³£³ÉÄê´óÊóÐļ¡×éÖ¯ÀàËÆ£¬ÃâÒß×黯½á¹ûÏÔʾÓзḻµÄÐļ¡Ï¸°û¡£µç¾µÏÔʾÌõ´øÖеÄÐļ¡Ï¸°ûº¬ÓзḻµÄ¼¡Ô­ÏËά,¼¡½Ú½á¹¹ºÍZÏßÇåÎú¿É¼û¡£½áÂÛ ¸Ã·½·¨¿ÉÒԳɹ¦¹¹½¨ÀàËÆÌìÈ»Ðļ¡×éÖ¯µÄ¹¤³Ì»¯Ðļ¡Æ¬²ã¡£

Abstract:

AIM To construct engineered cardiac patch in vitro. METHODS Liquid collagen type I, Matrigel and 2 DMEM were mixed with neonatal rat cardiac myocytes. The mixture was then pippetted into square molds to construct cardiac patch. Five days later, the cardiac patch was subjected to dynamic stretch for another 7 days. Microscopy and transmission electron microscopy, routine HE staining and immunohistochemical staining were used to analyze the EHTs. RESULTS Punctual spontaneous beating was seen in the cardiac patch at the first day of culture and more beating areas were seen thereafter. Areas with stronger and stronger beating and asynchronous beating were seen at the third day. The patch came to rhythmic synchronous beating at the second day after stretching. HE staining revealed that cardiac myocytes within the cardiac patch resembled those of the native adult cardiac tissue in morphology. Transmission electron microscopy revealed that the cardiac myocytes within the patch contained abundant myofibrils, clearly defined sarcomeres and Z lines. Histological and immunohistochemical analysis also showed more positive cardiac myocytes. CONCLUSION The method described in this study is helpful in constructing tissue engineered cardiac patch.

²Î¿¼ÎÄÏ×/References

£Û1£Ý Zimmermann WH, Eschenhagen T.Cardiac tissue engineering for replacement therapy£ÛJ£Ý. Heart Fail Rev,2003, 8(3):259-269.

£Û2£Ý Shimizu T,Yamato M,Isoi Y,et al. Fabrication of pulsatile cardiac tissue grafts using a novel 3ª²dimensional cell sheet manipulation technique and temperatureª²responsive cell culture suface£ÛJ£Ý. Circ Res,2002,90(3):e40-e48.

£Û3£Ý ѦÇìϲ. ÌåÍâÅàÑøµÄÔ­ÀíÓë¼¼Êõ£ÛM£Ý. ±±¾©:¿Æѧ³ö°æÉç,2001.20.

£Û4£Ý Li RK, Yau TM, Weisel RD,et al.Construction of a bioengineered cardiac graft£ÛJ£Ý. J Thorac Cardiovasc Surg,2000,119(2):368-375.

£Û5£ÝÎľþ,Áõ³ΰ ,·¶ÔÆ,µÈ. Ò»ÖÖÐļ¡Ï¸°ûÌ滻ʵÑé¼¼ÊõµÄÑо¿£ÛJ£Ý.ÐÄÔàÔÓÖ¾,2005,17(5):445-446.

£Û6£Ý Fink C,Ergun S, Kralisch D,et al. Chronic stretch of engineered heart tissue induces hypertrophy and functional improvement£ÛJ£Ý. FASEB J,2000,14(5):669-679.

£Û7£Ý Carrier RL, Papadaki M, Rupnick M, et al. Cardiac tissue engineering: cell seeding, cultivation parameters, and tissue construct characterization£ÛJ£Ý. Biotechnol Bioeng,1999,64(5):580-589.

£Û8£Ý Zimmermann WH, Schneiderbanger K, Schubert P,et al. Tissue Engineering of a differentiated cardiac muscle construct£ÛJ£Ý. Circ Rese,2002,90(2):223-230.

±¸×¢/Memo

±¸×¢/Memo:

ÊÕ¸åÈÕÆÚ£º2006-03-10.»ù½ðÏîÄ¿£º¾ü¶Ó¡°Ê®Î塱ҽÁÆÎÀÉú¿ÆÑлù½ðÏîÄ¿×ÊÖú£¨No.01MB126£©Í¨Ñ¶×÷ÕߣºÖ£Ç¿Ý¥£¬Ö÷ÈÎҽʦ£¬Ö÷Òª´ÓÊÂÐÄÂÉʧ³£µÄ»ù´¡ºÍÁÙ´²Ñо¿ Tel£º(029)84777422 Email:qingshu@fmmu.edu.cn ×÷Õß¼ò½é£º³£º£Ï¼£¬Ë¶Ê¿Éú Tel: (029)84777123 Email:chx8432@163.com

³£Óù¦ÄÜ

¸üÐÂÈÕÆÚ/Last Update: