Assessment of cardiomyocyte DNA synthesis in normal and injured adult mouse hearts

被引：235

作者：

Soonpaa, MH ^{[1
]}

Field, LJ ^{[1
]}

机构：

[1] Indiana Univ, Sch Med, Krannert Inst Cardiol, Indianapolis, IN 46202 USA

来源：

AMERICAN JOURNAL OF PHYSIOLOGY-HEART AND CIRCULATORY PHYSIOLOGY | 1997年 / 272卷 / 01期

关键词：

terminal differentiation; myocardial regeneration; binucleation; nuclear ploidy; MYOCYTE CELLULAR HYPERTROPHY; NUCLEAR MITOTIC DIVISION; CARDIAC-MUSCLE-CELLS; AUTOCRINE SYSTEM; RATS; REPLICATION; HYPERPLASIA; CONTRIBUTE; INFARCTION; MYOCARDIUM;

D O I：

10.1152/ajpheart.1997.272.1.H220

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Cardiomyocyte DNA synthesis was examined in normal and injured adult mouse hearts. In preliminary studies DNA synthesis was monitored by [H-3]thymidine incorporation, followed by autoradiographic analysis of dispersed cell preparations. No synthetic cells mere identified when 20,000 ventricular cardiomyocytes from normal adult hearts were examined. A high throughput assay was developed to establish the actual labeling index for the adult mouse heart. The assay utilized [H-3]thymidine incorporation in transgenic mice which expressed a nuclear-localized beta-galactosidase (beta-Gal) reporter gene exclusively in cardiac myocytes. Cardiomyocyte DNA synthesis was evidenced by colocalization of beta-Gal activity and silver grains in autoradiograms of histological sections. Examination of 180,000 ventricular cardiomyocyte nuclei from normal adult transgenic mice identified a single synthetic nucleus, suggesting a maximum labeling index of 0.0005%. Cardiomyocyte DNA synthesis was next examined in hearts injured by focal cauterization of the left ventricular fi ee wall. Only three synthetic nuclei were identified when 36,000 cardiomyocyte nuclei in the perine-crotic zone of the injured heart were examined. No additional synthetic nuclei were identified when 180,000 nuclei in regions distal to the necrotic zone were examined. These data confirm that cardiomyocyte DNA synthesis in the adult mouse heart is extremely rare and provide baseline data for analyses in genetically modified animals.

引用

页码：H220 / H226

页数：7

共 19 条

[1]

Bullock G.R., 1982, Techniques in immunocytochemistry

[2] ACQUISITION OF MULTIPLE NUCLEI AND THE ACTIVITY OF DNA POLYMERASE-ALPHA AND REINITIATION OF DNA-REPLICATION IN TERMINALLY DIFFERENTIATED ADULT CARDIAC-MUSCLE-CELLS IN CULTURE [J].

CLAYCOMB, WC ;

BRADSHAW, HD .

DEVELOPMENTAL BIOLOGY, 1983, 99 (02) :331-337

[3] MYOCYTE CELLULAR HYPERPLASIA AND MYOCYTE CELLULAR HYPERTROPHY CONTRIBUTE TO CHRONIC VENTRICULAR REMODELING IN CORONARY-ARTERY NARROWING-INDUCED CARDIOMYOPATHY IN RATS [J].

KAJSTURA, J ;

ZHANG, X ;

REISS, K ;

SZOKE, E ;

LI, P ;

LAGRASTA, C ;

CHENG, W ;

DARZYNKIEWICZ, Z ;

OLIVETTI, G ;

ANVERSA, P .

CIRCULATION RESEARCH, 1994, 74 (03) :383-400

[4] NUCLEAR-DNA CONTENT AND NUCLEATION PATTERNS IN RAT CARDIAC MYOCYTES FROM DIFFERENT MODELS OF CARDIAC-HYPERTROPHY [J].

KELLERMAN, S ;

MOORE, JA ;

ZIERHUT, W ;

ZIMMER, HG ;

CAMPBELL, J ;

GERDES, AM .

JOURNAL OF MOLECULAR AND CELLULAR CARDIOLOGY, 1992, 24 (05) :497-505

[5] ZUNAHME DNS-SYNTHETISIERENDER HERZMUSKELKERNE DURCH TRAINING [J].

KUNZE, WP ;

CITOLER, P .

NATURWISSENSCHAFTEN, 1967, 54 (20) :540-+

[6] OXYRADICAL-INDUCED ANTIOXIDANT AND LIPID CHANGES IN CULTURED HUMAN CARDIOMYOCYTES [J].

LI, RK ;

SHAIKH, N ;

WEISEL, RD ;

WILLIAMS, WG ;

MICKLE, DAG .

AMERICAN JOURNAL OF PHYSIOLOGY, 1994, 266 (06) :H2204-H2211

[7] PROLIFERATING CELL NUCLEAR ANTIGEN IN DEVELOPING AND ADULT-RAT CARDIAC-MUSCLE-CELLS [J].

MARINO, TA ;

HALDAR, S ;

WILLIAMSON, EC ;

BEAVERSON, K ;

WALTER, RA ;

MARINO, DR ;

BEATTY, C ;

LIPSON, KE .

CIRCULATION RESEARCH, 1991, 69 (05) :1353-1360

[8] DNA-SYNTHESIS IN RAT-HEART CELLS AFTER INJURY AND THE REGENERATION OF MYOCARDIA [J].

NAG, AC ;

CAREY, TR ;

CHENG, M .

TISSUE & CELL, 1983, 15 (04) :597-613

[9]

OBERPRILLER JO, 1991, DEV REGENERATIVE POT, P463

[10]

OLIVETTI G, 1992, AM J PATHOL, V141, P227

← 1 2 →