Expression of {alpha} and {beta} integrins during terminal differentiation of cardiomyocytes

doi:10.1016/S0008-6363(00)00140-1

Cardiovascular Research 2000 47(4):715-725; doi:10.1016/S0008-6363(00)00140-1
© 2000 by European Society of Cardiology

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Expression of ${alpha}$ and β integrins during terminal differentiation of cardiomyocytes

Niranjan Maitra^a, Irwin L. Flink^a^,*, Joseph J. Bahl^a and Eugene Morkin^a^,b

^aUniversity of Arizona Sarver Heart Center and Department of Medicine, 1501 N. Campbell Avenue, University of Arizona, Tucson, AZ 85724, USA
^bDepartment of Physiology and Pharmacology, 1501 N. Campbell Avenue, University of Arizona, Tucson, AZ 85724, USA

^* Corresponding author. Tel.: +1-520-626-6639; fax: +1-520-626-8408 iflink{at}u.arizona.edu

Background: In the myocardium, myocyte cell division is irreversiblyblocked shortly after birth. The signal that initiates cellcycle withdrawal is unknown. The purpose of this study was torelate changes in expression of β1 integrin and its associated ${alpha}$ subunits to cardiomyocyte cell cycle progression during thefetal-to-neonatal developmental transition in rat. Methods andresults: The developmental expression pattern and function ofβ1 integrin and several of its associated ${alpha}$ subunits wereexamined using reverse transcription (RT) polymerase chain reaction(PCR) and β1 blocking antibodies. During the fetal to neonataltransition, a dramatic shift occurred in the levels of β1and ${alpha}$ isoforms. At the 17-day fetal stage only β1A was present,which remained relatively constant until immediately after birththen decreased by 30% at the adult stage. By contrast, β1Dappeared at fetal day 18, increased at neonatal day 2, and afterwardsremained constant. This resulted in a ratio of β1A to β1Dof about 1:1 in the adult heart. The integrin β1-associatedsubunits, ${alpha}$ 3, ${alpha}$ 6, and ${alpha}$ 7, were expressed at extremely low levelsin 17-day fetal cardiomyocytes. After birth ${alpha}$ 3 and ${alpha}$ 6 transientlyincreased at the 2-day neonatal stage, while ${alpha}$ 7 isoforms B, C,and X2 progressively increased to the adult stage. Unlike skeletalmuscle cells, fluorescence-activated cell sorting analysis (FACS)showed no down regulation of the ${alpha}$ 5β1 fibronectin receptorduring cell cycle withdrawal. Treatment of cultured cardiomyocyteswith β1 blocking antibody inhibited the cell cycle in fetalbut not in neonatal cells. Conclusion: These results suggestthat progression through the cardiomyocyte cell cycle may bedependent upon cell attachment via integrin β1 and correlatewith changes that occur in β1 spliced variants and theirrespective ${alpha}$ isoforms.

KEYWORDS Cell culture/isolation; Developmental biology; Extracellular matrix; Myocytes

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Cardiovascular Research

Expression of and β integrins during terminal differentiation of cardiomyocytes

Expression of ${alpha}$ and β integrins during terminal differentiation of cardiomyocytes