Cyclin-Dependent Kinase-2 in the Birth and Death of Cardiac Muscle Cells

Table of Contents | Next Article »

Circulation Research. 2001;88:367-369

This Article

	Full Text
	Full Text (PDF)
	Alert me when this article is cited
	Alert me if a correction is posted
	Citation Map

Services

	Email this article to a friend
	Similar articles in this journal
	Similar articles in PubMed
	Alert me to new issues of the journal
	Download to citation manager
	Request Permissions

Citing Articles

	Citing Articles via HighWire
	Citing Articles via Google Scholar

Google Scholar

	Articles by Schneider, M. D.
	Articles by MacLellan, W. R.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Schneider, M. D.
	Articles by MacLellan, W. R.

Related Collections

	Apoptosis
	Cell biology/structural biology
	Gene expression
	Gene regulation
	Genetically altered mice

(Circulation Research. 2001;88:367.)
© 2001 American Heart Association, Inc.

Editorial

Cyclin-Dependent Kinase-2 in the Birth and Death of Cardiac Muscle Cells

Michael D. Schneider, W. Robb MacLellan

From the Center for Cardiovascular Development, Departments of Medicine, Molecular and Cellular Biology, and Molecular Physiology & Biophysics (M.D.S.), Baylor College of Medicine, Houston, Tex, and the Cardiovascular Research Laboratories, Department of Medicine (W.R.M.), UCLA School of Medicine, Los Angeles, Calif.

Correspondence to Michael D. Schneider, MD, Molecular Cardiology Unit, Baylor College of Medicine, One Baylor Plaza, Room 506C, Houston, TX 77030. E-mail michaels@bcm.tmc.edu

Key Words: apoptosis • cell cycle • cyclin • cyclin-dependent kinase • cardiac muscle

Introduction

The proliferative cell cycle in both vertebrates and much simplerorganisms entails the transduction of mitogenic signals to cyclicallyexpressed proteins known as cyclins and, hence, to their catalyticallyactive targets, the cyclin-dependent protein kinases (cdks).¹² In yeast, a single kinase, cdc28, suffices to partner withall of the cyclins, which are expressed sequentially in theG1 (cln 1/2/3), S (clb 5/6), and G2/M phases of the cycle, respectively.In mammals, by contrast, D-type cyclins in G1 partner with cdk4/6,cyclins E and A sequentially partner with cdk2 in S phase, andcyclin B interacts with cdc2 for entry into M phase. Whereasone family of cdk inhibitors is specific for cdk4/6 (the INK4family, comprising p15, p16, p18, and p19), a second, the Cip/Kipfamily, has much broader activity, inhibiting cdk2 and cdc2in addition. Activation of the cell cycle through inductionof cyclin D occurs in large part by the titration of Cip/Kipproteins away from cdk2 to the cyclin D–cdk complexes. Substratesof primary importance to the actions of cdk4/6 are the retinoblastomafamily of pocket proteins, whereas much less is known aboutthe substrates for cdk2, although some have been identified.³ One source of positive feedback within this process is thatphosphorylation by cdc28 and cdk2 can promote the degradationof cdk inhibitors using the ubiquitin-proteasome pathway. Asecond source is that cdk2, whose enzymatic activation thusdepends on cdk4/6, also phosphorylates pocket proteins in sequentialor processive fashion. In addition, the mitogen-induced transcriptionfactor Myc . . . [Full Text of this Article]

This article has been cited by other articles:

S. E. Hardt and J. Sadoshima
Glycogen Synthase Kinase-3{beta}: A Novel Regulator of Cardiac Hypertrophy and Development
Circ. Res., May 31, 2002; 90(10): 1055 - 1063.
[Abstract] [Full Text] [PDF]

M. D. Grounds, J. D. White, N. Rosenthal, and M. A. Bogoyevitch
The Role of Stem Cells in Skeletal and Cardiac Muscle Repair
J. Histochem. Cytochem., May 1, 2002; 50(5): 589 - 610.
[Abstract] [Full Text] [PDF]

				M. D. Grounds, J. D. White, N. Rosenthal, and M. A. Bogoyevitch The Role of Stem Cells in Skeletal and Cardiac Muscle Repair J. Histochem. Cytochem., May 1, 2002; 50(5): 589 - 610. [Abstract] [Full Text] [PDF]