TY - JOUR
T1 - Regulation of cyclin dependent kinase inhibitor proteins during neonatal cerebella development
AU - Watanabe, Genichi
AU - Pena, Pilar
AU - Shambaugh, George E.
AU - Haines, George K.
AU - Pestell, Richard G.
N1 - Funding Information:
We thank Dr. Li-Huei Tsai, Dr. M. Nicolic, Dr. B. Dynlacht and Dr. L. Binder for gifts of antibodies and cell lines, and Dr. A. Koch and Dr. E. Mugnaini for their expert advice. This work was supported in part by the NIH FIRST award 1R29CA70897 and grant R55CA75503 (to R.G.P.) and Merit Reviews from the Department of Veterans Affairs (G.E.S.). Work at the Albert Einstein College of Medicine was also supported by Cancer Center Core National Institute of Health grant 5-P30-CA13330-26.
PY - 1998/6/15
Y1 - 1998/6/15
N2 - The cyclin dependent kinase holoenzymes (CDKs), composed of catalytic (cdk) and regulatory (cyclin) subunits, promote cellular proliferation and are inhibited by cyclin dependent kinase inhibitor proteins (CDKIs). The CDKIs include the Ink4 family (p15(Ink4b), p16(Ink4a), p18(Ink4c), p19(Ink4d)) and the KIP family (p21(Cip1) and p27(Kip1)). The sustained induction of p21 and p18 during myogenesis implicates these CDKI in maintaining cellular differentiation. Herein we examined the CDK (cyclin D1, cdk5) and CDKI expression profiles during the first 24 days of postnatal rat cerebella development. Cdk5 abundance increased and cyclin D1 decreased from day 9 through to adulthood. The CDKIs increased transiently during differentiation. p27 increased 20-fold between days 4 and 24, whereas p21 rose twofold between 6 to 11 days. p19, p18 and p16 increased approximately two- to threefold, falling to low levels in the adult. Immunostaining of cyclin D1 was localized in the external granular cells, whereas p27, was found primarily in the Purkinje cells. The period of maximal differentiation between days 9 to 13 was associated with a change in p21 and p16 staining from the external granular and Purkinje cells to a primarily Purkinje cell distribution. Protein-calorie malnutrition, which was previously shown to arrest rat cerebella development, reduced cyclin D1 kinase activity and p27 levels. However, p16 and p21 levels were unchanged. We conclude that the CDKIs are induced with distinct kinetics in specific cell types and respond differentially to growth factors during cerebella development, suggesting discrete roles for these proteins in normal cerebella development.
AB - The cyclin dependent kinase holoenzymes (CDKs), composed of catalytic (cdk) and regulatory (cyclin) subunits, promote cellular proliferation and are inhibited by cyclin dependent kinase inhibitor proteins (CDKIs). The CDKIs include the Ink4 family (p15(Ink4b), p16(Ink4a), p18(Ink4c), p19(Ink4d)) and the KIP family (p21(Cip1) and p27(Kip1)). The sustained induction of p21 and p18 during myogenesis implicates these CDKI in maintaining cellular differentiation. Herein we examined the CDK (cyclin D1, cdk5) and CDKI expression profiles during the first 24 days of postnatal rat cerebella development. Cdk5 abundance increased and cyclin D1 decreased from day 9 through to adulthood. The CDKIs increased transiently during differentiation. p27 increased 20-fold between days 4 and 24, whereas p21 rose twofold between 6 to 11 days. p19, p18 and p16 increased approximately two- to threefold, falling to low levels in the adult. Immunostaining of cyclin D1 was localized in the external granular cells, whereas p27, was found primarily in the Purkinje cells. The period of maximal differentiation between days 9 to 13 was associated with a change in p21 and p16 staining from the external granular and Purkinje cells to a primarily Purkinje cell distribution. Protein-calorie malnutrition, which was previously shown to arrest rat cerebella development, reduced cyclin D1 kinase activity and p27 levels. However, p16 and p21 levels were unchanged. We conclude that the CDKIs are induced with distinct kinetics in specific cell types and respond differentially to growth factors during cerebella development, suggesting discrete roles for these proteins in normal cerebella development.
KW - Cell-cycle
KW - Cerebella
KW - Cyclin dependent kinase inhibitor protein
UR - http://www.scopus.com/inward/record.url?scp=0032526830&partnerID=8YFLogxK
U2 - 10.1016/S0165-3806(98)00032-7
DO - 10.1016/S0165-3806(98)00032-7
M3 - Article
C2 - 9693786
AN - SCOPUS:0032526830
SN - 0165-3806
VL - 108
SP - 77
EP - 87
JO - Developmental Brain Research
JF - Developmental Brain Research
IS - 1-2
ER -