Abrogation of p27  by cDNA Antisense Suppresses Quiescence (G0 State) in Fibroblasts

Rivard, Nathalie; L’Allemain, Gilles; Bártek, Jiří; Pouysségur, Jacques

doi:10.1074/jbc.271.31.18337

Cited by 200 publications

(161 citation statements)

References 43 publications

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“…These investigators did not, however, examine possible e ects of overexpression of p27 on di erentiation. Increased expression of p27 can enhance exit from the cell cycle (Hengst and Reed, 1996;Rivard et al, 1996). The ability of p27 to enhance the differentiation of HT29 cells observed in the present studies is consistent with previous evidence that the levels of this protein increase in HL60 promyelocyctic leukemia cells (Hengst and Reed, 1996) or neuroblastoma cells (Kranenburg et al, 1995) that are induced to di erentiate by vitamin D3 or DMSO, respectively.…”

Section: Discussionsupporting

confidence: 92%

Comparative effects of overexpression of p27Kip1 and p21Cip1/Waf1 on growth and differentiation in human colon carcinoma cells

et al. 1999

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Recent studies have shown that decreased expression of p27 Kip1 is associated with high grade tumors and an unfavorable prognosis in several types of human cancer. To clarify the role of p27 Kip1 in colon cancer, we have overexpressed this protein in the HT29 colon cancer cell line. The derivatives displayed an increase in the p27 Kip1 protein in cyclin E/CDK2 immunoprecipitates and a decrease in cyclin E-associated kinase activity when compared to vector control clones, providing evidence that the overexpressed protein was functional. Clones with a high level of p27 Kip1 displayed partial growth inhibition in monolayer culture and a decrease in plating e ciency, even though they expressed increased levels of the cyclin D1 protein. Using alkaline phosphatase expression as a marker, we found that the p27 Kip1 overexpressor clones displayed a 2 ± 3-fold increase in sensitivity to induction of di erentiation by 2 mM sodium butyrate. In contrast to these results, derivatives of HT29 cells that stably overexpressed p21 Cip1/Waf1 displayed decreased sensitivity to the induction of di erentiation. These ®ndings may explain why decreased levels of p27 Kip1 in certain human cancers is associated with high grade (poorly di erentiated) tumors, and suggest that strategies that increase the level of p27 Kip1 may be useful in cancer therapy.

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Section: Discussionsupporting

confidence: 92%

Comparative effects of overexpression of p27Kip1 and p21Cip1/Waf1 on growth and differentiation in human colon carcinoma cells

et al. 1999

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“…As a consequence, Kip1 À cells lack the G1pm phase. In simulations (not shown), cells deprived of GF or treated with CHX keep on proliferating, which agrees with the observation that Kip1 À cells are less serum-dependent than Kip1 + cells (Coats et al, 1996;Rivard et al, 1996).…”

Section: Kip1 àsupporting

confidence: 84%

A model for restriction point control of the mammalian cell cycle

Novák

Tyson

2004

Journal of Theoretical Biology

267

273

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“…It is well documented that p27 restricts entry of cells into S phase by binding and inhibiting the activity of cyclin/ CDK complexes Sherr and Roberts, 1999). Overexpression of p27 blocks cells in G1 while suppression of p27 mRNA translation by antisense oligonucleotides maintains cells in a proliferative state (Coats et al, 1996;Rivard et al, 1996). Although p27 protein levels clearly¯uctuate during progression through the cell cycle, p27 mRNA levels remain relatively constant (Hengst and Reed, 1996).…”

Section: Discussionmentioning

confidence: 99%

p27Kip1-deficient mice exhibit accelerated growth hormone-releasing hormone (GHRH)-induced somatotrope proliferation and adenoma formation

et al. 2000

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p27 Kip1 (p27) controls cell cycle progression by binding to and inhibiting the activity of cyclin dependent kinases. Disruption of the p27 gene in mice (p277/7) results in increased body growth with a disproportionate enlargement of the spleen, thymus, testis, ovary and pituitary. The increase in pituitary size is due to selective hyperplasia of the intermediate lobe (IL) while the anterior lobe (AL) is not overtly a ected. p27 heterozygous mice (p27+/7), as well as p277/7 mice, are hypersensitive to radiation-and chemical-induced tumors compared to wildtype (p27+/+) littermates. Therefore, unlike classical tumor suppressors, only a reduction in p27 levels is necessary to predispose tissues to secondary tumor promoters. Consistent with these studies is the fact that the p27 gene sequence and mRNA levels appear normal in human pituitary adenomas while p27 protein levels are decreased. Therefore, a reduction in p27 levels could be su cient to sensitize pituitary cells to tumorigenic factors. To test this hypothesis, metallothionein promoter-driven, human growth hormone-releasing hormone (MT-hGHRH) transgenic mice, that exhibit somatotrope hyperplasia before 9 months of age and subsequent adenoma formation with 30 ± 40% penetrance, were crossbred with p27+/7 mice for two successive generations to produce p27+/+, p27+/7 and p277/7 mice that expressed the hGHRH transgene. At 10 ± 12 weeks of age, p277/7 and p27+/+, hGHRH mice were larger than their p27+/+ littermates and displayed characteristic hyperplasia of the IL and AL, respectively. Expression of the hGHRH transgene in both p27+/7 and p277/7 mice selectively expanded the population of somatotropes within the AL, where pituitaries of p27+/7, hGHRH and p277/7, hGHRH mice were two-and ®vefold larger than p27+/+, hGHRH pituitaries, respectively. There was also a synergistic e ect of hGHRH transgene expression and p27-de®ciency on liver, spleen and ovarian growth. At 6 ± 8 months of age, 83% of p27+/7, hGHRH mice displayed macroscopic AL adenomas (4100 mg), while all pituitaries from p27+/+, hGHRH mice remained hyperplastic (520 mg). In contrast to the dramatic e ects of p27-de®ciency on hGHRH-induced organ growth, elimination of p53, by crossbreeding MT-hGHRH mice to p53-de®cient mice, did not augment the hyperplastic/ tumorigenic e ects of hGHRH transgene expression.Taken together these results demonstrate that a reduction in p27 expression is su cient to sensitize somatotropes to the proliferative actions of excess GHRH, resulting in the earlier appearance and increased penetrance of hGHRH-induced pituitary tumors.

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Abrogation of p27 by cDNA Antisense Suppresses Quiescence (G0 State) in Fibroblasts

Cited by 200 publications

References 43 publications

Comparative effects of overexpression of p27Kip1 and p21Cip1/Waf1 on growth and differentiation in human colon carcinoma cells

Comparative effects of overexpression of p27Kip1 and p21Cip1/Waf1 on growth and differentiation in human colon carcinoma cells

A model for restriction point control of the mammalian cell cycle

p27Kip1-deficient mice exhibit accelerated growth hormone-releasing hormone (GHRH)-induced somatotrope proliferation and adenoma formation

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