2001
DOI: 10.1096/fj.00-0416com
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Cyclin D1 is an early target in hepatocyte proliferation induced by thyroid hormone (T3)

Abstract: The thyroid hormone (T3) affects cell growth, differentiation, and regulates metabolic functions via its interaction with the thyroid hormone nuclear receptors (TRs). The mechanism by which TRs mediate cell growth is unknown. To investigate the mechanisms responsible for the mitogenic effect of T3, we have determined changes in activation of transcription factors, mRNA levels of immediate early genes, and levels of proteins involved in the progression from G1 to S phase of the cell cycle. We show that hepatocy… Show more

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Cited by 125 publications
(112 citation statements)
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“…Specifically, cyclin D1 has been shown to regulate a number of sequence-specific transcription factors, including C/EBPb (Lamb et al, 2003), STAT3 (Bienvenu et al, 2001), DMP1 (Inoue and Sherr, 1998), and BETA2/NeuroD (Ratineau et al, 2002). The largest class of transcription factors regulated by cyclin D1 belong to the nuclear receptor superfamily, and include the estrogen receptor (Zwijsen et al, 1998;Lamb et al, 2000), androgen receptor (Knudsen et al, 1999;Reutens et al, 2001;Petre et al, 2002;Burd et al, 2005), thyroid hormone receptor (Pibiri et al, 2001), and peroxisome proliferator activated receptor-g (Qin et al, 2003). In many cases cyclin D1 was shown to directly associate with the transcription factors, independent of CDK4 association, and modify transcription factor action through cell-cycle independent mechanisms.…”
Section: Cell Cyclementioning
confidence: 99%
“…Specifically, cyclin D1 has been shown to regulate a number of sequence-specific transcription factors, including C/EBPb (Lamb et al, 2003), STAT3 (Bienvenu et al, 2001), DMP1 (Inoue and Sherr, 1998), and BETA2/NeuroD (Ratineau et al, 2002). The largest class of transcription factors regulated by cyclin D1 belong to the nuclear receptor superfamily, and include the estrogen receptor (Zwijsen et al, 1998;Lamb et al, 2000), androgen receptor (Knudsen et al, 1999;Reutens et al, 2001;Petre et al, 2002;Burd et al, 2005), thyroid hormone receptor (Pibiri et al, 2001), and peroxisome proliferator activated receptor-g (Qin et al, 2003). In many cases cyclin D1 was shown to directly associate with the transcription factors, independent of CDK4 association, and modify transcription factor action through cell-cycle independent mechanisms.…”
Section: Cell Cyclementioning
confidence: 99%
“…T 3 acts via its nuclear receptors which are ligand-dependent nuclear transcription factors, 24 causes an increase in cyclin D 1 mRNA and protein levels at an early phase of hepatocyte regeneration in rats, and in turn leads to transition of G 1 phase to the S phase of the cell cycle. 25 Thus, T 3 pretreatment may be considered as a potential non-invasive approach in the stimulation of hepatocyte proliferation for gene delivery experiments.…”
Section: Liposome-mediated Liver Gene Deliverymentioning
confidence: 99%
“…13 The finding that many hepatomitogens are ligands of nuclear receptors of the same superfamily led us to postulate that: (a) ligands of nuclear receptors could represent a novel class of liver mitogens; and, (b) signal transduction pathways involved in nuclear receptormediated hepatocyte proliferation could be different from those involved in liver regeneration and mediated by classical membrane-receptors. 4,14 It is now known that early changes such as activation of transcription factors (AP-1, NF-kB and STAT3, C/EBP) and increased expression of immediate early genes (c-fos, c-jun, c-myc, LRF-1, egr-1) or growth factors (TGF-a, HGF) considered to be essential for liver regeneration after two-thirds PH, are not required in nuclear receptormediated hepatocyte proliferation. 14 Hepatocyte proliferation induced by ligands of nuclear receptors is also TNF-a and IL-6-independent.…”
Section: Direct Hyperplasia Induced By Ligands Of Nuclear Receptorsmentioning
confidence: 99%
“…The accelerated entry into S phase, following treatment with TCPOBOP, nafenopin (a member of PPs family) and T3, is correlated with a very rapid induction of cyclin D1, suggesting that activation of this cyclin by ligands of nuclear receptors is an early critical event, rather than the results of a series of gene activations, as seen in the PH model. 14 Thus, an unified concept is emerging regarding the possible mechanisms of hepatocyte proliferation induced by several ligands of the nuclear receptors. Further studies to characterize molecular interactions between cyclin D1 gene and TRs, PPARs, CAR and possibly other nuclear hormone receptors may be critical to verify the validity of this concept.…”
Section: Direct Hyperplasia Induced By Ligands Of Nuclear Receptorsmentioning
confidence: 99%