The gene PC3<sup>TIS21/BTG2</sup>, prototype member of the PC3/BTG/TOB family: Regulator in control of cell growth, differentiation, and DNA repair?

Tirone, Felice

doi:10.1002/jcp.1062

Cited by 202 publications

(170 citation statements)

References 93 publications

(153 reference statements)

Supporting

Mentioning

159

Contrasting

Order By: Relevance

“…2). We further examine the expressions of RhoA (neurite extension [43]) and PC3 (neuronal birth [44]), resulting in no clear differences of their expression levels between the adult and embryonic NP cells. Expression of SCG10, enriched in the growth cones of the developing neurons [45], was rather decreased in the SVZ and WM cultures compared with that of E14 NP cells.…”

Section: Discussionmentioning

confidence: 99%

Generation of Functional Dopamine Neurons from Neural Precursor Cells Isolated from the Subventricular Zone and White Matter of the Adult Rat Brain Using Nurr1 Overexpression

et al. 2007

View full text Add to dashboard Cite

show abstract

Section: Discussionmentioning

confidence: 99%

Generation of Functional Dopamine Neurons from Neural Precursor Cells Isolated from the Subventricular Zone and White Matter of the Adult Rat Brain Using Nurr1 Overexpression

et al. 2007

View full text Add to dashboard Cite

show abstract

“…It has been suggested that Btg proteins exert cellular functions by interacting with transcriptional coactivators or corepressors, hence modulating their transcriptional activities (Matsuda et al, 2001;Tirone, 2001;Duriez et al, 2004;Lim, 2006). For example, it has been found that Btg2 impairs G1-S cell cyclephase progression by inhibiting cyclin D1 transcription (Guardavaccaro et al, 2000), that it can associate with HoxB9 (Prevot et al, 2000), and BMPregulated Smad1 and 8 (Park et al, 2004) to promote their transcriptional activity, and that it can enhance Math1 promoter activity (Canzoniere et al, 2004).…”

Section: Discussionmentioning

confidence: 99%

“…Btg/ Tob genes are a newly characterized family of cell cycle modulators (Guehenneux et al, 1997). Studies in different model systems suggest that they act as antiproliferative genes, they can promote cell differentiation and also regulate apoptosis and cellular senescence (Matsuda et al, 2001;Tirone, 2001;Duriez et al, 2004;Lim, 2006). Btg/Tob genes encode for a group of structurally related proteins, characterized by the presence of two novel and highly conserved domains ("antiproliferative" boxes A and B) located in the first 120 residues of the protein (Guehenneux et al, 1997;Guardavaccaro et al, 2000).…”

Section: Introductionmentioning

confidence: 99%

“…In spite of having similar N-terminal sequences and activities, BTG proteins are smaller than Tob proteins and both groups are generally considered as subfamilies (Matsuda et al, 2001;Tirone, 2001;Jia and Meng, 2007). The Btg2 gene was the first member to be identified, as an immediate response gene in mouse and rat, in two different cellular contexts.…”

Section: Introductionmentioning

confidence: 99%

“…Overexpression of Btg/Tob members in different cellular models have assigned them antriproliferative and/or pro-differentiative functions (reviewed in (Tirone, 2001;Duriez et al, 2004). Btg1 has been shown to modulate avian myoblast differentiation in vitro (Marchal et al, 1995;Rodier et al, 1999), and Btg2 can promote differentiation and survival of cultured-neural cells (Corrente et al, 2002;el-Ghissassi et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Btg1 and Btg2 gene expression during early chick development

Kamaid

Giráldez

2008

Developmental Dynamics

View full text Add to dashboard Cite

Btg/Tob genes encode for a new family of proteins with antiproliferative functions, which are also able to stimulate cell differentiation. Btg1 and Btg2 are the most closely related members in terms of gene sequence. We analyzed their expression patterns in avian embryos by in situ hybridization, from embryonic day 1 to 3. Btg1 was distinctively expressed in the Hensen's node, the notochord, the cardiogenic mesoderm, the lens vesicle, and in the apical ectodermal ridge and mesenchyme of the limb buds. On the other hand, Btg2 expression domains included the neural plate border, presomitic mesoderm, trigeminal placode, and mesonephros. Both genes were commonly expressed in the myotome, epibranchial placodes, and dorsal neural tube. The results suggest that Btg1 and Btg2 are involved in multiple developmental processes. Overlapping expression of Btg1 and Btg2 may imply redundant functions, but unique expression patterns suggest also differential regulation and function.

show abstract

Multiple interaction nodes define the postreplication repair response to UV‐induced DNA damage that is defective in melanomas and correlated with UV signature mutation load

et al. 2019

View full text Add to dashboard Cite

Ultraviolet radiation‐induced DNA mutations are a primary environmental driver of melanoma. The reason for this very high level of unrepaired DNA lesions leading to these mutations is still poorly understood. The primary DNA repair mechanism for UV‐induced lesions, that is, the nucleotide excision repair pathway, appears intact in most melanomas. We have previously reported a postreplication repair mechanism that is commonly defective in melanoma cell lines. Here we have used a genome‐wide approach to identify the components of this postreplication repair mechanism. We have used differential transcript polysome loading to identify transcripts that are associated with UV response, and then functionally assessed these to identify novel components of this repair and cell cycle checkpoint network. We have identified multiple interaction nodes, including global genomic nucleotide excision repair and homologous recombination repair, and previously unexpected MASTL pathway, as components of the response. Finally, we have used bioinformatics to assess the contribution of dysregulated expression of these pathways to the UV signature mutation load of a large melanoma cohort. We show that dysregulation of the pathway, especially the DNA damage repair components, are significant contributors to UV mutation load, and that dysregulation of the MASTL pathway appears to be a significant contributor to high UV signature mutation load.

show abstract

The gene PC3^TIS21/BTG2, prototype member of the PC3/BTG/TOB family: Regulator in control of cell growth, differentiation, and DNA repair?

Cited by 202 publications

References 93 publications

Generation of Functional Dopamine Neurons from Neural Precursor Cells Isolated from the Subventricular Zone and White Matter of the Adult Rat Brain Using Nurr1 Overexpression

Generation of Functional Dopamine Neurons from Neural Precursor Cells Isolated from the Subventricular Zone and White Matter of the Adult Rat Brain Using Nurr1 Overexpression

Btg1 and Btg2 gene expression during early chick development

Multiple interaction nodes define the postreplication repair response to UV‐induced DNA damage that is defective in melanomas and correlated with UV signature mutation load

Contact Info

Product

Resources

About

The gene PC3TIS21/BTG2, prototype member of the PC3/BTG/TOB family: Regulator in control of cell growth, differentiation, and DNA repair?

Cited by 202 publications

References 93 publications

Generation of Functional Dopamine Neurons from Neural Precursor Cells Isolated from the Subventricular Zone and White Matter of the Adult Rat Brain Using Nurr1 Overexpression

Generation of Functional Dopamine Neurons from Neural Precursor Cells Isolated from the Subventricular Zone and White Matter of the Adult Rat Brain Using Nurr1 Overexpression

Btg1 and Btg2 gene expression during early chick development

Multiple interaction nodes define the postreplication repair response to UV‐induced DNA damage that is defective in melanomas and correlated with UV signature mutation load

Contact Info

Product

Resources

About

The gene PC3^TIS21/BTG2, prototype member of the PC3/BTG/TOB family: Regulator in control of cell growth, differentiation, and DNA repair?