U. Hibner scite author profile

The tumor suppressor protein p53 is ubiquitously expressed as a major isoform of 53 kD, but several forms of lower molecular weight have been observed. Here, we describe a new isoform, DN-p53, produced by internal initiation of translation at codon 40 and lacking the N-terminal first transactivation domain. This isoform has impaired transcriptional activation capacity, and does not complex with the p53 regulatory protein Mdm2. Furthermore, DN-p53 oligomerizes with full-length p53 (FL-p53) and negatively regulates its transcriptional and growth-suppressive activities. Consistent with the lack of Mdm2 binding, DN-p53 does not accumulate in response to DNA-damage, suggesting that this isoform is not involved in the response to genotoxic stress. However, in serum-starved cells expressing wild-type p53, DN-p53 becomes the predominant p53 form during the synchronous progression into S phase after serum stimulation. These results suggest that DN-p53 may play a role as a transient, negative regulator of p53 during cell cycle progression.

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Heterogeneity of B Lineage Acute Lymphoblastic Leukemias (B-ALL) with Regard to their in Vitro Spontaneous Proliferation, Growth Factor Response and BCL-2 Expression

Pontvert-Delucq

Hibner

Vilmer³

et al. 1996

Leukemia & Lymphoma

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The spontaneous proliferation and the effects of 8 various growth factors (GF) were evaluated on leukemic cells from 27 patients with B-lineage ALL. Two groups of ALLs were distinguished. ALLs from group I (21 patients) exhibited a low spontaneous proliferative rate and were stimulated by IL-3 + IL-7 +/- SCF and/or LIF, while ALLs from group II (6 patients) had a high spontaneous proliferative rate and did no longer require this combination of GFs for proliferation. No effect of bFGF, IGF-I, IL-10 and IL-11 alone or in combination, was observed. Such differences in the behaviour of B-ALLs indicated that the GF requirement of ALL blasts was not related to the presence of serum in the culture nor to the pattern of reactivity of ALL blasts for B lymphoid markers or CD34 antigen. Furthermore, we showed in 1/9 cases that high proliferation might be due to an overexpression of the bcl-2 proto-oncogene and to the acquisition of an autocrine secretion.

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Inhibition of RHO GTPases delineates a novel P53‐dependent apoptotic pathway

Roux

Lassus

Zugasti

et al. 1999

Biology of the Cell

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U. Hibner

ΔN-p53, a natural isoform of p53 lacking the first transactivation domain, counteracts growth suppression by wild-type p53

Heterogeneity of B Lineage Acute Lymphoblastic Leukemias (B-ALL) with Regard to their in Vitro Spontaneous Proliferation, Growth Factor Response and BCL-2 Expression

Inhibition of RHO GTPases delineates a novel P53‐dependent apoptotic pathway

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