Mobility Within the Nucleus and Neighboring Cytosol Is a Key Feature of Prothymosin-α

Enkemann, Steven A.; Ward, Rita D.; Berger, Shelby L.

doi:10.1177/002215540004801005

Cited by 30 publications

(30 citation statements)

References 63 publications

(86 reference statements)

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“…On the other hand, monoclonal antibodies are usually characterized by rather low affinity for the corresponding antigen, and consequently, they are also difficult to apply to the development of sensitive competitive immunoassays. This is probably true for the few monoclonals for ProTa reported until now in the literature (Staehli et al 1983;Sukhacheva et al 2002); as a consequence, few immunoassays have been reported for a thymosins and even fewer have been applied to the analysis of biological samples (Panneerselvam et al 1987;Tsitsiloni et al 1994;Costopoulou et al 1998;Mitani et al 2000), whereas their quantitative experimental results seem to vary and therefore have been approached with caution by some researchers (Enkemann et al 2000b). However, provided that their specificity is appropriate, carefully selected antibodies for ProTa may be of great value for certain clinical applications and especially for the immunostaining of tissue samples, in which they can be used in excess.…”

Section: Discussionmentioning

confidence: 99%

“…We strongly believe that the ProTa molecule does behave in a tricky way in the Western blot (Freire et al 2002;Lal et al 2005), and the slightest changes in the experimental conditions may greatly affect its immobilization onto the membrane, which is probably the main reason for the often reported poor Western blotting results. However, under Enkemann et al (2000b), who used COS-1 and NIH3T3 cells transfected with genes of epitope-tagged ProTa proteins in combination with antibodies against the epitope tags. The intensity of the fluorescent signal was stronger in the cancer cells than in normal ones.…”

Section: Discussionmentioning

confidence: 99%

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Immunocytological and Preliminary Immunohistochemical Studies of Prothymosin α, a Human Cancer–associated Polypeptide, With a Well-characterized Polyclonal Antibody

Klimentzou

Drougou

Fehrenbacher

et al. 2008

J Histochem Cytochem.

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Prothymosin α (ProTα) is a nuclear polypeptide of great biological and, possibly clinical, importance, because its expression levels have been associated with early diagnosis/prognosis of human cancer. It is therefore interesting to raise easily available and cost-effective antibodies that would be applied to develop reliable ProTα immunodiagnostics. In this study, New Zealand white rabbits and laying hens were parallel immunized against intact ProTα or the synthetic fragments ProTα[1-28], ProTα[87-109], and ProTα[101-109], all conjugated to keyhole limpet hemocyanin (KLH). The corresponding antibodies G and Y were immunochemically evaluated in parallel with ELISA and Western blot systems and applied to fluorescence immunocytology experiments using various cancer cell lines and normal cells. The antibody G raised against ProTα[101-109]/KLH had excellent functional characteristics in the Western blot and immunocytology experiments, where the fluorescent signal was almost exclusively shown in the cell nucleus independently of the cells assayed. The above antibody has been applied to preliminary IHC staining of human cancer prostate tissues, leading to a high percentage of clearly and intensively stained nuclei in the adenocarcinoma tissue; this antibody can be further used in cancer tissue immunostaining and in research concerning the role of ProTa in tumorigenesis.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Immunocytological and Preliminary Immunohistochemical Studies of Prothymosin α, a Human Cancer–associated Polypeptide, With a Well-characterized Polyclonal Antibody

Klimentzou

Drougou

Fehrenbacher

et al. 2008

J Histochem Cytochem.

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“…The use of cell lines with different genetic alterations are likely to be important, and cell lines with an impaired p53 pathway may predominantly proliferate in response to PTMA. It is furthermore very likely that protein tags significantly alter results for PTMA, such as subcellular localization and biological functions (52,53). We have tested NH 2 -terminally tagged PTMA (FLAG, Myc, and glutathione S-transferase tags) in p53 reporter gene assays and found that none were able to stimulate p53 activity, despite expression levels similar to native PTMA.…”

Section: Discussionmentioning

confidence: 99%

Overexpression of the Oncoprotein Prothymosin α Triggers a p53 Response that Involves p53 Acetylation

Kobayashi

Wang²,

Maezawa

et al. 2006

Cancer Research

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Activation of the tumor suppressor protein p53 is a critical cellular response to various stress stimuli and to inappropriate activity of growth-promoting proteins, such as Myc, Ras, E2F, and B-catenin. Protein stability and transcriptional activity of p53 are modulated by protein-protein interactions and post-translational modifications, including acetylation. Here, we show that inappropriate activity of prothymosin A (PTMA), an oncoprotein overexpressed in human cancers, triggers a p53 response. Overexpression of PTMA enhanced p53 transcriptional activity in reporter gene assays for p53 target gene promoters hdm2, p21, and cyclin G. Overexpressed PTMA resulted in increased mRNA and protein levels for endogenous p53 target genes, hdm2 and p21, and in growth suppression. In contrast, reduction of endogenous PTMA through RNA interference decreased p53 transcriptional activity. Histone acetyltransferases (HATs) act as p53 coactivators and acetylate p53. PTMA, known to interact with HATs, led to increased levels of acetylated p53. PTMA did not increase the transcriptional activity of an acetylation-deficient p53 mutant, suggesting that p53 acetylation is an indispensable part of the p53 response to PTMA. Chromatin immunoprecipitation assays showed that excess PTMA associates with the p21 promoter and results in increased levels of acetylated p53 at the p21 promoter. Our findings indicate that overexpressed PTMA elicits a p53 response that involves p53 acetylation. (Cancer Res 2006; 66(6): 3137-44)

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“…For these studies we used immunofluorescence staining to determine if the same cells that express PTa are also proliferating. PTa has been proposed to move between nuclear and cytoplasmic compartments (Enkemann et al, 2000). However the relative importance of nuclear and cytoplasmic localization on its proliferative effects has not been examined.…”

Section: Determination Of the Relevance Of Era Regulation Of Pta Tranmentioning

confidence: 99%

Estrogen Regulation of Prothymosin Alpha

Montano¹

2003

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Mobility Within the Nucleus and Neighboring Cytosol Is a Key Feature of Prothymosin-α

Cited by 30 publications

References 63 publications

Immunocytological and Preliminary Immunohistochemical Studies of Prothymosin α, a Human Cancer–associated Polypeptide, With a Well-characterized Polyclonal Antibody

Immunocytological and Preliminary Immunohistochemical Studies of Prothymosin α, a Human Cancer–associated Polypeptide, With a Well-characterized Polyclonal Antibody

Overexpression of the Oncoprotein Prothymosin α Triggers a p53 Response that Involves p53 Acetylation

Estrogen Regulation of Prothymosin Alpha

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