| Autor: | Mila Jhamai, G. J. C. M. van den Bemd, Albert O. Brinkmann, G. T. G. Chang |
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| Rok vydání: | 2002 |
| Předmět: |
Pharmacology
Regulation of gene expression Cancer Research medicine.medical_specialty Programmed cell death medicine.drug_class Biochemistry (medical) Clinical Biochemistry Pharmaceutical Science Cell Biology Biology urologic and male genital diseases medicine.disease Androgen Prostate cancer medicine.anatomical_structure Endocrinology Prostate Cell culture Apoptosis Internal medicine medicine Cancer research Transcription factor |
| Zdroj: | APOPTOSIS. 7:13-21 |
| ISSN: | 1360-8185 |
| DOI: | 10.1023/a:1013504710343 |
| Popis: | Expression of death-signaling genes induces many biochemical cascades resulting in elimination of cells via apoptosis or programmed cell death. GC79/TRPS1 is a novel apoptosis associated gene that encodes a multitype zinc finger GATA-type transcription factor. Expression of GC79/TRPS1 is repressed in the rat ventral prostate and significantly elevated after androgen withdrawal by castration. Castration leads to regression of the prostate caused by apoptosis of androgen-dependent prostate cells. Prostate cancer consists of androgen-dependent and androgen-independent cells. The androgen-independent cells, usually present in the prostate of advanced prostate cancer patients do not have the ability to undergo apoptosis after androgen withdrawal. GC79/TRPS1 expression in androgen-dependent prostate cancer cells is repressed by androgens, while GC79/TRPS1 expression is hardly detectable in androgen-independent prostate cancer cells under cell culture conditions. This suggests that lack of GC79/TRPS1 expression could be a mechanism for the inability to induce the apoptotic pathway in androgen-independent prostate cancer cells after androgen withdrawal. This review will focus on the current knowlegde of the structure and function of GC79/TRPS1, a novel androgen-repressible apoptosis gene. |
| Databáze: | OpenAIRE |
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