Peng Y C, Breiding D E, Sverdrup F, Richard J, Androphy E J
Department of Dermatology, New England Medical Center, Tufts University School of Medicine, Boston, MA 02111, USA.
J Virol. 2000 Jul;74(13):5872-9. doi: 10.1128/jvi.74.13.5872-5879.2000.
The cellular protein AMF-1 (Gps2) positively modulates gene expression by the papillomavirus E2 protein (D. E. Breiding et al., Mol. Cell. Biol. 17:7208-7219, 1997). We show here that AMF-1 also binds the transcriptional coactivator p300 in vitro and in vivo. E2 interacted weakly with p300. These observations led to a model in which AMF-1 recruits p300 into a complex with E2. Cotransfection of AMF-1 or p300 stimulated levels of E2-dependent transcription, while cotransfection of both AMF-1 and p300 showed an additive effect. The functional significance of p300 recruitment for E2 transactivation was evidenced by repression of E2-activated transcription by adenovirus E1A, which inhibits both coactivator and acetylase activities of p300. Antibodies to AMF-1 or E2 immunoprecipitated histone acetylase activity from cell lysates. Western blotting using antibody against acetyl-lysine failed to detect acetylation of AMF-1 or E2 in complex with p300. These results suggest that AMF-1 facilitates the recruitment of p300 and its histone acetylase activity into complexes with E2 and represents a novel mechanism of transcriptional activation.
细胞蛋白AMF-1(Gps2)通过乳头瘤病毒E2蛋白正向调节基因表达(D. E. 布雷丁等人,《分子细胞生物学》17:7208 - 7219,1997年)。我们在此表明,AMF-1在体外和体内也与转录共激活因子p300结合。E2与p300的相互作用较弱。这些观察结果得出一个模型,即AMF-1将p300招募到与E2形成的复合物中。共转染AMF-1或p300可刺激E2依赖的转录水平,而同时共转染AMF-1和p300则显示出相加效应。腺病毒E1A对E2激活转录的抑制证明了p300招募对E2反式激活的功能意义,E1A可抑制p300的共激活因子和乙酰化酶活性。针对AMF-1或E2的抗体从细胞裂解物中免疫沉淀出组蛋白乙酰化酶活性。使用抗乙酰赖氨酸抗体的蛋白质印迹未能检测到与p300形成复合物的AMF-1或E2的乙酰化。这些结果表明,AMF-1促进p300及其组蛋白乙酰化酶活性招募到与E2形成的复合物中,并代表了一种新的转录激活机制。