1. Blocking cytoplasmic translocation of nucleolar protein NOP53 by deleting its nuclear export sequence abrogated its support of viral replication. Recombinant N3-T protein, containing NOP53 residues 330-432 and a human immunodeficiency virus-derived cell-penetrating Tat peptide, attenuated the expression of IFN-beta; and IFN-stimulated genes, as well as decreased the phosphorylation of interferon regulatory factor3. PMID: 29677136
2. The findings of this study suggest that disruption of PICT-1 protein expression and codon 389 polymorphism can contribute to the pathogenesis or neoplastic progression of endometrial cancer. PMID: 29617699
3. The study presented evidence that viral infection induced translocation of GLTSCR2 from nucleus to cytoplasm, and cytoplasmic translocation enabled GLTSCR2 to effectively attenuate IFN-beta and support viral replication; however, viral infection did not result in elevating GLTSCR2 in cells. PMID: 27824081
4. PICT-1 triggers pro-death autophagy through inhibition of rRNA transcription and the inactivation of AKT/mTOR/p70S6K pathway in glioblastoma cells. PMID: 27729611
5. PICT-1 is a major nucleolar sensor of the DNA damage repair response and an important upstream regulator of p53 via the RPL11-MDM2-p53 pathway. PMID: 27829214
6. Codon 389 polymorphism in PICT-1 is a risk factor for uterine cervical cancers.PICT-1 counteracts HPV-induced p53 degradation. PMID: 27996172
7. GLTSCR2 is a crucially involved in the positive regulation of telomerase and chromosome stability. PMID: 27357325
8. The expression of GLTSCR2 was suppressed in renal cell carcinomas, accentuating the malignant phenotype. PMID: 26724143
9. GLTSCR2 is crucial for normal cellular function as well as for preventing the development or progression of cancer. The JNK-c-jun axis is indispensible for regulating the activities of GLTSCR2. PMID: 26903295
10. GLTSCR2 was an upstream negative regulator of the nucleophosmin (NPM)-MYC axis involved in controlling the transcriptional activity of MYC. GLTSCR2 may be a candidate for suppressing the growth of cancer cells stimulated by MYC hyperactivation. PMID: 25956029
11. Data show that tumor sppressor protein GLTSCR2 down-regulates total nucleophosmin (NPM) expression levels by decreasing its protein stability. PMID: 25818168
12. We demonstrated the GLTSCR2 expression decreased with the rise of the grade of cervical lesions; GLTSCR2 may play an important role in carcinogenesis of cervical cancer PMID: 25118835
13. These results suggest that PICT1 employs atypical proteasome-mediated degradation machinery to sense nucleolar stress within the nucleolus. PMID: 24923447
14. High PICT1 expression is associated with hepatocellular carcinoma. PMID: 23532381
15. GLTSCR2 is down-regulated in squamous cell carcinomas of the skin and UV light exposure decreases the stability of GLTSCR2 and sensitizes keratinocytes to DNA damage. PMID: 23942755
16. Authors confirmed the interaction of PICT-1 with itself by direct yeast two-hybrid assay and also showed self-association of PICT-1 in mammalian cells by co-immunoprecipitation and fluorescence resonance energy transfer assays. PMID: 24735870
17. GLTCR2 may play a role in the tumorigenesis, progression and biological behavior in breast cancer. PMID: 24054033
18. GLTSCR2 controls cellular proliferation and metabolism via the transcription factor Myc, and is induced by mitochondrial stress, suggesting it may constitute a significant component of the mitochondrial signaling pathway. PMID: 24556985
19. Findings suggest that PICT1 has a crucial role in gastric cancer progression by regulating the MDM2-TP53 pathway through RPL11. PMID: 24045667
20. GLTSCR2 functions as a tumor suppressor in prostatic adenocarcinomas. PMID: 23920125
21. The glioma tumor-suppressor candidate region gene 2 (GLTSCR2)is as a new member of the nucleolus-nucleoplasmic axis for p53 regulation. PMID: 22522597
22. Repeated hypoxia downregulates p53-upstream regulator, GLTSCR2, which resulted in increased death resistance and invasive potential of glioblastoma cells. Restoration of GLTSCR2 expression suppressed the malignant potential of hypoxia-selected cells. PMID: 22850112
23. PICT-1 exhibits a nucleolar distribution similar to proteins involved in ribosomal RNA processing, yet does not colocalize precisely with either UBF1 or Fibrillarin under normal or stressed conditions. PMID: 22292050
24. GLTSCR2 seems to act as a tumor suppressor by participating in optimal DNA damage response because DNA damage is a frequent and crucial event in oncogenesis. PMID: 21741933
25. PICT1 is a potent regulator of the MDM2-P53 pathway and promotes tumor progression by retaining RPL11 in the nucleolus. PMID: 21804542
26. merlin mediates PICT-1-induced growth inhibition by translocating to the nucleolus and binding PICT-1 PMID: 21167305
27. Our results show a down-regulation of GLTSCR2 in seborrheic keratosis, indicating that GLTSCR2 may have a protective effect on the development of SK. PMID: 20185249
28. study describes a novel interaction between KS-Bcl-2 & PICT-1 cellular protein, encoded by a candidate tumor suppressor gene, GLTSCR2; show this interaction specifically targets KS-Bcl-2 to the nucleolus & decreases its antiapoptotic activity PMID: 20042497
29. These results suggest that PICT-1 plays a role in phosphatidylinositol 3,4,5-trisphosphate signals through controlling PTEN protein stability. PMID: 16971513
30. results suggest that the induction of PTEN-modulated apoptosis is one of the putative mechanisms of tumor suppressive activity by GLTSCR2 PMID: 17657248
31. GLTSCR2 as a proapoptotic protein sensitizing cells to hypoxic injury when overexpressed PMID: 17890897
32. GLTSCR2 expression is down-regulated in glioblastomas. Direct sequencing analysis and fluorescence in situ hybridization clearly demonstrates the presence of genetic alterations, such as a nonsense mutation and deletion, in the GLTSCR2 gene. PMID: 18729076

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HGNC: 4333

OMIM: 605691

KEGG: hsa:29997

STRING: 9606.ENSP00000246802

UniGene: Hs.421907