1. Moreover, SRSF10, hnRNP A1/A2 and Sam68 collaborate to drive the DNA damage-induced splicing response of several transcripts that produce components implicated in apoptosis, cell-cycle control and DNA repair. PMID: 29396485
2. SAM68 is required for efficient recruitment of PUM2 to NORAD, regulation of Pum activity by NORAD, and proper chromosome segregation in mammalian cells. PMID: 29386330
3. Results revealed that upregulation of Sam68 significantly inhibited cisplatin-induced apoptosis in oral tongue squamous cell carcinoma cells. PMID: 27473117
4. The PRMT2 interacts with SAM68 in cells and regulates its subcellular localization via the SH3 domain of PRMT2, prompting us to investigate the potential role of PRMT2 in BCL-X alternative splicing. PMID: 28057797
5. Data suggest that the first 22 bp of exon 3 in BIRC5 contain cis-acting elements that enhance the exclusion of exon 3 to generate the survivin DEx3 mRNA isoform via exclusion/deletion of exon 3; Sam68 is a possible trans-acting factor that binds to this cis-acting element and regulates exon 3 splicing. (BIRC5/survivin = baculoviral IAP repeat containing 5; Sam68 = GAP-associated tyrosine phosphoprotein p62) PMID: 28655776
6. our results indicated that Sam68 modulates apoptosis of intestinal epithelial cells via mediating NF-kappaB activation in ulcerative colitis PMID: 27235792
7. Sam68 possibly participated in the progresses of T-acute lymphoblastic leukemia at least partially via AKT/mTOR signaling pathway PMID: 27107742
8. Sam68 is essential for DNA damage-induced NF-kappaB activation and colon tumorigenesis. PMID: 27458801
9. These findings define a hitherto novel mechanism of action for Sam68 in governing p53 transcriptional activation, and represent the first report of Sam68 in the regulation of tumor suppressor activities. PMID: 27365047
10. HNRNPL acts as the adaptor to combine the two substructures and form the intact Sam68 nuclear body through the interaction of two sets of RNA recognition motifs with the putative architectural RNA in the respective substructures. PMID: 27377249
11. Sam68 was overexpressed in EOC tissue in association with such cancer malignant factors of FIGO stage, histological grade, and lymph node metastasis, and also positively regulated the proliferation of EOC cells. PMID: 27623016
12. Taken together, these results illuminated that enterovirus 71 infections can induce stress granule formation, and Sam68, as a stress granule component, migrates alone with stress granules dependent on intact microtubule upon the viral infections. PMID: 27057671
13. The host factor Sam68 interact with both, foot-and-mouth disease virus RNA motifs in the internal ribosome binding site and viral non-structural proteins 3C(pro) and 3D(pol). PMID: 26695943
14. Sam68 has separable effects on the regulation of AR-V7 expression and transcriptional activity, through its RNA-binding capacity. PMID: 26310125
15. The RNA-binding protein Sam68 regulates tumor cell viability and hepatic carcinogenesis by inhibiting the transcriptional activity of FOXOs PMID: 26438629
16. Sam68 Promotes NF-kappaB Activation and Apoptosis Signaling in Articular Chondrocytes during Osteoarthritis PMID: 26350037
17. MicroRNA-203 inhibits the malignant progression of neuroblastoma by targeting Sam68. PMID: 26136151
18. Here we review recent studies on the role of SAM68 in splicing regulation and we discuss its contribution to aberrant pre-mRNA processing in cancer. [review] PMID: 26273626
19. Sam68 could promote esophageal squamous cell carcinoma(ESCC) cell proliferation via the activation of Akt/GSK-3beta pathway. This research indicated that Sam68 might accelerate the cell cycle progression and be considered as a new therapy target in ESCC PMID: 26050229
20. Results show that SAM68 expression is increased in muscle invasive bladder cancer (MIBC) and correlated with poor prognosis suggesting it as a potentially useful prognostic marker for MIBC. PMID: 25944080
21. Conclusively, the cleavage of Sam68 is a new indicator for the cell damaging effects of ionizing radiation. PMID: 25666188
22. The nuclear protein Sam68 is found as an additional new host factor that interacts with the enterovirus 71 IRES during infection and could potentially enhance the translation of virus protein. PMID: 26202240
23. results reveal the complex molecular mechanism underlying SMAR1-mediated signal-dependent and -independent regulation of alternative splicing via Sam68 deacetylation PMID: 26080397
24. Sam68 may be useful prognostic marker for EC, and it plays an important role in promoting the cellular proliferation. PMID: 25874492
25. The expression of Sam68 was significantly elevated in non-small cell lung carcinoma tissues as compared with adjacent non-cancerous tissues. PMID: 24522888
26. This study provides evidence that both high expression level and nuclear localization of Sam68 correlate with invasiveness and aggressiveness characteristics in coloretal cancer, and poorer survival. PMID: 23937454
27. Sam68 is a role in the regulation of differential expression and mRNA processing and translation according to internal and external signals. PMID: 24287914
28. FBI-1 affects recruitment of SAM68 on the BCL-X transcript through an HDAC dependent mechanism. PMID: 24514149
29. These data, plus the fact that Sam68 is known to be a signaling adaptor protein, indicated that Sam68 is a signal molecule with a functional role in the PI3K/Akt signal pathway during enterovirus 71 infection. PMID: 24316008
30. Deficient SAM68 expression was observed in the human testis with maturation arrest at the spermatocyte stage and Sertoli cell-only syndrome. PMID: 24794312
31. Sam68 is identified as a novel non-Rel component in the nuclear factor-kappaB (NF-kappaB) complex that confers CD25 transcription. PMID: 23715268
32. Emerging roles for Sam68 in adipogenesis and neuronal development. PMID: 23018781
33. Study propose that Sam68 functions as a classical scaffold protein in this context, assembling components of an osteoclast-specific signalling pathway. PMID: 22745667
34. Sam68 could induce cervical cancer lymph node metastasis through regulating epithelial-mesenchymal transition PMID: 21700735
35. The results show that DDX3, eIF5A, and hRIP enhanced HIV-1 internal ribosomal entry site-mediated translation, whereas Sam68 does not. PMID: 21360055
36. The tyrosine-rich domain of Sam68 is bound in a bent conformation to the APC groove. PMID: 22000517
37. Sam68 interacts with insulin receptor substrate (IRS)-1 in basal conditions, and insulin increases the affinity between these two partners. PMID: 22005517
38. Sam68 is required for both NF-kappaB activation and apoptosis signaling by the TNF receptor PMID: 21620750
39. High Sam68 expression is associated with pancreatic cancer progression. PMID: 21642356
40. These results demonstrated for the first time that Hsp22 regulates Sam68 expression and the ratio of Sam68 to Hsp22 may determine the proliferative potential of glioblastoma cells. PMID: 21678403
41. Met receptors induce Sam68-dependent cell migration by activation of alternate extracellular signal-regulated kinase family members PMID: 21489997
42. These results strongly suggest the participation of Sam68 in leptin receptor signaling in human trophoblastic cells, and therefore, Sam68 may mediate some of the leptin effects in placenta. PMID: 21035519
43. Sam68 modulation of SF2/ASF splicing is controlled by epithelial cell-derived soluble factors that act through the ERK1/2 signaling pathway to regulate Sam68 phosphorylation. PMID: 20876280
44. the Qua1 homodimerization domain is required for regulation of alternative splicing by Sam68. PMID: 20610388
45. Sam68 is sequestered by expanded CGG repeats and thereby loses its splicing-regulatory function. PMID: 20186122
46. In vivo splicing assays showed that Sam68 triggers SMN2 exon-7 skipping. PMID: 20186123
47. SAM68 could represent a novel and useful prognostic marker for renal cell carcinoma. High SAM68 expression and cytoplasmic localization are associated with poor overall survival in renal cell carcinoma patients PMID: 19755649
48. Sam68 interacts with HIV-1 Rev protein and directly participates in nuclear exportation of HIV-1 unspliced or singly spliced RNA. PMID: 19535902
49. Our results identify Sam68 as the first splicing factor to affect CCND1 alternative splicing in prostate cancer cells PMID: 20028857
50. Sam68 is recruited into stress granules through complexing with TIA-1 in response to oxidative stress PMID: 19615357

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HGNC: 18116

OMIM: 602489

KEGG: hsa:10657

STRING: 9606.ENSP00000313829

UniGene: Hs.445893