Differentially expressed proteins in positive versus negative HNSCC lymph nodes

Vidotto, Alessandra; Polachini, Giovana Mussi; Paula-Silva, Marina de; Oliani, Sônia Maria; Henrique, Tiago; López, Rossana Verónica Mendoza; Cury, Patrí­cia Maluf; Nunes, Fábio Daumas; Gois-filho, J.F; Carvalho, Marcos Brasilino de; Leopoldino, Andréia Machado; Tajara, Eloíza H.

doi:10.1186/s12920-018-0382-6

“…47 Inflammation within the tumor microenvironment (cancer-related inflammation (CRI)) is now known to be a significant contributing factor in the development and progression of cancer, particularly in tumor invasion and metastasis. 44,48 Of the 50 genes identified here, a number have previously been reported to be differentially expressed (GBP2, 49 DUOX2, 50 IGFBP3 [51][52] ), or were associated with a more invasive and metastatic phenotype (AKR1B10, 53 FABP5, [53][54] Importantly, compound 35 seems to modulate these genes in a direction which opposes that identified in these previously reported studies, thus may be of therapeutic value.…”

Section: Spin149-262 Ic50mentioning

confidence: 49%

“…Of the 50 genes identified here, a number have previously been reported to be differentially expressed (GBP2, DUOX2, IGFBP3 , ) or were associated with a more invasive and metastatic phenotype (AKR1B10, FABP5, , HSPB1, KRT1, S100A9, CNFN, ID2, LCN2 (NGAL), IGFBP2, IFIT1, CCL5 ,, ) in squamous cell carcinomas (SCC).…”

Section: Resultsmentioning

confidence: 95%

See 1 more Smart Citation

A Chemical Probe for Tudor Domain Protein Spindlin1 to Investigate Chromatin Function

Fagan

¹

,

Johansson

²

,

Gileadi

³

et al. 2019

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Modifications of histone tails, including lysine/arginine methylation, provide the basis of a 'chromatin or histone code'. Proteins that contain 'reader' domains can bind to these modifications and form specific effector complexes, which ultimately mediate chromatin function. The spindlin1 (SPIN1) protein contains three Tudor methyllysine/arginine reader domains and was identified as a putative oncogene and transcriptional co-activator. Here we report a SPIN1 chemical probe inhibitor with low nanomolar in vitro activity, exquisite selectivity on a panel of methyl reader and writer proteins, and with submicromolar cellular activity. X-ray crystallography showed that this Tudor domain chemical probe simultaneously engages Tudor domains 1 and 2 via a bidentate binding mode. Small molecule inhibition and siRNA knockdown of SPIN1, as well as chemoproteomic studies, identified genes which are transcriptionally regulated by SPIN1 in squamous cell carcinoma and suggest that SPIN1 may have a roll in cancer related inflammation and/or cancer metastasis. a n ≥ 2. Abbreviations; BLI (BioLayer Interferometry), ITC (Isothermal Titration Calorimetry), nd (not determined).

show abstract

“…47 Inflammation within the tumor microenvironment (cancer-related inflammation (CRI)) is now known to be a significant contributing factor in the development and progression of cancer, particularly in tumor invasion and metastasis. 44,48 Of the 50 genes identified here, a number have previously been reported to be differentially expressed (GBP2, 49 DUOX2, 50 IGFBP3 [51][52] ), or were associated with a more invasive and metastatic phenotype (AKR1B10, 53 FABP5, [53][54] HSPB1, 53 KRT1, 53 S100A9, 53 CNFN, 55 ID2, 56 LCN2 (NGAL), 57 IGFBP2, 52 IFIT1, 58 CCL5 48,[59][60] ) in squamous cell carcinomas (SCC). Importantly, compound 35 seems to modulate these genes in a direction which opposes that identified in these previously reported studies, thus may be of therapeutic value.…”

Section: Resultsmentioning

confidence: 90%

A Chemical Probe For Tudor Domain Protein Spindlin1 to Investigate Chromatin Functions

Fagan¹,

Johansson²,

Gileadi³

et al. 2019

Preprint

View full text Add to dashboard Cite

Modifications of histone tails, including lysine/arginine methylation, provide the basis of a 'chromatin or histone code'. Proteins that contain 'reader' domains can bind to these modifications and form specific effector complexes, which ultimately mediate chromatin function. The spindlin1 (SPIN1) protein contains three Tudor methyllysine/arginine reader domains and was identified as a putative oncogene and transcriptional co-activator. Here we report a SPIN1 chemical probe inhibitor with low nanomolar in vitro activity, exquisite selectivity on a panel of methyl reader and writer proteins, and with submicromolar cellular activity. X-ray crystallography showed that this Tudor domain chemical probe simultaneously engages Tudor domains 1 and 2 via a bidentate binding mode. Small molecule inhibition and siRNA knockdown of SPIN1, as well as chemoproteomic studies, identified genes which are transcriptionally regulated by SPIN1 in squamous cell carcinoma and suggest that SPIN1 may have a roll in cancer related inflammation and/or cancer metastasis.<br>

show abstract

“…On the other hand, the overexpression of this molecule has been reported in many cancers, although its clinical meaning is still controversial (140)(141)(142), which could be, in part, due to the localization of ANXA1 in the nuclear and cytoplasmic compartments, and also associated to the membrane (131). In fact, the expression level of ANXA1 is down-regulated in numerous types of cancer and is linked with metastasis, relapse, and poor prognosis (141,143); ANXA1 is an endogenous inhibitor of NF-κB that may be stimulated in human cancer cells and in experimental mice models by powerful anti-inflammatory glucocorticoids and altered by non-steroidal anti-inflammatory drugs (143).…”

Section: Annexin A1 As a Candidate For Enhancing Radiotherapymentioning

confidence: 99%