Chang-Chieh Wu’s research while affiliated with National Defense Medical Center and other places

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Publications (106)


The effect of Tazarotene-induced gene 1 (TIG1) on cell viability and death of A2058 and A375 cells. A2058 (A) or A375 (C) cells were transfected with empty vector or TIG1-myc-his expression vector and expressed for 24–48 h. Cell viability and death were measured by water-soluble tetrazolium 1 (WST-1) and lactate dehydrogenase (LDH) release, respectively. Caspase-3 activity was measured using a colorimetric substrate following the transfection of A2058 (B) and A375 (D) cells with empty vector or with TIG1-myc-his expression vector for 24 h. *p < 0.05 compared with the control group.
RNA-seq analysis of genes that were differentially regulated by TIG1 in A2058 cells. A2058 cells were transfected with empty vector or TIG1-myc-his expression vector and expressed for 24 h. RNA-seq was used to determine gene expression profiles, and the Bland-Altman (MA) (A) and Volcano (B) plots are shown. Red dots indicate significant differences between groups transfected with the empty vector or the TIG1-myc expression vector. Genes with a more than two-fold difference in expression ratio between cells transfected with empty vector or TIG1 are presented as a heatmap for the top 50 genes (C). RNA-seq, RNA-sequencing.
The category of gene ontology (GO) biological process affected by TIG1 and derived from the RNA-seq data. Following transfection of A2058 cells with TIG1 expression vector, significant gene expression changes were mapped to cellular pathways, as represented by GO enrichment dot plots (A). Genes associated with Endoplasmic Reticulum (ER) stress response and unfolded protein response are shown (B).
The effect of TIG1 on the expression of ER stress response-related genes in A2058 and A375 cells. A2058 cells (A) and A375 cells (B) were transfected with empty vector or with the TIG1-myc-his expression vector and expressed for 24 h. Total RNA was extracted and relative levels of the indicated mRNAs were measured by quantitative real-time polymerase chain reaction (PCR) after normalization to the expression of β-actin. *p < 0.05 compared with the control group.
The effect of TIG1 on the expression of ER stress response-related proteins in A2058 and A375 cells. A2058 cells (A,C) and A375 cells (B) were transfected with empty vector or TIG1-myc-his expression vector and expressed for 24 h (A,B) or 6–48 h (C). Cell lysates were collected and the protein expression levels of HERPUD1, BIP and DDIT3 were measured by immunoblotting. The bar graphs quantify the indicated protein, with each sample normalized to the level of β-actin protein, based on three replicate western blot data. *p < 0.05 compared with the control group.

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Tazarotene-induced Gene 1 Induces Melanoma Cell Death by Triggering Endoplasmic Reticulum Stress Response
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June 2024

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1 Citation

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Lu-Kai Wang

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Background This study investigated the mechanism by which tazarotene-induced gene 1 (TIG1) inhibits melanoma cell growth. The main focus was to analyze downstream genes regulated by TIG1 in melanoma cells and its impact on cell growth. Methods The effects of TIG1 expression on cell viability and death were assessed using water-soluble tetrazolium 1 (WST-1) mitochondrial staining and lactate dehydrogenase release assays. RNA sequencing and Western blot analysis were employed to investigate the genes regulated by TIG1 in melanoma cells. Additionally, the correlation between TIG1 expression and its downstream genes was analyzed in a melanoma tissue array. Results TIG1 expression in melanoma cells was associated with decreased cell viability and increased cell death. RNA-sequencing (RNA-seq), quantitative reverse transcription PCR (reverse RT-QPCR), and immunoblots revealed that TIG1 expression induced the expression of Endoplasmic Reticulum (ER) stress response-related genes such as Homocysteine-responsive endoplasmic reticulum-resident ubiquitin-like domain member 1 (HERPUD1), Binding immunoglobulin protein (BIP), and DNA damage-inducible transcript 3 (DDIT3). Furthermore, analysis of the melanoma tissue array revealed a positive correlation between TIG1 expression and the expression of HERPUD1, BIP, and DDIT3. Additionally, attenuation of the ER stress response in melanoma cells weakened the impact of TIG1 on cell growth. Conclusions TIG1 expression effectively hinders the growth of melanoma cells. TIG1 induces the upregulation of ER stress response-related genes, leading to an increase in caspase-3 activity and subsequent cell death. These findings suggest that the ability of retinoic acid to prevent melanoma formation may be associated with the anticancer effect of TIG1.

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Safety and Efficacy of Oral Nalbuphine on Postoperative Pain in Hemorrhoidectomy Patients: A Randomized, Double-blind, Placebo-controlled, Pivotal Trial

September 2023

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37 Reads

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1 Citation

Clinical Journal of Pain

Objectives Severe postoperative pain requiring opioid treatment has been reported in 20–40% of hemorrhoidectomy patients. Compared to morphine, nalbuphine offers better hemodynamic stability, a lower risk of respiratory depression, and a lower potential for addiction. Nalbuphine was developed from intravenous form into an oral form (PHN131) to alleviate moderate-to-severe pain. Methods A randomized, double-blind, placebo-controlled, multiple-dose, parallel-design trial was conducted to evaluate the safety and efficacy of PHN131 in patients undergoing hemorrhoidectomy. Eligible patients were randomly assigned to receive either PHN131 soft capsules containing nalbuphine hydrochloride 60 mg or placebo capsules. Intramuscular diclofenac was the rescue analgesic. Pain was measured by the area under the curve of mean Visual Analog Scale (VAS) pain intensity scores. Results VAS results in patients receiving PHN131 were significantly lower than placebo group scores through 48 hours postoperatively (149.2±75.52 vs. 179.6±65.97; P =0.0301). According to Brief Pain Inventory Short Form scores, the impact of pain on quality of life was significantly smaller for the PHN131 group than for the placebo group. Time to the first use of diclofenac postoperatively was significantly longer in the PHN131 group than in the placebo group. The cumulative dosage of diclofenac in the PHN131 group was only around half of that in the placebo group ( P <0.0001). Drug-related adverse events were mild-to-moderate and resolved by treatment end. No drug-related severe adverse events were observed. Discussion Our findings demonstrate that PHN131 is effective and well-tolerated in the treatment of moderate-to-severe pain and may provide another option for patients to control their pain.


TIG1 Inhibits the mTOR Signaling Pathway in Malignant Melanoma Through the VAC14 Protein

May 2023

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6 Reads

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3 Citations

Anticancer Research

Background/aim: Currently, there are few drug options available to treat malignant melanoma. Tazarotene-inducible gene 1 (TIG1) was originally isolated from skin tissue, but its function in skin tissue has not been clarified. The aim of this study was to elucidate the effect of TIG1 and mTOR signaling pathways associated with VAC14 on melanoma. Materials and methods: The expression of TIG1 and VAC14 in melanoma tissue was analyzed using a melanoma tissue cDNA array. The interaction between TIG1 and VAC14 was analyzed using immunoprecipitation and immunostaining. Western blot was used to investigate the molecular targets of TIG1 and VAC14 in melanoma cells. Results: TIG1 was highly expressed in normal skin tissue but was low in malignant melanoma, while VAC14 showed the opposite trend. TIG1 inhibited insulin-induced cell proliferation and insulin-activated mammalian target of rapamycin complex 1 (mTORC1)-p70 S6 kinase but did not affect the level of phospho-AKT in A2058 melanoma cells. This suggests that the main target of TIG1 regulating cell growth is phosphatidylinositol 3,5-bisphosphate [PI(3,5)P2] rather than the PI(4,5)P2 signaling pathway. Additional TIG1 showed no additive effect on the inhibition of mTOR signaling in the absence of VAC14 expression, suggesting that TIG1 inhibited the activation of mTOR mainly by inhibiting VAC14. Conclusion: TIG1 may play an important role in preventing malignant melanoma through retinoic acid via VAC14.


Seselin promotes cisplatin-induced apoptosis of AGS gastric cancer cells by inhibiting β-catenin expression

January 2023

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39 Reads

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2 Citations

Archives of Biological Sciences

Gastric cancer is a commonly diagnosed form of cancer, and cisplatin is commonly used as a chemotherapy drug for treating it. However, the side effects of cisplatin may reduce patients? willingness to use it. Seselin, a derivative of coumarin, has been found to have anticancer properties as well as anticoagulant effects. In this study, we investigated the effect of seselin on promoting cisplatininduced gastric cancer cell death using the cell proliferation reagent WST-1, BrdU incorporation and lactate dehydrogenase release. The role of seselin and cisplatin in the apoptosis of gastric cancer cells was analyzed using a phospho-kinase array and Western blot analysis. Seselin did not affect G2/M stasis, but it promoted cell death in AGS cells treated with cisplatin. Phospho-kinase array analysis revealed that cisplatin regulates intracellular p53 phosphorylation, while seselin regulates intracellular ?-catenin expression by affecting the phosphorylation of glycogen synthase kinase-3 beta (GSK-3?), extracellular-signal-regulated kinase (ERK) and Src tyrosine kinase. Seselin and cisplatin promote the apoptosis of gastric cancer cells by the synergistic effect of two distinct signaling pathways. These findings suggest that seselin may be used as a complementary therapy to reduce the clinical dose of chemotherapy.


Fig. 1 Schematic of number of patients with CRC and assays performed
Fig. 2 Differentially abundant co-abundance groups (CAGs) of cancer and polyp tissues. The differentially abundant CAGs of cancer tissues (TC) and polyp tissues (TA) are displayed in box plots overlaid with paired dot plots. *P value < 0.05; **P value < 0.01.
Fig. 4 Effects of Prevotella intermedia on cell growth varied across cell lines and MOIs. A HCT116 cells and B HT29 cells were treated with Prevotella intermedia (PI), Fusobacterium nucleatum (FN), or E. coli DH5a at an MOI of 100 on day 0. Cell growth curves were measured using a hemocytometer. Cells treated with PBS served as controls. C HCT116 cells and D HT29 cells were co-cultured with Prevotella intermedia at various MOIs, and cell growth was measured using the RTCA iCELLigence System. The arrowhead indicates the time when the bacteria were added to the cell culture. *P value < 0.05; **P value < 0.01; ****P value < 0.0001
Fig. 5 Prevotella intermedia and Fusobacterium nucleatum additively enhances CRC cell migration and invasion. A-C Migration and D-F invasion assays were performed on CRC cells cultured with Prevotella intermedia (PI), Fusobacterium nucleatum (FN), PI plus FN (PI + FN), or nontoxigenic B. fragilis (NTBF) at an MOI of 100. Cells treated with PBS served as untreated controls, and NTBF served as a negative control. The relative percentage of migrated and invaded cells is presented as mean ± standard deviation. Data were obtained from three independent experiments. *P value < 0.05; ****P value < 0.0001; ns not significant
Enrichment of Prevotella intermedia in human colorectal cancer and its additive effects with Fusobacterium nucleatum on the malignant transformation of colorectal adenomas

October 2022

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146 Reads

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37 Citations

Journal of Biomedical Science

Background: Owing to the heterogeneity of microbiota among individuals and populations, only Fusobacterium nucleatum and Bacteroides fragilis have been reported to be enriched in colorectal cancer (CRC) in multiple studies. Thus, the discovery of additional bacteria contributing to CRC development in various populations can be expected. We aimed to identify bacteria associated with the progression of colorectal adenoma to carcinoma and determine the contribution of these bacteria to malignant transformation in patients of Han Chinese origin. Methods: Microbiota composition was determined through 16S rRNA V3-V4 amplicon sequencing of autologous adenocarcinomas, adenomatous polyps, and non-neoplastic colon tissue samples (referred to as "tri-part samples") in patients with CRC. Enriched taxa in adenocarcinoma tissues were identified through pairwise comparison. The abundance of candidate bacteria was quantified through genomic quantitative polymerase chain reaction (qPCR) in tissue samples from 116 patients. Associations of candidate bacteria with clinicopathological features and genomic and genetic alterations were evaluated through odds ratio tests. Additionally, the effects of candidate bacteria on CRC cell proliferation, migration, and invasion were evaluated through the co-culture of CRC cells with bacterial cells or with conditioned media from bacteria. Results: Prevotella intermedia was overrepresented in adenocarcinomas compared with paired adenomatous polyps. Furthermore, co-abundance of P. intermedia and F. nucleatum was observed in tumor tissues. More notably, the coexistence of these two bacteria in adenocarcinomas was associated with lymph node involvement and distant metastasis. These two bacteria also exerted additive effects on the enhancement of the migration and invasion abilities of CRC cells. Finally, conditioned media from P. intermedia promoted the migration and invasion of CRC cells. Conclusion: This report is the first to demonstrate that P. intermedia is enriched in colorectal adenocarcinoma tissues and enhances the migration and invasion abilities of CRC cells. Moreover, P. intermedia and F. nucleatum exert additive effects on the malignant transformation of colorectal adenomas into carcinomas. These findings can be used to identify patients at a high risk of malignant transformation of colorectal adenomas or metastasis of CRC, and they can accordingly be provided optimal clinical management.


Reciprocal regulation of Daxx and PIK3CA promotes colorectal cancer cell growth

July 2022

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48 Reads

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8 Citations

Cellular and Molecular Life Sciences

Upregulation of death-domain-associated protein (Daxx) is strongly associated with diverse cancer types. Among these, the clinicopathological significance and molecular mechanisms of Daxx overexpression in colorectal cancer (CRC) remain unknown. Here, we showed that Daxx expression was increased in both clinical CRC samples and CRC cell lines. Daxx knockdown significantly reduced proliferation activity in CRC cells and tumor growth in a xenograft model. Further studies revealed that Daxx expression could be attenuated by either treatment with the PIK3CA inhibitor PIK-75 or PIK3CA depletion in CRC cells. Conversely, expression of PIK3CA constitutively active mutants could increase Daxx expression. These data suggest that PIK3CA positively regulates Daxx expression. Consistently, the expression levels of PIK3CA and Daxx were positively correlated in sporadic CRC samples. Interestingly, Daxx knockdown or overexpression yielded decreased or increased levels of PIK3CA, respectively, in CRC cells. We further demonstrated that Daxx activates the promoter activity and expression of PIK3CA. Altogether, our results identify a mechanistic pathway of Daxx overexpression in CRC and suggest a reciprocal regulation between Daxx and PIK3CA for CRC cell growth.


Genomic and Metabolomic Landscape of Right-Sided and Left-Sided Colorectal Cancer: Potential Preventive Biomarkers

February 2022

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40 Reads

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10 Citations

Cells

Colorectal cancer (CRC) is the third most common cancer worldwide. The incidence and mortality rates of CRC are significantly higher in Taiwan than in other developed countries. Genes involved in CRC tumorigenesis differ depending on whether the tumor occurs on the left or right side of the colon, and genomic analysis is a keystone in the study and treatment of CRC subtypes. However, few studies have focused on the genetic landscape of Taiwanese patients with CRC. This study comprehensively analyzed the genomes of 141 Taiwanese patients with CRC through whole-exome sequencing. Significant genomic differences related to the site of CRC development were observed. Blood metabolomic profiling and polygenic risk score analysis were performed to identify potential biomarkers for the early identification and prevention of CRC in the Taiwanese population. Our findings provide vital clues for establishing population-specific treatments and health policies for CRC prevention in Taiwan.


Tazarotene‐induced gene 1 interacts with Polo‐like kinase 2 and inhibits cell proliferation in HCT116 colorectal cancer cells

July 2021

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15 Reads

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9 Citations

Cell Biology International

Tazarotene-induced gene 1 (TIG1) is considered to be a tumor suppressor gene that is highly expressed in normal or well-differentiated colon tissues, while downregulation of TIG1 expression occurs in poorly differentiated colorectal cancer (CRC) tissues. However, it is still unclear how TIG1 regulates the tumorigenesis of CRC. Polo-like kinases (Plks) are believed to play an important role in regulating the cell cycle. The performance of PLK2 in CRC is negatively correlated with the differentiation status of CRC tissues. Here, we found that PLK2 can induce the growth of CRC cells and that TIG1 can prevent PLK2 from promoting the proliferation of CRC cells. We also found that the expression of PLK2 in CRC cells was associated with low levels of Fbxw7 protein and increased expression of cyclin E1. When TIG1 was coexpressed with PLK2, the changes in Fbxw7/cyclin E1 levels induced by PLK2 were reversed. In contrast, silencing TIG1 promoted the proliferation of CRC, and when PLK2 was also silenced, the proliferation of CRC cells induced by TIG1 silencing was significantly inhibited. The above research results suggest that TIG1 can regulate the tumorigenesis of CRC by regulating the activity of PLK2. This article is protected by copyright. All rights reserved.


Cathepsin V Mediates the Tazarotene-induced Gene 1-induced Reduction in Invasion in Colorectal Cancer Cells

December 2020

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111 Reads

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23 Citations

Cell Biochemistry and Biophysics

Tazarotene-induced gene 1 (TIG1) is a retinoid acid receptor-responsive gene involved in cell differentiation and tumorigenesis. Aberrant methylation of CpG islands in the TIG1 promoter is found in multiple cancers. Currently, the exact mechanism underlying the anticancer effect of TIG1 is unknown. Here, we show that TIG1 interacts with cathepsin V (CTSV), which reduces CTSV stability and subsequently affects the production of activated urokinase-type plasminogen activator (uPA), an epithelial-mesenchymal transition-associated protein. Ectopic expression of CTSV increased the expression of activated uPA and the number of migrated and invaded cells, whereas ectopic TIG1 expression reversed the effects of CTSV on the uPA signaling pathway. Similar patterns in the production of activated uPA and number of migrated and invaded cells were also observed in TIG1-expressing and CTSV-knockdown cells. The results suggest that CTSV may participate in TIG1-regulated uPA activity and the associated downstream signaling pathway.


Fig. 2. CONSORT diagram. Tx, treatment.
Clinicopathological features of the 213 enrolled patients with mCRC.
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Determination of the UGT1A1 polymorphism as guidance for irinotecan dose escalation in metastatic colorectal cancer treated with first-line bevacizumab and FOLFIRI (PURE FIST)

October 2020

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92 Reads

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32 Citations

European Journal of Cancer

Aim Uridine diphosphate glucuronosyltransferase 1A1 (UGT1A1) polymorphism plays a crucial role in the increased susceptibility of patients to irinotecan and its toxicity. This study is a multicenter, randomised clinical trial comparing the clinical outcomes and adverse events (AEs) in metastatic colorectal cancer (mCRC) patients treated with bevacizumab plus FOLFIRI with or without UGT1A1 genotyping and irinotecan dose escalation as the first-line therapy. Methods The control group received conventional biweekly FOLFIRI plus bevacizumab without UGT1A1 genotyping, whereas the study group received the same regimen with irinotecan dose escalation based on UGT1A1 genotyping. The primary end-point was progression-free survival (PFS), and secondary end-points were overall response rate (ORR), disease control rate (DCR), overall survival (OS), AEs and metastasectomy rate. Results Over a median follow-up of 26.0 months (IQR, 17.0–35.0 months), study group (n = 107) was superior to the control group (n = 106) in PFS, OS, ORR, DCR, and metastasectomy rate (all P < 0.05). Furthermore, there were no significant differences in AEs ≥ grade III between the two groups, even with the 1.36-fold increase in the relative dose intensity of irinotecan in the study group. Dose escalation of irinotecan, an independent factor of ORR (P < 0.001) and DCR (P = 0.006), improved PFS in mCRC patients with wild-type and mutant KRAS (P = 0.007 and P = 0.019, respectively). Conclusion The current study revealed that mCRC patients, regardless of KRAS gene status, with UGT1A1 genotyping can tolerate escalated doses of irinotecan and potentially achieve a more favourable clinical outcome without significantly increased toxicities. Clinical trial registration NCT02256800.


Citations (69)


... Tumor suppressor gene TIG1 expression inhibits cell proliferation in malignant melanoma. [28,29] with poorer kidney survival rates, suggesting that TIG1 is a risk factor for RA-induced kidney disease [37]. Additionally, analysis of data from The Cancer Genome Atlas showed that TIG1 expression was negatively correlated with the survival rate of patients with renal cell carcinoma. ...

Reference:

The role of tazarotene-induced gene 1 in carcinogenesis: is it a tumor suppressor gene or an oncogene?
Tazarotene-induced Gene 1 Induces Melanoma Cell Death by Triggering Endoplasmic Reticulum Stress Response

... Considering that over 80% of patients experience moderate to severe postoperative pain, there is a pressing need to emphasize the significance of postoperative analgesia (24). Until now, numerous studies have been undertaken to explore effective strategies for managing pain after hemorrhoidectomy (18,(24)(25)(26)(27)(28)(29). Nevertheless, the persistent issue of inadequate postoperative pain relief remains a significant concern, even with the adoption of multimodal pain management strategies (30). ...

Safety and Efficacy of Oral Nalbuphine on Postoperative Pain in Hemorrhoidectomy Patients: A Randomized, Double-blind, Placebo-controlled, Pivotal Trial
  • Citing Article
  • September 2023

Clinical Journal of Pain

... Tumor suppressor gene TIG1 expression inhibits cell proliferation in malignant melanoma. [28,29] with poorer kidney survival rates, suggesting that TIG1 is a risk factor for RA-induced kidney disease [37]. Additionally, analysis of data from The Cancer Genome Atlas showed that TIG1 expression was negatively correlated with the survival rate of patients with renal cell carcinoma. ...

TIG1 Inhibits the mTOR Signaling Pathway in Malignant Melanoma Through the VAC14 Protein
  • Citing Article
  • May 2023

Anticancer Research

... After transfection of A2058 and A375 cells with empty vector or TIG1-myc-his expression vector, cells were lysed with RIPA buffer. Caspase-3 activity was measured using a caspase-3 substrate as described previously [23]. Briefly, cell lysates were incubated in a buffer containing 25 mM HEPES [pH 7.5], 0.1% CHAPS, 5% sucrose, 5 mM DTT, 2 mM EDTA, and 2 mM caspase-3 substrate (Ac-DEVD-pNA; Sigma). ...

Seselin promotes cisplatin-induced apoptosis of AGS gastric cancer cells by inhibiting β-catenin expression

Archives of Biological Sciences

... Members of the genus Peptostreptococcus, Peptostreptococcus stomatis are two of the four universal fecal microbial signatures for CRC that have been found in Chinese, Danish, Austrian and French cohorts (Yu et al., 2017). Prevotella intermedia has been described to be more abundant in colorectal adenocarcinoma tissues as well as in the fecal samples of CRC patients, which may promote migration and invasion of CRC tumor cells (Avuthu and Guda, 2022;Lo et al., 2022;Tito et al., 2024). In addition, the relative dominance of Bacteroides and Parabacteroides species (B. ...

Enrichment of Prevotella intermedia in human colorectal cancer and its additive effects with Fusobacterium nucleatum on the malignant transformation of colorectal adenomas

Journal of Biomedical Science

... CD24 promotes adhesion and signifies the spread of cancer, whereas Daxx expression positively correlates with CD4 expression in CRC patients [17]. Daxx interacts with Tcf4 and inhibits its transcriptional function, thereby modifying downstream gene expression of Tcf4 and facilitating G1 arrest in colon cancer cells [18,19]. ...

Reciprocal regulation of Daxx and PIK3CA promotes colorectal cancer cell growth

Cellular and Molecular Life Sciences

... The prognosis of metastatic CRC (mCRC) is influenced by tumor gene profiles, primary tumor location, and response to combinations of systemic therapies [3][4][5][6]. Emerging evidence suggests that left-sided CRC is associated with a better prognosis than is right-sided CRC, with notable differences in the genomic and metabolic landscapes between these two subtypes [7,8]. CRC treatment has evolved considerably, benefiting from advancements in surgical techniques, radiation therapy, and chemotherapy. ...

Genomic and Metabolomic Landscape of Right-Sided and Left-Sided Colorectal Cancer: Potential Preventive Biomarkers

Cells

... Importantly, the novel constructed a prognostic risk model with independent prognostic value to help clinicians provide a meaningful reference for the prognosis and treatment of colon cancer patients. Among them, PLK2 was found to induce the growth and proliferation of colorectal cancer cells, whereas TIG1 prevents this process [30]. VSIG4 positivity in patients with advanced gastric cancer is associated with an adverse prognosis, but the relationship between VSIG4 expression and colon cancer survival has not been observed [31]. ...

Tazarotene‐induced gene 1 interacts with Polo‐like kinase 2 and inhibits cell proliferation in HCT116 colorectal cancer cells
  • Citing Article
  • July 2021

Cell Biology International

... Reduced expression of RA target genes correlates with poorer prognosis in CRC, suggesting that RA signaling pathways could serve as therapeutic targets for CRC [55]. A study by Wang et al. revealed that TIG1 was highly expressed in normal colon tissues, but its expression tended to decrease in cancerous tissues [22,23]. Analysis of the distribution of the TIG1 protein in colorectal cancer tissues revealed that TIG1 was located primarily in normal colon tissues and in highly differentiated colorectal adenocarcinomas, while its expression was low in poorly differentiated colorectal adenocarcinomas [5]. ...

Cathepsin V Mediates the Tazarotene-induced Gene 1-induced Reduction in Invasion in Colorectal Cancer Cells

Cell Biochemistry and Biophysics

... [21][22][23][24] The majority of available literature evaluating UGT1A1irinotecan was performed in colorectal cancer patients receiving FOLFIRI and did not find associations between UGT1A1 IM and increased toxicity risk. [25][26][27][28] In fact, there have been multiple prospective studies that have concluded that UGT1A1 IM likely tolerates higher doses of irinotecan within this regimen. However, there is an increasing amount of evidence that irinotecan toxicity is also increased in UGT1A1 intermediate metabolizers when administered as part of a three-agent regimen with both fluoropyrimidine and oxaliplatin that may need to be considered. ...

Determination of the UGT1A1 polymorphism as guidance for irinotecan dose escalation in metastatic colorectal cancer treated with first-line bevacizumab and FOLFIRI (PURE FIST)

European Journal of Cancer