Upregulation of soluble resistance-related calcium-binding protein (sorcin) in gastric cancer

Deng, Langmei; Su, Tao; Leng, Ai‐Min; Zhang, Xiaomei; Xu, Meihua; Liu, Yan; Gu, Huan; Zhang, Guiying

doi:10.1007/s12032-009-9342-5

Cited by 47 publications

(28 citation statements)

References 24 publications

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“…Sorcin has been implicated in chemoresistance and cancer as well. In fact, high levels of this protein have been reported in cancer cell lines and vincristine-resistant gastric cancer cell lines (16)(17)(18). Furthermore, Sorcin expression might be responsible for drug resistance and poor prognosis in non-small cell lung tumors (19,20).…”

Section: Discussionmentioning

confidence: 99%

“…Both these proteins have previously been implicated in chemoresistance, in part due to their ability to modulate Ca 2+ levels. Other reports suggest a correlation between Sorcin and the multidrug-resistant MDR1/P-glycoprotein: it has been shown that the knockdown of Sorcin induces the upregulation of MDR1 in HeLa cells (15); by contrast, a direct correlation between Sorcin and multidrug resistance overexpression has also been reported in human gastric cancer cell lines and vincristine-resistant gastric cancer cells (16)(17)(18). Finally, recent studies aimed at evaluating changes in gene expression profile in oral squamous cell carcinoma and non-small cell lung cancer identified a cDNA homologous to Sorcin expressed only in tumors, apparently responsible for drug resistance and poor prognosis (19,20).…”

Section: Introductionmentioning

confidence: 99%

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Mitochondrial Chaperone Trap1 and the Calcium Binding Protein Sorcin Interact and Protect Cells against Apoptosis Induced by Antiblastic Agents

et al. 2010

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TRAP1, a mitochondrial chaperone (Hsp75) with antioxidant and antiapoptotic functions, is involved in multidrug resistance in human colorectal carcinoma cells. Through a proteomic analysis of TRAP1 coimmunoprecipitation complexes, the Ca 2+ -binding protein Sorcin was identified as a new TRAP1 interactor. This result prompted us to investigate the presence and role of Sorcin in mitochondria from human colon carcinoma cells. Using fluorescence microscopy and Western blot analysis of purified mitochondria and submitochondrial fractions, we showed the mitochondrial localization of an isoform of Sorcin with an electrophoretic motility lower than 20 kDa that specifically interacts with TRAP1. Furthermore, the effects of overexpressing or downregulating Sorcin and/or TRAP1 allowed us to demonstrate a reciprocal regulation between these two proteins and to show that their interaction is required for Sorcin mitochondrial localization and TRAP1 stability. Indeed, the depletion of TRAP1 by short hairpin RNA in colorectal carcinoma cells lowered Sorcin levels in mitochondria, whereas the depletion of Sorcin by small interfering RNA increased TRAP1 degradation. We also report several lines of evidence suggesting that intramitochondrial Sorcin plays a role in TRAP1 cytoprotection. Finally, preliminary evidence that TRAP1 and Sorcin are both implicated in multidrug resistance and are coupregulated in human colorectal carcinomas is provided. These novel findings highlight a new role for Sorcin, suggesting that some of its previously reported cytoprotective functions may be explained by involvement in mitochondrial metabolism through the TRAP1 pathway.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Mitochondrial Chaperone Trap1 and the Calcium Binding Protein Sorcin Interact and Protect Cells against Apoptosis Induced by Antiblastic Agents

et al. 2010

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“…[7][8][9][10][11][12] Furthermore, the soluble resistance-related calcium binding protein (sorcin) is involved in the up-regulation of P-gp in GC cell lines and thus in the development of the MDR phenotype. [13][14][15][16] Hypoxia, a common characteristic of many tumors, has also been described as a crucial player in the drug resistance mechanisms. [17][18][19] In particular, hypoxia-inducible factor-1a (HIF-1a) is involved in the tumor response to cellular hypoxia through the transcriptional regulation of a large number of hypoxia-related genes, including MDR genes.…”

Section: Introductionmentioning

confidence: 99%

The potential predictive role of nuclear NHERF1 expression in advanced gastric cancer patients treated with epirubicin/oxaliplatin/capecitabine first line chemotherapy

Mangia

Caldarola

Dell'Endice

et al. 2015

Cancer Biology & Therapy

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Cellular resistance in advanced gastric cancer (GC) might be related to function of multidrug resistance (MDR) proteins. The adaptor protein NHERF1 (Na C /H C exchanger regulatory factor) is an important player in cancer progression for a number of solid malignancies, even if its role to develop drug resistance remains uncertain. Herein, we aimed to analyze the potential association between NHERF1 expression and P-gp, sorcin and HIF-1a MDR-related proteins in advanced GC patients treated with epirubicin/oxaliplatin/capecitabine (EOX) chemotherapy regimen, and its relation to response. Total number of 28 untreated patients were included into the study. Expression and subcellular localization of all proteins were assessed by immunohistochemistry on formalin-fixed paraffin embedded tumor samples. We did not found significant association between NHERF1 expression and the MDR-related proteins. A trend was observed between positive cytoplasmic NHERF1 (cNHERF1) expression and negative nuclear HIF-1a (nHIF-1a) expression (68.8% versus 31.3% respectively, P D 0.054). However, cytoplasmic P-gp (cP-gp) expression was positively correlated with both cHIF-1a and sorcin expression (P D 0.011; P D 0.002, respectively). Interestingly, nuclear NHERF1 (nNHERF1) staining was statistically associated with clinical response. In detail, 66.7% of patients with high nNHERF1 expression had a disease control rate, while 84.6% of subjects with negative nuclear expression of the protein showed progressive disease (P D 0.009). Multivariate analysis confirmed a significant correlation between nNHERF1 and clinical response (OR 0.06, P D 0.019). These results suggest that nuclear NHERF1 could be related to resistance to the EOX regimen in advanced GC patients, identifying this marker as a possible independent predictive factor.

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“…Sorcin was first identified in a vincristine-resistant Chinese hamster lung cell line, and was later demonstrated to be overexpressed in several tumor cell types [33][34][35] and many multidrug resistance (MDR) cell lines [36,37]. As to the role of sorcin overexpression in human gastric cancer and the underlying mechanisms of sorcin in drug resistance, Deng et al [38] argued that the overexpression of sorcin was related to the depth of invasion, TNM stage, and lymph node metastasis, which suggested that sorcin may contribute to progression and metastasis of gastric carcinoma and sorcin plays an important role in the development of gastric carcinoma probably by regulating the apoptotic pathways in gastric carcinoma cells, which was further elucidated in another paper [39]. It was reported that sorcin was identified as a new binding partner of TRAP1 (a mitochondrial chaperone HSP75) in MDR of human colorectal carcinoma cells, indicating that the cytoprotective function of sorcin may be involved in TRAP1-associated signaling pathway, which was coincident with the result of Maddalena et al [36] They found that RNAi-mediated silencing of sorcin activated caspase-3, caspase-12, and GRP78/ BiP, and then triggered apoptosis through the mitochondrial pathway, which established that human colorectal cancer cells overexpressing sorcin as an adaptive mechanism to escape apoptosis triggered by chemotherapeutic agents, while He et al [40] argued that regulation of P-glycoprotein (P-gp) might be one of the mechanisms of sorcin-mediated MDR, for they found that overexpression of sorcin up-regulated the expression of P-gp, and P-gp inhibitor verapamil partially reversed the sorcin-mediated MDR in SGC7901 cell.…”

Section: Discussionmentioning

confidence: 99%

Proteomics-based analysis of differentially expressed proteins in the CXCR1-knockdown gastric carcinoma MKN45 cell line and its parental cell

Hu¹,

Wang²,

Luo³

et al. 2013

ABBS

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C-X-C chemokine receptor types 1 (CXCR1), a cell-surface G-protein-coupled receptor has been found to be associated with tumorigenesis, development, and progression of some tumors. Previously, we have found that CXCR1 overexpression is associated with late-stage gastric adenocarcinoma. We also have demonstrated that knockdown of CXCR1 could inhibit cell proliferation in vitro and in vivo. In this study, we compared the changes of protein expression profile between gastric carcinoma MKN45 cell line and CXCR1-knockdown MKN45 cell line by 2D electrophoresis. Among the 101 quantified proteins, 29 spots were significantly different, among which 13 were downregulated and 16 were up-regulated after CXCR1 knockdown. These proteins were further identified by mass spectrometry analysis. Among them, several up-regulated proteins such as hCG2020155, Keratin8, heterogeneous nuclear ribonucleoprotein C (C1/C2), and several downregulated proteins such as Sorcin, heat shock protein 27, serpin B6 isoform b, and heterogeneous nuclear ribonucleoprotein K were confirmed. These proteins are related to cell cycle, the transcription regulation, cell adherence, cellular metabolism, drug resistance, and so on. These results provide an additional support to the hypothesis that CXCR1 might play an important role in proliferation, invasion, metastasis, and prognosis, and drug resistance of gastric carcinoma.

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Upregulation of soluble resistance-related calcium-binding protein (sorcin) in gastric cancer

Cited by 47 publications

References 24 publications

Mitochondrial Chaperone Trap1 and the Calcium Binding Protein Sorcin Interact and Protect Cells against Apoptosis Induced by Antiblastic Agents

Mitochondrial Chaperone Trap1 and the Calcium Binding Protein Sorcin Interact and Protect Cells against Apoptosis Induced by Antiblastic Agents

The potential predictive role of nuclear NHERF1 expression in advanced gastric cancer patients treated with epirubicin/oxaliplatin/capecitabine first line chemotherapy

Proteomics-based analysis of differentially expressed proteins in the CXCR1-knockdown gastric carcinoma MKN45 cell line and its parental cell

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