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151. Overexpression of endothelial cell specific molecule-1 (ESM-1) in gastric cancer

Author

Ni Liu, Gui-guo Zhang, Jiafu Ji, Lianhai Zhang, Hong Du, Ji-You Li, Xiaohong Wang, and Ying Hu

Subjects
Adult, Male, Pathology, medicine.medical_specialty, Blotting, Western, Adenocarcinoma, Immunoenzyme Techniques, Surgical oncology, Stomach Neoplasms, medicine, Humans, Clinical significance, Neoplasm Invasiveness, RNA, Messenger, RNA, Small Interfering, Gene, Cells, Cultured, Peritoneal Neoplasms, Aged, Cell Proliferation, Aged, 80 and over, Endothelial Cell-Specific Molecule 1, Neovascularization, Pathologic, business.industry, Reverse Transcriptase Polymerase Chain Reaction, Microcirculation, Liver Neoplasms, Cancer, Middle Aged, medicine.disease, Prognosis, Neoplasm Proteins, Up-Regulation, Survival Rate, Oncology, Lymphatic Metastasis, Cancer research, Disease Progression, Surgery, Female, Proteoglycans, business, Carcinoma, Signet Ring Cell, Follow-Up Studies
Abstract

The endothelial cell-specific molecule-1 (ESM-1) gene is involved in various biological events. This study was designed to clarify its clinical significance and explore its biological behavior in gastric cancer (GC).ESM-1 mRNA expression was evaluated by real-time PCR in GC (n = 34) and matched adjacent normal tissues (n = 14). The expression of ESM-1 protein was investigated by immunohistochemistry in GC (n = 159) and matched normal tissues (n = 40), and its correlation with the clinicopathological features and overall survival of patients was analyzed. Microvessel density (MVD) in GC was assessed by anti-CD34 and the pattern of ESM-1 expression in tumor-related vascular was evaluated. The effect of ESM-1 promotion of proliferation in the GC MKN28 cell line and human microvascular endothelial cell line HMEC-1 were tested using the MTT assay.ESM-1 mRNA was significantly overexpressed in GC compared with adjacent noncarcinoma controls (P 0.01). ESM-1 protein was predominantly expressed in GC. ESM-1 expression was associated with distant metastasis and Borrmann type IV (P 0.05) and was strongly associated with vascular invasion (P = 0.0057). Patients with ESM-1 expression showed lower 5-year survival rate (P = 0.0339). Multivariate analysis revealed that ESM-1 was an independent prognostic factor. In GC, CD34-MVD of GC vessels positively expressing ESM-1 was higher than that of GC with negative vessels expression of ESM-1 (P 0.05). Besides, ESM-1 antibody dose-dependently impaired MKN28 and HMEC-1 growth.ESM-1 is overexpressed in GC and can serve as a tumor biomarker to predict survival of GC patients, and it might promote tumor angiogenesis and growth in GC and, hence, may represent a potential therapeutic target.

Published
2009

152. Abstract 4692: BGB-283, a novel RAF kinase and EGFR dual inhibitor, displays potent antitumor activity in B-RAF mutated colorectal cancers

Author

Lai Wang, Lusong Luo, Shuangxi Li, Min Wei, Wenfeng Gong, Yuan Zhao, Yong Liu, Yunguang Du, Rong Du, Yi Zhang, Changyou Zhou, Rui Hao, Lianhai Zhang, Xiaoxia Hu, Yajuan Gao, Yingcai Feng, David Sutton, Xi Yuan, Jing Wei, Jiafu Ji, Shing-Hu Cheung, Guoliang Zhang, and Zhiyu Tang

Subjects
MAPK/ERK pathway, Cancer Research, Cell growth, Kinase, business.industry, Cancer, Dabrafenib, medicine.disease, Oncology, Cancer cell, Cancer research, medicine, Vemurafenib, business, EGFR inhibitors, medicine.drug
Abstract

Oncogenic B-RAF, which drives cell transformation and proliferation, has been detected in approximately 70% of human malignant melanomas and 5-15% of colorectal cancers (CRC). B-RAFV600E mutation, which gives rise to constitutive MAPK signaling, accounts for at least 90% of oncogenic B-RAF mutations. Despite the remarkable clinical activities achieved by vemurafenib and dabrafenib in treating B-RAFV600E metastatic melanoma, their clinical efficacy in B-RAFV600E CRC is far less impressive. Prior studies suggested that feedback activation of EGFR and MAPK signaling upon B-RAF inhibition contributed to the intrinsic resistance of CRC to the first generation B-RAF inhibitors. This report represents the first characterization of a dual RAF kinase/EGFR inhibitor, BGB-283, which is currently under clinical investigations. BGB-283 is a potent and selective pan-RAF and EGFR inhibitor with IC50 ranging from 5 to 47 nM on RAF and EGFR kinases. In vitro, BGB-283 potently inhibits B-RAFV600E-activated ERK phosphorylation and cell proliferation. It demonstrates selective cytotoxicity and preferentially inhibits proliferation of cancer cells harbouring B-RAFV600E and EGFR mutation/amplification. In B-RAFV600E CRC cell lines, BGB-283 effectively inhibits the reactivation of EGFR and achieved sustained inhibition of MAPK pathway. In vivo, BGB-283 is highly efficacious in inhibiting tumor growth accompanied by partial and complete tumor regressions in both BRAFV600E mutant cell derived CRC xenograft models, including HT29, Colo205, WiDr, as well as two primary human CRC xenograft models. In particular, BGB-283 shows compelling efficacy and potent inhibition of EGFR/MAPK signaling in WiDr xenograft model where EGFR reactivation occurs upon B-RAF inhibition. These findings support BGB-283 as a potent antitumor drug candidate with clinical potential for treating CRC harboring B-RAFV600E mutation. Citation Format: Zhiyu Tang, Xi Yuan, Rong Du, Shing-Hu Cheung, Guoliang Zhang, Jing Wei, Yuan Zhao, Yingcai Feng, Yi Zhang, Yunguang Du, Xiaoxia Hu, Wenfeng Gong, Yong Liu, Yajuan Gao, Rui Hao, Jiafu Ji, Lianhai Zhang, Shuangxi Li, David Sutton, Min Wei, Changyou Zhou, Lai Wang, Lusong Luo. BGB-283, a novel RAF kinase and EGFR dual inhibitor, displays potent antitumor activity in B-RAF mutated colorectal cancers. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 4692. doi:10.1158/1538-7445.AM2015-4692

Published
2015

153. Response to cetuximab by ESCC PDXs directly correlate to EGFR overexpression

Author

Jie Yang, Xuesong Huang, Xiaohong Wang, Henry Li, Jianyun Deng, Lianhai Zhang, Jiafu Ji, Sheng Guo, and Jean-Pierre Wery

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Cetuximab, business.industry, EGFR Overexpression, Esophageal squamous cell carcinoma, digestive system diseases, Internal medicine, medicine, Target therapy, business, neoplasms, medicine.drug
Abstract

e15078 Background: Esophageal squamous cell carcinoma (ESCC) is a deadly malignance prevalent in parts of China and no target therapy option. Cetuximab, approved for treating subset of metastatic c...

Published
2015

154. LAPTM4B-35, a Cancer-Related Gene, Is Associated with Poor Prognosis in TNM Stages I-III Gastric Cancer Patients

Author

Xian-Zi Wen, Xiaofang Xing, Jiafu Ji, Zhixue Zheng, Hong Du, Zhaode Bu, Ying Hu, Shen Li, Rouli Zhou, Xiaohong Wang, Lin Li, Lianhai Zhang, Xiaojing Cheng, and Xiaojiang Wu

Subjects
Adult, Male, Pathology, medicine.medical_specialty, Lymphovascular invasion, lcsh:Medicine, Biology, Disease-Free Survival, Metastasis, LAPTM4B, Cell Movement, Stomach Neoplasms, medicine, Humans, Neoplasm Invasiveness, lcsh:Science, Survival rate, Survival analysis, Aged, Cell Proliferation, Neoplasm Staging, Aged, 80 and over, Oncogene Proteins, Multidisciplinary, lcsh:R, Membrane Proteins, Cancer, Middle Aged, medicine.disease, Immunohistochemistry, Gene Expression Regulation, Neoplastic, Survival Rate, Hepatocellular carcinoma, lcsh:Q, Female, Research Article
Abstract

Background Lysosome-associated transmembrane protein 4β-35 (LAPTM4B-35), a member of the mammalian 4-tetratransmembrane spanning protein superfamily, has been reported to be overexpressed in several cancers. However the expression of LAPTM4B-35 and its role in the progression of gastric cancer (GC) remains unknown. The aim of this study was to investigate LAPTM4B-35 expression in GC, its potential relevance to clinicopathologic parameters and role of LAPTM4B-35 during gastric carcinogenesis. Methods In the present study, paraffin-embedded specimens with GC (n = 240, including 180 paired specimens) and 24 paired fresh frozen tissues were analyzed. qRT-PCR and immunohistochemistry (IHC) were used to analyze the expression of LAPTM4B-35 in GC. The effects of LAPTM4B-35 on GC cell proliferation, migration and invasion were determined by overexpression and knockdown assays. Results IHC showed that LAPTM4B-35 was expressed in 68.3% (123/180) of GC tissues, while in 16.1% (29/180) of their paired adjacent noncancerous gastric tissues (P = 0.000). LAPTM4B-35 mRNA levels in GC tissues were also significantly elevated when compared with their paired adjacent noncancerous tissues (P = 0.017). Overexpression of LAPTM4B-35 was significantly associated with degree of differentiation, depth of invasion, lymphovascular invasion and lymph node metastasis (P

Published
2015

156. Molecular profiling of hepatocellular carcinomas by cDNA microarray

Author

Jiafu Ji and Lianhai Zhang

Subjects
Carcinoma, Hepatocellular, Microarray, Gene Expression Profiling, Liver Neoplasms, Gastroenterology, General Medicine, Computational biology, Review, Biology, Malignancy, medicine.disease, Bioinformatics, Genetic analysis, digestive system diseases, Gene expression profiling, Hepatocellular carcinoma, Complementary DNA, medicine, Profiling (information science), Humans, Gene, neoplasms, Oligonucleotide Array Sequence Analysis
Abstract

Hepatocellular carcinoma (HCC) is one of the most common cancers in the world. Conventional diagnosis and treatment of this malignancy have been dismal and should be complemented by novel tools. The development and progress of HCC are believed to be caused by the accumulation of genetic changes resulting in altered expression of thousands of cancer-related genes, which can be measured by globe genetic analysis. Gene expression profiling of HCC has been employed to elucidate hepatocarcinogenesis and disclose molecular mechanisms underlying complex clinical features. Identifying phenotype-associated genes/profiles has impacts on current diagnosis and management strategy of HCC. In spite of some pitfalls of this technology and challenges in improving the research process, scrutinous validation of profiling data of HCC combined with other approaches will eventually benefit the patients.

Published
2005

157. Allelic imbalance regions on chromosomes 8p, 17p and 19p related to metastasis of hepatocellular carcinoma: comparison between matched primary and metastatic lesions in 22 patients by genome-wide microsatellite analysis

Author

Xin Wu, Zhao-You Tang, Sheng-Long Ye, Yinkun Liu, Wei Huang, Lun-Xiu Qin, Qing-Hai Ye, Lianhai Zhang, and Zeng-Chen Ma

Subjects
Adult, Male, Cancer Research, Carcinoma, Hepatocellular, Biology, Allelic Imbalance, Polymerase Chain Reaction, Metastasis, Loss of heterozygosity, Carcinoma, medicine, Humans, Aged, Liver Neoplasms, General Medicine, Middle Aged, medicine.disease, Metastasis Suppressor Gene, Oncology, Hepatocellular carcinoma, Cancer cell, Cancer research, Disease Progression, Female, Chromosomes, Human, Pair 19, Comparative genomic hybridization, Chromosomes, Human, Pair 17, Chromosomes, Human, Pair 8, Microsatellite Repeats
Abstract

To understand the molecular mechanisms of metastasis in hepatocellular carcinoma (HCC), it is necessary to identify the accumulating genetic alterations during its progression as well as those responsible for the acquisition of metastatic potential in cancer cells. In our previous study, using comparative genomic hybridization (CGH), we found that loss on chromosome 8p is more frequent in metastatic lesions than in matched primary tumors of HCC. Thus, 8p deletion might contribute to HCC metastasis. To narrow the location of metastasis-related alteration regions, we analyzed 22 primary and matched metastatic lesions of HCC by genome-wide microsatellite analysis. Common regions with high levels of allelic imbalance (AI) were identified on 17p, 8p11-cen, 8p21-23, 4q32-qter, 4q13-23, 16q, and 1p33. Regions with increased AI in metastatic lesions were 8p23.3, 8p11.2, 17p11.2-13.3, 4q21-22, 4q32-qter, 8q24.1, 9p11, 9q31, 11q23.1, 13q14.1-31, 13q32-qter, 16p13.3, 16q13, 16q22, and 19p13.1, and these were considered to be related to the metastasis phenotype. Among them, loss on 8p was again proved to be related to progression and metastasis of HCC, and 8p23.3 and 8p11.2 were two likely regions harboring metastasis-related genes. It was also shown for the first time in HCC that AI of 19p13.1 might also be related to metastatic potential. These results provide some candidate regions for further study to identify putative genes suppressing metastasis of HCC.

Published
2002

158. CMTM3 inhibits cell migration and invasion and correlates with favorable prognosis in gastric cancer

Author

Yu, Su, primary, Yi, Lin, primary, Lianhai, Zhang, primary, Baocai, Liu, primary, Xiaohong, Wang, primary, Henan, Li, primary, Xiaofang, Xing, primary, Xiaojing, Cheng, primary, Bin, Dong, primary, Ying, Hu, primary, Hong, Du, primary, Ying-ai, Li, primary, Yubing, Zhu, primary, Ning, Ding, primary, Jiyou, Li, primary, Weili, Liu, primary, Yongzhen, Ma, primary, Xiaoyan, Qiu, primary, Dalong, Ma, primary, Jiafu, Ji, primary, and Wenling, Han, primary

Published
2013
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160. Abstract B43: A subset of gastric cancers with EGFR amplification and overexpression respond to cetuximab therapy

Author

Aiwen Wu, Jiafu Ji, Ziyu Li, Shuangxi Li, Jean-Pierre Wery, Jianyun Deng, Dawei Chen, Zhongwu Li, Henry Li, Jie Cai, Mengmeng Yang, Jie Yang, Lianhai Zhang, Xiaoming Song, Yiqian Liu, Xuesong Huang, and Yiyou Chen

Subjects
Oncology, Cisplatin, Cancer Research, medicine.medical_specialty, Chemotherapy, Cetuximab, EGFR Amplification, business.industry, medicine.medical_treatment, Clinical trial, Capecitabine, Internal medicine, medicine, Effective treatment, Immunohistochemistry, business, medicine.drug
Abstract

Gastric carcinoma (GC) is a common cancer of high mortality and particularly prevalent in East Asia. There are only a few treatment options: surgery, chemotherapy, as well as Herceptin® for a small subset of patients with erbb2 amplification. Cetuximab has been approved for CRC (colorectal) and SCCHN, but not yet for gastric carcinoma. Cetuximab, combined with capecitabine/cisplatin, has recently been tested in Phase III clinical trial (EXPAND) in GC patients (1), but failed to demonstrate benefit over the existing chemotherapy (capecitabine/cisplatin). One of the reasons for the failure is only small subset of patients responding to cetuximab, which constitutes little effects on large trial populations, while the identity of the responders yet to be revealed. One of the keys to a successful search for effective treatment is the development of experimental model that truly mimics patient conditions. Patient derived xenograft (PDX or HuPrime®) is believed to best mimic human cancers (2). Recently, we have established a cohort of ∼70 GC xenograft (PDX) models from Asian and Caucasian patients. In the present study, we conducted a mouse clinical trial (MCT, or PDX trial) to test cetuximab in a cohort of GC-PDX, aiming at identifying those responsive to cetuximab. Interestingly, our trial result identified 4 of 20 (20%) GC-PDX responded to cetuximab. Genome-wide profiling and additional investigations revealed that high EGFR mRNA expression and immunohistochemistry score (3+) are associated with tumor growth inhibition. Furthermore, EGFR amplification were observed in 4/4 (50%) responders by DNAchip analysis or 2/4 confirmed with FISH analysis, with average copy number 5.8 and >15 respectively. Our data suggest that a GC subtype with EGFR amplification and overexpression benefit from cetuximab treatment. Citation Information: Mol Cancer Ther 2013;12(11 Suppl):B43. Citation Format: Lianhai Zhang, Jie Yang, Yiyou Chen, Jie Cai, Xiaoming Song, Xuesong Huang, Jianyun Deng, Dawei Chen, Mengmeng Yang, Shuangxi Li, Aiwen Wu, Ziyu Li, Zhongwu Li, Yiqian Liu, Jean-Pierre Wery, Henry Li, Jiafu Ji. A subset of gastric cancers with EGFR amplification and overexpression respond to cetuximab therapy. [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference: Molecular Targets and Cancer Therapeutics; 2013 Oct 19-23; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Ther 2013;12(11 Suppl):Abstract nr B43.

Published
2013

161. Discovery and validation of prognostic markers in gastric cancer by genome-wide expression profiling

Author

Shuqin Jia, William Cs Cho, Changqing Zeng, Feng Cheng, De-Yun Niu, Yang Gao, Yue-Zheng Zhang, Lianhai Zhang, Ni Liu, Jiafu Ji, and Chaohua Li

Subjects
Male, Kaplan-Meier Estimate, Computational biology, Bioinformatics, Stomach Neoplasms, Ribosomal protein, Biomarkers, Tumor, Humans, Profiling (information science), Medicine, Genome wide expression, Aged, Oligonucleotide Array Sequence Analysis, Genome, Human, business.industry, Gene Expression Profiling, fungi, digestive, oral, and skin physiology, Gastroenterology, food and beverages, Reproducibility of Results, General Medicine, Middle Aged, Prognosis, digestive system diseases, Gene expression profiling, Original Article, Female, business, Genome-Wide Association Study
Abstract

To develop a prognostic gene set that can predict patient overall survival status based on the whole genome expression analysis.Using Illumina HumanWG-6 BeadChip followed by semi-supervised analysis, we analyzed the expression of 47,296 transcripts in two batches of gastric cancer patients who underwent surgical resection. Thirty-nine samples in the first batch were used as the training set to discover candidate markers correlated to overall survival, and thirty-three samples in the second batch were used for validation.A panel of ten genes were identified as prognostic marker in the first batch samples and classified patients into a low- and a high-risk group with significantly different survival times (P = 0.000047). This prognostic marker was then verified in an independent validation sample batch (P = 0.0009). By comparing with the traditional Tumor-node-metastasis (TNM) staging system, this ten-gene prognostic marker showed consistent prognosis results. It was the only independent prognostic value by multivariate Cox regression analysis (P = 0.007). Interestingly, six of these ten genes are ribosomal proteins, suggesting a possible association between the deregulation of ribosome related gene expression and the poor prognosis.A ten-gene marker correlated with overall prognosis, including 6 ribosomal proteins, was identified and verified, which may complement the predictive value of TNM staging system.

Published
2011

162. Gastrectomy in comprehensive treatment of advanced gastric cancer with synchronous liver metastasis: a prospectively comparative study.

Author

Ziyu Li, Biao Fan, Fei Shan, Lei Tang, Zhaode Bu, Aiwen Wu, Lianhai Zhang, Xiaojiang Wu, Xianglong Zong, Shuangxi Li, Hui Ren, and Jiafu Ji

Subjects
GASTRECTOMY complications, STOMACH cancer treatment, LIVER metastasis, CANCER chemotherapy, ONCOLOGIC surgery
Abstract

Background: Systemic chemotherapy is the key treatment for advanced gastric cancer. The benefit of adjuvant surgery following preoperative chemotherapy in gastric cancer with liver metastasis has not been well established. Methods: Forty-nine gastric cancer patients diagnosed with synchronous liver metastasis initially treated with chemotherapy were categorized into the following two groups: surgery group: 25 patients who underwent gastrectomy and subsequently received postoperative chemotherapy and control group: 24 patients who received chemotherapy alone. Results: The median overall survival of patients in the surgery group and control group was 20.5 and 9.1 months, respectively, (P = 0.006). The median progression-free survival in the surgery group was 10.9 months, with statistical significance when compared with 5.0 months in the control group (P = 0.001). Multivariate analysis demonstrated that response to chemotherapy was the only independent factor in predicting prognosis. The survival of patients who achieved partial response (PR) was prolonged if they received adjuvant surgery (P = 0.024). No significant difference in the survival of patients underwent combined hepatic resection when compared with patients performed gastrectomy only. Conclusions: For gastric cancer with synchronous liver metastasis, adjuvant gastrectomy followed by chemotherapy might be beneficial for survival comparing with chemotherapy alone, especially in patients response to initial preoperative chemotherapy. [ABSTRACT FROM AUTHOR]

Published
2015
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163. Oncogenic HER2 fusions in gastric cancer.

Author

De-Hua Yu, Lili Tang, Hua Dong, Zhengwei Dong, Lianhai Zhang, Jiangang Fu, Xinying Su, Tianwei Zhang, Haihua Fu, Lu Han, Liang Xie, Hao Chen, Ziliang Qian, Guanshan Zhu, Jia Wang, Qingqing Ye, Jingchuan Zhang, Xiaolu Yin, Xiaolin Zhang, and Jiafu Ji

Subjects
ONCOGENIC viruses, STOMACH cancer, NEOPLASTIC cell transformation, CANCER invasiveness, TRASTUZUMAB, HER2 protein
Abstract

Background: Genetic amplification of HER2 drives tumorigenesis and cancer progression in a subset of patients with gastric cancer (GC), and treatment with trastuzumab, a humanized HER2-neutralizing antibody, improves the overall survival rate of HER2-positive patients. However, a considerable portion of the patients does not respond to trastuzumab and the molecular mechanisms underlying the intrinsic resistance to anti-HER2 therapy in GC is not fully understood. Methods: We performed whole-transcriptome sequencing on 21 HER2-positive tumor specimens from Chinese GC patients. Whole genome sequencing was performed on the three samples with HER2 fusion to discover the DNA integration structure. A multicolor FISH assay for HER2 split screening was conducted to confirm HER2 fusion and IHC (HercepTest™) was used to detect the membranous expression of HER2. Fusion cDNA were transfected into NIH/3T3 cells and generate stable cell line by lentivirus. The expression of exogenous HER2 fusion proteins and pHER2 were examined by western blot analysis. In vitro efficacy studies were also conducted by PD assay and softagar assay in cell line expression wild type and fusion HER2. T-DM1 was used to assess its binding to NIH/3T3 cells ectopically expressing wild-type and fusion HER2. Finally, the anti-tumor efficacy of trastuzumab was tested in NIH/3 T3 xenografts expressing the HER2 fusion variants. Results: We identified three new HER2 fusions with ZNF207, MDK, or NOS2 in 21 HER2-amplified GC samples (14%; 3/21). Two of the fusions, ZNF207-HER2, and MDK-HER2, which are oncogenic, lead to aberrant activation of HER2 kinase. Treatment with trastuzumab inhibited tumor growth significantly in xenografts expressing MDK-HER2 fusion. In contrast, trastuzumab had no effect on the growth of xenografts expressing ZNF207-HER2 fusion, due to its inability to bind to trastuzumab. Conclusions: Our results provide the molecular basis of a novel resistance mechanism to trastuzumab-based anti-HER2 therapy, supporting additional molecule stratification within HER2-positive GC patients for more effective therapy options. [ABSTRACT FROM AUTHOR]

Published
2015
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164. Urgent need for implementation of precision medicine in gastric cancer in China.

Author

Shuqin Jia, Lianhai Zhang, Jianmin Wu, Yang Shao, Fangping Zhao, Qijing Li, Hai Yan, Liang Zong, and Jiafu Ji

Subjects
*INDIVIDUALIZED medicine, *STOMACH cancer, *MEDICAL care, *COMPANION diagnostics, *PHARMACOGENOMICS
Abstract

The article examines the importance of precision medicine implementation in gastric cancer in China. Topics discussed include factors contributing to the decline in cancer deaths in China, anatomic, histologic and molecular classifications of gastric cancer, and challenges for precision medicine in the country.

Published
2016

165. CSBF/C10orf99, a novel potential cytokine, inhibits colon cancer cell growth through inducing G1 arrest.

Author

Wen Pan, Yingying Cheng, Heyu Zhang, Baocai Liu, Xiaoning Mo, Ting Li, Lin Li, Xiaojing Cheng, Lianhai Zhang, Jiafu Ji, Pingzhang Wang, and Wenling Han

Subjects
CYTOKINES, COLON cancer treatment, CANCER cell growth, CARCINOGENESIS, CYCLIN-dependent kinases, CYCLINS
Abstract

Cytokines are soluble proteins that exert their functions by binding specific receptors. Many cytokines play essential roles in carcinogenesis and have been developed for the treatment of cancer. In this study, we identified a novel potential cytokine using immunogenomics designated colon-derived SUSD2 binding factor (CSBF), also known as chromosome 10 open reading frame 99 (C10orf99). CSBF/C10orf99 is a classical secreted protein with predicted molecular mass of 6.5 kDa, and a functional ligand of Sushi Domain Containing 2 (SUSD2). CSBF/C10orf99 has the highest expression level in colon tissue. Both CSBF/ C10orf99 and SUSD2 are down-regulated in colon cancer tissues and cell lines with different regulation mechanisms. CSBF/C10orf99 interacts with SUSD2 to inhibit colon cancer cell growth and induce G1 cell cycle arrest by down-regulating cyclin D and cyclin-dependent kinase 6 (CDK6). CSBF/C10orf99 displays a bell-shaped activity curve with the optimal effect at∼10 ng/ml. Its growth inhibitory effects can be blocked by sSUSD2-Fc soluble protein. Our results suggest that CSBF/C10orf99 is a novel potential cytokine with tumor suppressor functions. [ABSTRACT FROM AUTHOR]

Published
2014
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166. A subset of gastric cancers with EGFR amplification and overexpression respond to cetuximab therapy.

Author

Lianhai Zhang, Jie Yang, Jie Cai, Xiaoming Song, Jianyun Deng, Xuesong Huang, Dawei Chen, Mengmeng Yang, Jean-Pierre Wery, Shuangxi Li, Aiwen Wu, Ziyu Li, Zhongwu Li, Yiqiang Liu, Yiyou Chen, Qixiang Li, and Jiafu Ji

Subjects
*CANCER patients, *CETUXIMAB, *TUMOR growth, *XENOGRAFTS, *IMMUNOHISTOCHEMISTRY
Abstract

A preclinical trial identified 4 of 20 (20%) gastric cancer (GC) patient-derived xenografts responded to cetuximab. Genome-wide profiling and additional investigations revealed that high EGFR mRNA expression and immunohistochemistry score (3+) are associated with tumor growth inhibition. Furthermore, EGFR amplification were observed in 2/4 (50%) responders with average copy number 5.8 and .15 respectively. Our data suggest that a GC subtype with EGFR amplification and overexpression benefit from cetuximab treatment. [ABSTRACT FROM AUTHOR]

Published
2013
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167. Phosphatase of regenerating liver-3 (PRL-3) is associated with metastasis and poor prognosis in gastric carcinoma.

Author

Xiaofang Xing, Shenyi Lian, Ying Hu, Ziyu Li, Lianhai Zhang, Xianzi Wen, Hong Du, Yongning Jia, Zhixue Zheng, Lin Meng, Chengchao Shou, and Jiafu Ji

Subjects
PHOSPHATASES, METASTASIS, PROGNOSIS, CARCINOMA in situ, IMMUNOHISTOCHEMISTRY
Abstract

Background PRL-3 is a member of phosphatases of regenerating liver family, characterized by phosphatase active domain and C-terminal prenylation motif. Overexpression of PRL-3 has been implicated in multiple cancers. Here we examined the clinical significance of PRL-3 in gastric cancer together with its metastatic biological functions utilizing different structural mutants. Methods PRL-3 expression was analyzed immunohistochemically in 196 gastric cancer patients and 21 cases of liver metastasis. A series of wild type PRL-3 or its mutant plasmids were expressed in BGC823 cells to investigate the relationship between its catalytic activity, cellular localization and metastatic potential in vitro. Results Positive staining of PRL-3 was observed in 19.4% (38/196) gastric cancer tissues compared with 76.2% (16/21) in liver metastasis. Statistical analysis revealed that PRL-3 expression correlated with lymph node metastasis and vascular invasion (P < 0.05). Patients with high PRL-3 expression showed poorer 5-year overall survival (P = 0.011). Wild type PRL-3 expressing cells resulted in enhanced migration and invasion ability, which were greatly crippled in form of PRL-3(C104S) or PRL-3(▵ CAAX) mutants accompanied with its alteration in subcellular localization. Conclusions Metastasis associated protein PRL-3 may serve as a potential prognostic biomarker in human gastric cancer. Both the phosphatase catalytic activity and cellular localization are critical for its function. [ABSTRACT FROM AUTHOR]

Published
2013
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168. Integration of DNA Copy Number Alterations and Transcriptional Expression Analysis in Human Gastric Cancer.

Author

Fan, Biao, Dachrut, Somkid, Coral, Ho, Siu Tsan Yuen, Kent Man Chu, Law, Simon, Lianhai Zhang, Jiafu Ji, Suet Yi Leung, and Xin Chen

Subjects
DNA, STOMACH cancer, GENOMICS, BACTERIAL artificial chromosomes, GENE expression
Abstract

Background: Genomic instability with frequent DNA copy number alterations is one of the key hallmarks of carcinogenesis. The chromosomal regions with frequent DNA copy number gain and loss in human gastric cancer are still poorly defined. It remains unknown how the DNA copy number variations contributes to the changes of gene expression profiles, especially on the global level. Principal Findings: We analyzed DNA copy number alterations in 64 human gastric cancer samples and 8 gastric cancer cell lines using bacterial artificial chromosome (BAC) arrays based comparative genomic hybridization (aCGH). Statistical analysis was applied to correlate previously published gene expression data obtained from cDNA microarrays with corresponding DNA copy number variation data to identify candidate oncogenes and tumor suppressor genes. We found that gastric cancer samples showed recurrent DNA copy number variations, including gains at 5p, 8q, 20p, 20q, and losses at 4q, 9p, 18q, 21q. The most frequent regions of amplification were 20q12 (7/72), 20q12-20q13.1 (12/72), 20q13.1-20q13.2 (11/72) and 20q13.2-20q13.3 (6/72). The most frequent deleted region was 9p21 (8/72). Correlating gene expression array data with aCGH identified 321 candidate oncogenes, which were overexpressed and showed frequent DNA copy number gains; and 12 candidate tumor suppressor genes which were down-regulated and showed frequent DNA copy number losses in human gastric cancers. Three networks of significantly expressed genes in gastric cancer samples were identified by ingenuity pathway analysis. Conclusions: This study provides insight into DNA copy number variations and their contribution to altered gene expression profiles during human gastric cancer development. It provides novel candidate driver oncogenes or tumor suppressor genes for human gastric cancer, useful pathway maps for the future understanding of the molecular pathogenesis of this malignancy, and the construction of new therapeutic targets. [ABSTRACT FROM AUTHOR]

Published
2012
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169. Neoadjuvant chemoradiation therapy for resectable esophago-gastric adenocarcinoma: a meta-analysis of randomized clinical trials

Author

Jiafu Ji, Ziyu Li, Aiwen Wu, Qiu-Shi Dong, Lianhai Zhang, Fei Shan, Xin Ji, Tao Fu, Zhaode Bu, and Xiaojiang Wu

Subjects
Oncology, medicine.medical_specialty, Cancer Research, Esophageal Neoplasms, medicine.medical_treatment, Adenocarcinoma, law.invention, Randomized controlled trial, Stomach Neoplasms, law, Internal medicine, medicine, Genetics, Humans, Overall survival, Neoadjuvant therapy, Survival analysis, Randomized Controlled Trials as Topic, business.industry, Hazard ratio, Chemoradiotherapy, Perioperative, Prognosis, medicine.disease, Combined Modality Therapy, Survival Analysis, Neoadjuvant Therapy, Radiation therapy, Meta-analysis, Esophago-gastric adenocarcinoma, Preoperative chemoradiation therapy, Radiology, business, Research Article
Abstract

Background The efficacy and safety of preoperative chemoradiation therapy (CRT) for advanced esophago-gastric adenocarcinoma are still in question, and the prognosis of these patients is poor. Methods We systematically searched electronic databases from January 1990 to July 2014. The primary outcome was overall survival. The secondary outcomes were a R0 resection rate, positive rate of lymph node metastasis, postoperative recurrence rate, pathological complete response (pCR) rate and perioperative mortality. Overall survival was measured with a hazard ratio (HR), while other secondary outcomes were measured with an odds ratio (OR). Results Seven randomized controlled trials (RCTs) including 1085 patients were searched and, of these, 869 had adenocarcinoma. Patients receiving preoperative CRT had a longer overall survival (HR 0.74; 95% confidence interval (CI) 0.63–0.88), higher likelihood of R0 resection and greater chance of pCR, while they had a lower likelihood of lymph node metastasis and postoperative recurrence. The difference of perioperative mortality was non-significant. In addition, the result of the comparison between preoperative CRT and preoperative chemotherapy (CT) in two RCTs was non-significant. Conclusion Patients with resectable esophago-gastric adenocarcinoma can gain a survival advantage from preoperative CRT. However, limited to the number of RCTs, the effect of adding radiotherapy to preoperative CT separately is still uncertain and more high-quality prospective trials are needed.

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170. International network of cancer genome projects

Author

Thomas J, Hudson, Warwick, Anderson, Axel, Artez, Anna D, Barker, Cindy, Bell, Rosa R, Bernabé, M K, Bhan, Fabien, Calvo, Iiro, Eerola, Daniela S, Gerhard, Alan, Guttmacher, Mark, Guyer, Fiona M, Hemsley, Jennifer L, Jennings, David, Kerr, Peter, Klatt, Patrik, Kolar, Jun, Kusada, David P, Lane, Frank, Laplace, Lu, Youyong, Gerd, Nettekoven, Brad, Ozenberger, Jane, Peterson, T S, Rao, Jacques, Remacle, Alan J, Schafer, Tatsuhiro, Shibata, Michael R, Stratton, Joseph G, Vockley, Koichi, Watanabe, Huanming, Yang, Matthew M F, Yuen, Bartha M, Knoppers, Martin, Bobrow, Anne, Cambon-Thomsen, Lynn G, Dressler, Stephanie O M, Dyke, Yann, Joly, Kazuto, Kato, Karen L, Kennedy, Pilar, Nicolás, Michael J, Parker, Emmanuelle, Rial-Sebbag, Carlos M, Romeo-Casabona, Kenna M, Shaw, Susan, Wallace, Georgia L, Wiesner, Nikolajs, Zeps, Peter, Lichter, Andrew V, Biankin, Christian, Chabannon, Lynda, Chin, Bruno, Clément, Enrique, de Alava, Françoise, Degos, Martin L, Ferguson, Peter, Geary, D Neil, Hayes, Amber L, Johns, Arek, Kasprzyk, Hidewaki, Nakagawa, Robert, Penny, Miguel A, Piris, Rajiv, Sarin, Aldo, Scarpa, Marc, van de Vijver, P Andrew, Futreal, Hiroyuki, Aburatani, Mónica, Bayés, David D L, Botwell, Peter J, Campbell, Xavier, Estivill, Sean M, Grimmond, Ivo, Gut, Martin, Hirst, Carlos, López-Otín, Partha, Majumder, Marco, Marra, John D, McPherson, Zemin, Ning, Xose S, Puente, Yijun, Ruan, Hendrik G, Stunnenberg, Harold, Swerdlow, Victor E, Velculescu, Richard K, Wilson, Hong H, Xue, Liu, Yang, Paul T, Spellman, Gary D, Bader, Paul C, Boutros, Paul, Flicek, Gad, Getz, Roderic, Guigó, Guangwu, Guo, David, Haussler, Simon, Heath, Tim J, Hubbard, Tao, Jiang, Steven M, Jones, Qibin, Li, Nuria, López-Bigas, Ruibang, Luo, Lakshmi, Muthuswamy, B F Francis, Ouellette, John V, Pearson, Victor, Quesada, Benjamin J, Raphael, Chris, Sander, Terence P, Speed, Lincoln D, Stein, Joshua M, Stuart, Jon W, Teague, Yasushi, Totoki, Tatsuhiko, Tsunoda, Alfonso, Valencia, David A, Wheeler, Honglong, Wu, Shancen, Zhao, Guangyu, Zhou, Mark, Lathrop, Gilles, Thomas, Teruhiko, Yoshida, Myles, Axton, Chris, Gunter, Linda J, Miller, Junjun, Zhang, Syed A, Haider, Jianxin, Wang, Christina K, Yung, Anthony, Cros, Anthony, Cross, Yong, Liang, Saravanamuttu, Gnaneshan, Jonathan, Guberman, Jack, Hsu, Don R C, Chalmers, Karl W, Hasel, Terry S H, Kaan, William W, Lowrance, Tohru, Masui, Laura Lyman, Rodriguez, Catherine, Vergely, David D L, Bowtell, Nicole, Cloonan, Anna, deFazio, James R, Eshleman, Dariush, Etemadmoghadam, Brooke B, Gardiner, Brooke A, Gardiner, James G, Kench, Robert L, Sutherland, Margaret A, Tempero, Nicola J, Waddell, Peter J, Wilson, Steve, Gallinger, Ming-Sound, Tsao, Patricia A, Shaw, Gloria M, Petersen, Debabrata, Mukhopadhyay, Ronald A, DePinho, Sarah, Thayer, Kamran, Shazand, Timothy, Beck, Michelle, Sam, Lee, Timms, Vanessa, Ballin, Youyong, Lu, Jiafu, Ji, Xiuqing, Zhang, Feng, Chen, Xueda, Hu, Qi, Yang, Geng, Tian, Lianhai, Zhang, Xiaofang, Xing, Xianghong, Li, Zhenggang, Zhu, Yingyan, Yu, Jun, Yu, Jörg, Tost, Paul, Brennan, Ivana, Holcatova, David, Zaridze, Alvis, Brazma, Lars, Egevard, Egor, Prokhortchouk, Rosamonde Elizabeth, Banks, Mathias, Uhlén, Juris, Viksna, Fredrik, Ponten, Konstantin, Skryabin, Ewan, Birney, Ake, Borg, Anne-Lise, Børresen-Dale, Carlos, Caldas, John A, Foekens, Sancha, Martin, Jorge S, Reis-Filho, Andrea L, Richardson, Christos, Sotiriou, Giles, Thoms, Laura, van't Veer, Daniel, Birnbaum, Hélène, Blanche, Pascal, Boucher, Sandrine, Boyault, Jocelyne D, Masson-Jacquemier, Iris, Pauporté, Xavier, Pivot, Anne, Vincent-Salomon, Eric, Tabone, Charles, Theillet, Isabelle, Treilleux, Paulette, Bioulac-Sage, Thomas, Decaens, Dominique, Franco, Marta, Gut, Didier, Samuel, Jessica, Zucman-Rossi, Roland, Eils, Benedikt, Brors, Jan O, Korbel, Andrey, Korshunov, Pablo, Landgraf, Hans, Lehrach, Stefan, Pfister, Bernhard, Radlwimmer, Guido, Reifenberger, Michael D, Taylor, Christof, von Kalle, Partha P, Majumder, Paolo, Pederzoli, Rita A, Lawlor, Massimo, Delledonne, Alberto, Bardelli, Thomas, Gress, David, Klimstra, Giuseppe, Zamboni, Yusuke, Nakamura, Satoru, Miyano, Akihiro, Fujimoto, Elias, Campo, Silvia, de Sanjosé, Emili, Montserrat, Marcos, González-Díaz, Pedro, Jares, Heinz, Himmelbauer, Heinz, Himmelbaue, Silvia, Bea, Samuel, Aparicio, Douglas F, Easton, Francis S, Collins, Carolyn C, Compton, Eric S, Lander, Wylie, Burke, Anthony R, Green, Stanley R, Hamilton, Olli P, Kallioniemi, Timothy J, Ley, Edison T, Liu, Brandon J, Wainwright, CCA -Cancer Center Amsterdam, Pathology, Other departments, Foie, métabolismes et cancer, Université de Rennes 1 (UR1), Université de Rennes (UNIV-RENNES)-Université de Rennes (UNIV-RENNES)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), Universitat de Barcelona, The International Cancer Genome Consortium, and Université de Rennes (UR)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique )

Subjects
Cancer therapy, Carcinogenesis, Genetics, Medical, International Cooperation, Systems biology, DNA Mutational Analysis, education, Genomics, Biology, Genome, Article, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Oncogènesi, Neoplasms, Databases, Genetic, medicine, Cancer genomics, Humans, Càncer, Molecular Biology, Cancer, 030304 developmental biology, Genetics, 0303 health sciences, Multidisciplinary, Genome, Human, [SDV.MHEP.HEG]Life Sciences [q-bio]/Human health and pathology/Hépatology and Gastroenterology, DNA Methylation, medicine.disease, Intellectual Property, Human genetics, 3. Good health, Cancer Genome Project, 030220 oncology & carcinogenesis, Mutation, cancer genome projects, Human genome, Genes, Neoplasm
Abstract

International audience; The International Cancer Genome Consortium (ICGC) was launched to coordinate large-scale cancer genome studies in tumors from 50 different cancer types and/or subtypes that are of clinical and societal importance across the globe. Systematic studies of over 25,000 cancer genomes at the genomic, epigenomic, and transcriptomic levels will reveal the repertoire of oncogenic mutations, uncover traces of the mutagenic influences, define clinically-relevant subtypes for prognosis and therapeutic management, and enable the development of new cancer therapies.

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