Your search keyword '"Sujie Akesu"' showing total 10 results

1. Proteogenomic insights into the biology and treatment of pan-melanoma

Author

Hang Xiang, Rongkui Luo, Yunzhi Wang, Bing Yang, Sha Xu, Wen Huang, Shaoshuai Tang, Rundong Fang, Lingli Chen, Na Zhu, Zixiang Yu, Sujie Akesu, Chuanyuan Wei, Chen Xu, Yuhong Zhou, Jianying Gu, Jianyuan Zhao, Yingyong Hou, and Chen Ding

Subjects

Cytology, QH573-671

Abstract

Abstract Melanoma is one of the most prevalent skin cancers, with high metastatic rates and poor prognosis. Understanding its molecular pathogenesis is crucial for improving its diagnosis and treatment. Integrated analysis of multi-omics data from 207 treatment-naïve melanomas (primary-cutaneous-melanomas (CM, n = 28), primary-acral-melanomas (AM, n = 81), primary-mucosal-melanomas (MM, n = 28), metastatic-melanomas (n = 27), and nevi (n = 43)) provides insights into melanoma biology. Multivariate analysis reveals that PRKDC amplification is a prognostic molecule for melanomas. Further proteogenomic analysis combined with functional experiments reveals that the cis-effect of PRKDC amplification may lead to tumor proliferation through the activation of DNA repair and folate metabolism pathways. Proteome-based stratification of primary melanomas defines three prognosis-related subtypes, namely, the ECM subtype, angiogenesis subtype (with a high metastasis rate), and cell proliferation subtype, which provides an essential framework for the utilization of specific targeted therapies for particular melanoma subtypes. The immune classification identifies three immune subtypes. Further analysis combined with an independent anti-PD-1 treatment cohort reveals that upregulation of the MAPK7-NFKB signaling pathway may facilitate T-cell recruitment and increase the sensitivity of patients to immunotherapy. In contrast, PRKDC may reduce the sensitivity of melanoma patients to immunotherapy by promoting DNA repair in melanoma cells. These results emphasize the clinical value of multi-omics data and have the potential to improve the understanding of melanoma treatment.

Published

2024

2. Proteomic characterization identifies clinically relevant subgroups of soft tissue sarcoma

Author

Shaoshuai Tang, Yunzhi Wang, Rongkui Luo, Rundong Fang, Yufeng Liu, Hang Xiang, Peng Ran, Yexin Tong, Mingjun Sun, Subei Tan, Wen Huang, Jie Huang, Jiacheng Lv, Ning Xu, Zhenmei Yao, Qiao Zhang, Ziyan Xu, Xuetong Yue, Zixiang Yu, Sujie Akesu, Yuqin Ding, Chen Xu, Weiqi Lu, Yuhong Zhou, Yingyong Hou, and Chen Ding

Subjects

Science

Abstract

Abstract Soft tissue sarcoma is a broad family of mesenchymal malignancies exhibiting remarkable histological diversity. We portray the proteomic landscape of 272 soft tissue sarcomas representing 12 major subtypes. Hierarchical classification finds the similarity of proteomic features between angiosarcoma and epithelial sarcoma, and elevated expression of SHC1 in AS and ES is correlated with poor prognosis. Moreover, proteomic clustering classifies patients of soft tissue sarcoma into 3 proteomic clusters with diverse driven pathways and clinical outcomes. In the proteomic cluster featured with the high cell proliferation rate, APEX1 and NPM1 are found to promote cell proliferation and drive the progression of cancer cells. The classification based on immune signatures defines three immune subtypes with distinctive tumor microenvironments. Further analysis illustrates the potential association between immune evasion markers (PD-L1 and CD80) and tumor metastasis in soft tissue sarcoma. Overall, this analysis uncovers sarcoma-type-specific changes in proteins, providing insights about relationships of soft tissue sarcoma.

Published

2024

3. Proteogenomics of diffuse gliomas reveal molecular subtypes associated with specific therapeutic targets and immune-evasion mechanisms

Author

Wang, Yunzhi, Luo, Rongkui, Zhang, Xuan, Xiang, Hang, Yang, Bing, Feng, Jinwen, Deng, Mengjie, Ran, Peng, Sujie, Akesu, Zhang, Fan, Zhu, Jiajun, Tan, Subei, Xie, Tao, Chen, Pin, Yu, Zixiang, Li, Yan, Jiang, Dongxian, Zhang, Xiaobiao, Zhao, Jian-Yuan, Hou, Yingyong, and Ding, Chen

Published

2023

4. Proteomic characterization of gastric cancer response to chemotherapy and targeted therapy reveals new therapeutic strategies

Author

Li, Yan, Xu, Chen, Wang, Bing, Xu, Fujiang, Ma, Fahan, Qu, Yuanyuan, Jiang, Dongxian, Li, Kai, Feng, Jinwen, Tian, Sha, Wu, Xiaohui, Wang, Yunzhi, Liu, Yang, Qin, Zhaoyu, Liu, Yalan, Qin, Jing, Song, Qi, Zhang, Xiaolei, Sujie, Akesu, Huang, Jie, Liu, Tianshu, Shen, Kuntang, Zhao, Jian-Yuan, Hou, Yingyong, and Ding, Chen

Published

2022

5. Ciliated Muconodular Papillary Tumors of the Lung Harboring STRN::ALK Fusion: Case Report and Review of the Literature.

Author

Zhang, Xinyi, Yuan, Wei, Luo, Rongkui, Luan, Lijuan, Huang, Jie, Lu, Shaohua, Sujie, Akesu, and Hou, Yingyong

Subjects

NON-small-cell lung carcinoma, LITERATURE reviews, OLDER people, MOLECULAR spectra, COLON cancer

Abstract

Ciliated muconodular papillary tumor (CMPT) is a rare pulmonary tumor, typically occurring in middle-aged and elderly individuals. The molecular mutation spectrum of CMPT remains insufficiently explored. Commonly known driver gene alterations include KRAS, BRAF, EGFR, and ALK rearrangement. This report details the clinicopathological features of 2 patients presenting with CMPT as pulmonary nodules during clinical examinations. Microscopic analysis revealed tumors with glandular or papillary structures, consisting of mucinous cells, ciliated columnar cells, and basal cells. Notably, both patients exhibited STRN::ALK fusion, a finding not previously associated with CMPT. STRN::ALK fusion serves as a target for therapy in various tumors, including non-small cell lung cancer, thyroid cancer, and colon cancer. Consequently, we conducted a review of relevant literature, summarizing the clinicopathological and molecular characteristics of CMPT to facilitate further research. Our insights enhance the understanding of this uncommon tumor and contribute to the expansion of its molecular alteration spectrum. [ABSTRACT FROM AUTHOR]

Published

2024

6. Clinical significance of assessing Her2/neu expression in gastric cancer with dual tumor tissue paraffin blocks

Author

Ge, Xiaowen, Wang, Haixing, Zeng, Haiying, Jin, Xuejuan, Sujie, Akesu, Xu, Chen, Liu, Yalan, Huang, Jie, Ji, Yuan, Tan, Yunshan, Liu, Tianshu, Hou, Yingyong, Qin, Jing, Sun, Yihong, and Qin, Xinyu

Published

2015

7. A retrospective study of endoscopic resection for 368 patients with early esophageal squamous cell carcinoma or precancerous lesions

Author

Jiang, Dongxian, Li, Xuquan, Wang, Haixing, Xu, Chen, Li, Xiaojing, Sujie, Akesu, Zeng, Haiying, Hou, Yingyong, and Zhong, Yunshi

Published

2017

8. Serous cystic neoplasms of the pancreas: a clinicopathologic and immunohistochemical analysis

Author

JI, Yuan, WANG, Xiu Nan, LOU, Wen Hui, SUJIE, Akesu, TAN, Yun Shan, and JIN, Da Yong

Published

2006

9. Prognostic impact and potential interaction of EGFR and c-Met in the progression of esophageal squamous cell carcinoma.

Author

Wang, Haixing, Jiang, Dongxian, Song, Qi, Xu, Chen, Shi, Yuan, Li, Xiaojing, Huang, Jie, Xu, Yifan, Sujie, Akesu, Zeng, Haiying, Zhong, Yunshi, Tan, Lijie, and Hou, Yingyong

Abstract

This study is to examine EGFR and c-Met variation in precancerous lesion, early esophageal squamous cell carcinoma (ESCC), and advanced ESCC and to explore their prognostic significance. EGFR and c-Met were detected by immunohistochemistry (IHC) and fluorescence in situ hybridization (FISH). Of 158 endoscopy resection (ER) specimens, c-Met high expression and FISH positive were 44.9 and 12.6 %, respectively. EGFR high expression and FISH positive were 2.5 and 19.6 %, respectively. Of 84 surgical specimens, c-Met high expression and FISH positive were 50 and 8.3 %, respectively. EGFR high expression and FISH positive were 7.1 and 28.5 %, respectively. A significant correlation was observed between c-Met and EGFR FISH positive both in ER ( P < 0.001) and surgical specimens ( P = 0.029). Patients with EGFR high expression had poorer disease-free survival (DFS) and overall survival (OS) ( P = 0.031 and P = 0.013) in c-Met high-expression group but not in c-Met low-expression group ( P = 0.301 and P = 0.439). C-Met FISH positive did not represent a statistically significant adverse prognosis until 24 months later ( P = 0.027 and 0.048). EGFR and c-Met might be involved in the tumorigenesis and development of ESCC. EGFR high expression has different prognostic significance in patients with differing c-Met expression status. C-Met FISH positive represent delayed prognostic factor. [ABSTRACT FROM AUTHOR]

Published

2016

10. Tumour infiltrating lymphocytes correlate with improved survival in patients with esophageal squamous cell carcinoma.

Author

Jiang, Dongxian, Liu, Yalan, Wang, Hao, Wang, Haixing, Song, Qi, Sujie, Akesu, Huang, Jie, Xu, Yifan, Zeng, Haiying, Tan, Lijie, Hou, Yingyong, and Xu, Chen

Abstract

We undertook a study of tumour infiltrating lymphocytes (TILs) in a large and relatively homogeneous group of patients with completely resected esophageal squamous cell carcinoma (ESCC). Hematoxylin and eosin-stained sections of 235 ESCC tumours were evaluated for density of TILs in intratumoural (iTIL) and stromal compartments (sTIL). Foxp3+, CD4+, and CD8+ T cells in tumoural and stromal areas were evaluated by immunohistochemistry. Of the 235 tumours, high sTIL (>10%), and iTIL (>10%) were observed in 101 (43.0%) and 98 (41.7%), respectively. The median follow-up period was 36.0 months (95% CI 29.929-42.071). Univariate analysis revealed that sTIL (>10%), iTIL (>20%), vessels involvement, lymph node metastasis, and clinical stage were significantly associated with postoperative outcome. In multivariate analysis, high sTIL (HR: 0.664, P = 0.019 for Disease free survival; HR: 0.608, P = 0.005 for Overall survival) was identified as independent better prognostic factor. Further analysis, sTIL was identified as independently prognostic factor in Stage III-IVa disease, which was not found in Stage I-II disease. Our study demonstrated that sTIL was associated with better ESCC patients' survival, especially in Stage III-IVa disease. Assessment of sTIL could be useful to discriminate biological behavior for ESCC patients. [ABSTRACT FROM AUTHOR]

Published

2017