

施煥中
從事肺臟免疫相關性疾病的基礎和臨床研究。
個性化簽名
- 姓名:施煥中
- 目前身份:
- 擔任導師情況:
- 學位:
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學術頭銜:
博士生導師, 教育部“新世紀優秀人才支持計劃”入選者
- 職稱:-
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學科領域:
內科學
- 研究興趣:從事肺臟免疫相關性疾病的基礎和臨床研究。
施煥中,男,1964年10月出生,博士,教授,國家杰出青年科學基金獲得者,現任華中科技大學同濟醫學院附屬協和醫院呼吸內科主任。
2002年獲全國優秀博士論文獎;2004年入選首批新世紀百千萬人才工程國家級人選以及國家教育部新世紀優秀人才支持計劃,獲吳階平醫學研究獎-保羅•楊森藥學研究獎,被授予衛生部有突出貢獻中青年專家稱號,同年起享受國務院政府特殊津貼;2006年獲首屆中國呼吸醫師獎;2007年獲中華醫學科技獎一等獎;2011年獲國家科學技術進步獎二等獎。
自1994年開始從事肺臟免疫相關性疾病的基礎和臨床研究。主要學術貢獻在于:(1) 證實白介素-4和白介素-5可直接導致哮喘患者的氣道炎癥和氣道高反應性,闡述調節性T細胞在哮喘發病的免疫調節活性及其作用機制,發現嗜酸粒細胞在體內能夠呈遞抗原從而參與哮喘的發病過程,長期致力于推動我國哮喘的規范化治療。關于哮喘的研究成果“支氣管哮喘的發病機制及規范化治療”獲2011年度獲國家科學技術進步獎二等獎。(2) 闡述多種T細胞亞群諸如Th17、Th22、Th9細胞及調節性T細胞等在胸腔積液中分布、表型和功能特征;發現這些免疫細胞浸潤到胸膜腔的全新機制。(3) 系統探討多種可溶性介質對于鑒別診斷良惡性胸腔積液的臨床價值,為臨床使用這些診斷指標提供循證醫學依據。
在相關學術領域編著或主編學術專著4部,作為第一作者和/或通訊作者在Am J Respir Crit Care Med、Thorax、Chest、Eur Respir J和J immunol等呼吸醫學和免疫學雜志發表科學論文40余篇,所發表論文迄今被SCI雜志他引800余次。
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施煥中
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施煥中
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施煥中, Q Zhou, Z J Ye, Y Su, J C Zhang, H Z Shi
Heart 2010; 96: 1207-1211.,-0001,():
-1年11月30日
Background N-terminal pro-brain natriuretic peptide (NT-proBNP) is a biomarker useful in diagnosis of pleural effusion due to heart failure. Thus far, its overall diagnostic accuracy has not been systematically reviewed. The aim of the present meta-analysis was to establish the overall diagnostic accuracy of the measurement of pleural NT-proBNP for identifying pleural effusion due to heart failure. Methods After a systematic review of English-language studies, sensitivity, specificity, and other measures of accuracy of NT-proBNP concentrations in pleural fluid in the diagnosis of pleural effusion resulting from heart failure were pooled using fixed-effects models. Summary receiver operating characteristic curves were used to summarise overall test performance. Results Eight publications met the inclusion criteria. The summary estimates for pleural NT-proBNP in the diagnosis of pleural effusion attributable to heart failure were: sensitivity 0.95 (95% CI 0.92 to 0.97), specificity 0.94 (0.92 to 0.96), positive likelihood ratio 14.12 (10.23 to 19.51), negative likelihood ratio 0.06 (0.04 to 0.09) and diagnostic OR 213.87 (122.50 to 373.40). Conclusions NT-proBNP levels in pleural fluid showed a high diagnostic accuracy and may help accurately differentiate cardiac from non-cardiac conditions in patients presenting with pleural effusion.
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【期刊論文】Generation and Differentiation of IL-17–Producing CD4+T Cells in Malignant Pleural Effusion
施煥中, Zhi-Jian Ye, *, Qiong Zhou, Yong-Yao Gu, ? Shou-Ming Qin, ? Wan-Li Ma, * Jian-Bao Xin, * Xiao-Nan Tao, * and Huan-Zhong Shi*
The Journal of Immunology Th17 CELLS IN MPE,-0001,():
-1年11月30日
IL-17–producing CD4+ T (Th17) cells have been found to be increased in some human cancers; however, the possible implication of Th17 cells in regulating antitumor responses in malignant pleural effusion (MPE) remains to be elucidated. In the current study, distribution and phenotypic features of Th17 cells in both MPE and peripheral blood from patients with lung cancer were determined by flow cytometry or double immunofluorescence staining. The impacts of cytokines on Th17 cell generation and differentiation were explored. The chemoattractant activity of chemokines CCL20 and CCL22 for Th17 cells in vitro was also observed. It was found that the increased Th17 cells could be found in MPE compared with blood. The in vitro experiments showed that IL-1b, IL-6, IL-23, or their various combinations could promote Th17 cell generation and differentiation from naive CD4+ T cells. MPE was chemotactic for Th17 cells, and this activity was partly blocked by anti-CCL20 and/or CCL22 Abs. Our data also showed that the accumulation of Th17 cells in MPE predicted improved patient survival. It could be concluded that the overrepresentation of Th17 cells in MPE might be due to Th17 cell differentiation and expansion stimulated by pleural proinflammatory cytokines and to recruitment of Th17 cells from peripheral blood induced by pleural chemokines CCL20 and CCL22. Furthermore, the accumulation of Th17 cells in MPE predicted improved patient survival. These data provide the basis for developing immune-boosting strategies based on ridding the cancer patient of this cell population. The Journal of Immunology,
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【期刊論文】Epithelial neutrophil-activating peptide-78 recruits neutrophils into pleural effusion
施煥中, G-N. Liu*, H-Z. Shi*, Z-H. Xie*, H-H. Shen#, H-Q. Huang#, J-M. Deng*, Q-L. Liang* and Y-B. Wu*
Eurr Respir J 2009; 34: 184-190,-0001,():
-1年11月30日
The aim of this study was to investigate the presence of epithelial neutrophil-activating peptide (ENA)-78 in pleural effusions, as well as the chemoattractant activity of pleural ENA-78 0n neutrophils. Pleural effusion and serum samples were collected from 75 patients who presented to the respiratory institute (19 with malignant pleural effusion, 21 with tuberculous pleural effusion, 18 with infectious pleural effusion and 17 with transudative pleural effusion). The concentrations of ENA-78, myeloperoxidase and neutrophil elastase were determined, and the chemoattractant activity of ENA-78 for neutrophils both in vitro and in vivo was also observed. The concentrations of ENA-78, myeloperoxidase and neutrophil elastase in infectious pleural effusion were significantly higher than those in malignant, tuberculous and transudative groups, respectively (all p<0.01). Infectious pleural fluid was chemotactic for neutrophils in vitro and anti-ENA-78 antibody could partly inhibit these chemotactic effects. Intrapleural administration of ENA-78 produced a marked progressive influx of neutrophils into pleural space. Compared with noninfectious pleural effusion, ENA-78 appeared to be increased in infectious pleural effusion. Our data suggested that ENA-78 was able to induce neutrophil infiltration into pleural space and might be responsible for pleural neutrophil degranulation.
Infections,, inflammatory cell,, neutrophil migration,, pleural effusion
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【期刊論文】CCL22 Recruits CD4-positive CD25-positive Regulatory T Cellsinto Malignant Pleural Effusion
施煥中, Xue-Jun Qin, Huan-Zhong Shi, Jing-Min Deng, Qiu-Li Liang, Jing Jiang, and Zhi-Jian Ye
Clin Cancewr Res 2009; 15(7) April 1, 2009 2231-2237,-0001,():
-1年11月30日
Purpose: The aim of this study was to explore the presence of the chemokines CCL22 and CCL17 in malignant pleural effusion, and the chemoattractant activity of these chemokines on CD4-positive CD25-positive Foxp3-positive reg ulatory Tcells infiltrating into the pleural space. Experimental Design: The concentrations of CCL22 and CCL17 in both pleural effusions and sera from 33 patients with lung cancer were determined. Flow cytometry was done to determine T lymphocyte subsets in cell pellets of pleural effusion. Pleural cells were analyzed for the expres-sion of CCL22 and CCL17. The chemoattractant activity of CCL22 for regulatory Tcells in vitro and in vivo was also observed. Results: The concentration of CCL22 in malignant pleural effusion was significantly higher than that in the corresponding serum. Pleural fluid from lung cancer patients was chemotactic for reg-ulatoryTcells, and this activity was partly blocked by an anti-CCL22, but not by an anti-CCL17 antibody. Intrapleural administration of CCL22 0f patients produced a marked progressive influx of reg ulatory T cells into pleural space. Conclusions: Compared with serum, CCL22 seemed to be increased in malignant pleural effu-sion, and could directly induce reg ulatory T cell infiltration into the pleural space in patients with malignant effusion.
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【期刊論文】Diagnostic value of carcinoembryonic antigen in malignant pleural effusion: A meta-analysis
施煥中
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【期刊論文】Diagnostic accuracy of adenosine deaminase in tuberculous pleurisy: A meta-analysis
施煥中
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【期刊論文】Diagnostic accuracy of tumour markers for malignant pleural effusion: a meta-analysis
施煥中
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