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find Author "周林福" 3 results
  • 胸腺基质淋巴细胞生成素在哮喘Th2优势免疫中的作用

    支气管哮喘( 简称哮喘) 是以树突状细胞( DC) 介导的Ⅱ型辅助性T 细胞( Th2) 优势免疫为特征的慢性气道炎症性疾病。哮喘气道产生大量的促炎症细胞因子, 募集嗜酸粒细胞、肥大细胞和淋巴细胞等炎症细胞, 释放一系列炎症因子, 引起气道炎症、黏膜水肿、黏液分泌和血管扩张等过敏症状。其中, 来源于上皮细胞的胸腺基质淋巴细胞生成素( thymic stromal lymphopoietin, TSLP) 在哮喘患者体内高表达, 在Th1/Th2 免疫失衡中起重要作用, 业已引起广泛关注。尤其随着对TSLP和TSLP受体( TSLPR) 的成功克隆与测序, TSLP 活化DC、启动Th2 免疫应答的分子机制, 以及TSLP在哮喘炎症上游阶段中的功能逐渐被识别, 人们对哮喘的免疫学发病机制有了更新的认识。

    Release date:2016-08-30 11:55 Export PDF Favorites Scan
  • Clinical Analysis of Erlotinib-induced Severe Rash and Fatal Interstitial Lung Disease: A Case Report and Literature Review

    ObjectiveTo improve the knowledge of erlotinib-induced severe rash and fatal interstitial lung disease (ILD). MethodsThe clinical feature and radiology of erlotinib-associated severe rash and fatal ILD were analyzed in one patient with advanced non-small cell lung cancer (NSCLC) in the 81st Hospital of Chinese PLA,and the related literatures were reviewed. ResultsThe patient was a 78-year-old male non-smoker with stage Ⅳ right lower lobe squamous cell carcinoma,and his epidermal growth factor receptor gene showed mutation at exon 21.He had a history of chronic obstructive pulmonary disease and mild pulmonary fibrosis.Following one cycle of chemotherapy with gemcitabine plus cisplatin,he received erlotinib 150 mg daily.After 40 days of targeting therapy,the size of the lung cancer was decreased significantly concomitant with severe rash.Again,severe rash and fatal ILD appeared after using erlotinib 100 mg daily for 4 days and 50 mg daily for 2 days,respectively.The tumor progressed markedly although both rash and ILD were almost abolished following withdrawal of erlotinib as well as empirical impact of glucocorticoid and sequential therapy. ConclusionPhysicians should be alerted to the possibility of erlotinib-induced severe rash and fatal ILD.Those with pathologic findings of usual interstitial pneumonia on resected lung specimens or known pulmonary fibrosis may be at particular risk for erlotinib-related pulmonary toxicity.

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  • The Efficacy of Omalizumab in Patients with Severe Allergic Asthma: A Meta-analysis

    ObjectiveTo determine the efficacy of omalizumab in patients (12~75 years of age) with severe allergic asthma, and guide its clinical application. MethodsDatabases, including Pubmed, Web of Science and Embase, were searched to collect randomized controlled trials (RCTs).Data were extracted, and the quality of included RCTs was assessed by two reviewers, followed by meta-analyses using Review Manage 5.1 software. ResultsMeta-analyses of ten included RCTs showed that, compared with placebo, omalizumab reduced the rate of exacerbation per patient during both stable-steroid phase [RR=0.56, 95% CI(0.42, 0.75), P < 0.000 1] and steroid-reduction phase for patients with severe asthma [RR=0.53, 95% CI(0.48, 0.60), P < 0.000 01], reduced the number of patients experienced at least one exacerbation [RR=0.71, 95% CI(0.61, 0.84), P < 0.000 01], and significantly reduced the dosage of beclomethasone dipropionate (≥50%) [RR=1.51, 95% CI(1.24, 1.84), P < 0.001].Omalizumab significantly improved asthma-related quality of life [RR=1.25, 95% CI(1.13, 1.38), P < 0.000 01], albeit no indications of omalizumab reducing the rate of emergency visits [RR=0.63, 95% CI(0.28, 1.44), P < 0.001]. ConclusionThe addition of omalizumab to standard asthma therapy reduces asthma exacerbations, decreases inhaled corticosteroid and rescue medication use, and improves the quality of life in severe asthma patients.

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