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type=\u0022text\/css\u0022 rel=\u0022stylesheet\u0022 href=\u0022\/\/d282kpwvnogo5m.cloudfront.net\/sites\/default\/files\/cdn\/css\/http\/css_Xg7z6oCTVgud_Q0huYz9x9iiD5H_2YPSJ5z2ZViSWdY.css\u0022 media=\u0022all\u0022 \/\u003E\n\u003Clink rel=\u0027stylesheet\u0027 type=\u0027text\/css\u0027 href=\u0027\/sites\/all\/modules\/contrib\/panels\/plugins\/layouts\/onecol\/onecol.css\u0027 \/\u003E\u003C\/head\u003E\u003Cbody\u003E\u003Cdiv class=\u0022panels-ajax-tab-panel panels-ajax-tab-panel-sageoa-tab-art\u0022\u003E\u003Cdiv class=\u0022panel-display panel-1col clearfix\u0022 \u003E\n  \u003Cdiv class=\u0022panel-panel panel-col\u0022\u003E\n    \u003Cdiv\u003E\u003Cdiv class=\u0022panel-pane pane-highwire-markup\u0022 \u003E\n  \n      \n  \n  \u003Cdiv class=\u0022pane-content\u0022\u003E\n    \u003Cdiv class=\u0022highwire-markup\u0022\u003E\u003Cdiv xmlns=\u0022http:\/\/www.w3.org\/1999\/xhtml\u0022 id=\u0022content-block-markup\u0022 xmlns:xhtml=\u0022http:\/\/www.w3.org\/1999\/xhtml\u0022\u003E\u003Cdiv class=\u0022article fulltext-view \u0022\u003E\u003Cspan class=\u0022highwire-journal-article-marker-start\u0022\u003E\u003C\/span\u003E\u003Cdiv class=\u0022section abstract\u0022 id=\u0022abstract-1\u0022\u003E\u003Ch2\u003ESummary\u003C\/h2\u003E\n            \u003Cp id=\u0022p-1\u0022\u003EEpidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs) may reduce excision repair cross-complementing group 1 (ERCC1) gene expression, potentially enhancing sensitivity to platinum-based chemotherapy in patients with non\u2014small cell lung cancer (NSCLC), according to results from a poster presented by Cheong et al. [Cheong HT et al. \u003Cem\u003EJ Thorac Oncol\u003C\/em\u003E 2014].\u003C\/p\u003E\n         \u003C\/div\u003E\u003Cul class=\u0022kwd-group\u0022\u003E\u003Cli class=\u0022kwd\u0022\u003EOncology Genomics\u003C\/li\u003E\u003Cli class=\u0022kwd\u0022\u003ECancer Clinical Trials\u003C\/li\u003E\u003Cli class=\u0022kwd\u0022\u003ERespiratory Cancers\u003C\/li\u003E\u003C\/ul\u003E\u003Cul class=\u0022kwd-group clinical-trial\u0022\u003E\u003Cli class=\u0022kwd\u0022\u003EOncology\u003C\/li\u003E\u003Cli class=\u0022kwd\u0022\u003EOncology Genomics\u003C\/li\u003E\u003Cli class=\u0022kwd\u0022\u003ECancer\u003C\/li\u003E\u003Cli class=\u0022kwd\u0022\u003EOncology Clinical Trials\u003C\/li\u003E\u003Cli class=\u0022kwd\u0022\u003ERespiratory Cancers\u003C\/li\u003E\u003C\/ul\u003E\u003Cp id=\u0022p-2\u0022\u003EEpidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs) may reduce excision repair cross-complementing group 1 (ERCC1) gene expression, potentially enhancing sensitivity to platinum-based chemotherapy in patients with non-small cell lung cancer (NSCLC), according to results from a poster presented by Cheong et al. [Cheong HT et al. \u003Cem\u003EJ Thorac Oncol\u003C\/em\u003E 2014].\u003C\/p\u003E\u003Cp id=\u0022p-3\u0022\u003EPlatinum-based chemotherapy is the standard first-line treatment for patients with EGFR-wild-type NSCLC, whereas EGFR-TKIs are the standard for patients with the ERCC1 mutation. A Phase 3 study showed that intercalated chemotherapy and erlotinib comprise a viable first-line option for patients with EGFR-mutation-positive NSCLC or selected patients with unknown EGFR mutation status [A Randomized, Placebo-Controlled, Double-Blind Phase III Study of the Effect of First-Line Treatment With Intercalated Tarceva Versus Placebo in Combination With Gemcitabine\/Platinum on Progression-Free Survival in Patients With Stage IIIB\/IV Non-Small Cell Lung Cancer (FASTACT-2: \u003Ca class=\u0022external-ref external-ref-type-clintrialgov\u0022 href=\u0022\/lookup\/external-ref?link_type=CLINTRIALGOV\u0026amp;access_num=NCT00883779\u0026amp;atom=%2Fspmdc%2F14%2F3%2F8.atom\u0022\u003ENCT00883779\u003C\/a\u003E); Wu YL et al. \u003Cem\u003ELancet Oncol\u003C\/em\u003E 2013]. At the same time, it was reported that subgroup biomarker studies showed that patients with EGFR-wild-type and ERCC1-positive NSCLC attained longer progression-free and overall survival.\u003C\/p\u003E\u003Cp id=\u0022p-4\u0022\u003EBased on these data, Cheong et al. postulated that EGFR-TKIs downregulate ERCC1 expression in wild-type EGFR NSCLC cells, thus enhancing the efficacy of chemotherapy. To test this hypothesis, they designed \u003Cem\u003Ein vitro\u003C\/em\u003E and \u003Cem\u003Ein vivo\u003C\/em\u003E studies to study the impact of EGFR-TKIs on ERCC1 expression.\u003C\/p\u003E\u003Cp id=\u0022p-5\u0022\u003EH358 and H1993 NSCLC cell lines were treated with EGFR-TKIs for 72 hours, and transient small interfering RNA (siRNA) transfection was performed for ERCC1 suppression. Cisplatin sensitivity of the transfected cells was tested by cell viability assay. The NSCLC cell lines H358 and H1993 were used to establish a xenograft tumor model, and animals were treated with 2 weeks of oral erlotinib. ERCC1 expression was studied by Western blot, and immunohistochemistry (IHC) by the Mab clone 8F1.\u003C\/p\u003E\u003Cp id=\u0022p-6\u0022\u003EFindings indicated that ERCC1 expression is not directly related to EGFR-TKI sensitivity. The expression of ERCC1 was, however, reduced progressively throughout 72 hours of EGFR-TKI exposure. Cell sensitivity for cisplatin was increased in the ERCC1 knockdown model, and the half maximal inhibitory concentration (IC\u003Csub\u003E50\u003C\/sub\u003E) for H358 and H1993 was reduced from 11.94 \u03bcM to 0.31 \u03bcM and from 14.67 \u03bcM to 0.16 \u03bcM, respectively. Conversely, EGFR-TKIs showed no effect on tumor volume of the EGFR-wild-type xenografts, but there was a significant reduction in the ERCC1 level on IHC staining after treatment with EGFR-TKIs.\u003C\/p\u003E\u003Cp id=\u0022p-7\u0022\u003EAlmost 75% of patients with NSCLC are incurable at diagnosis. For many, chemotherapy is a good treatment option that is associated with longer survival and better quality of life. Treatment for those with advanced NSCLC is, however, palliative. Treatments that include cisplatin or carboplatin plus another agent are the most widely used drug combinations, but they can be associated with undesirable toxicity. Thus, it is desirable to have an equally or more effective treatment that is less toxic.\u003C\/p\u003E\u003Cp id=\u0022p-8\u0022\u003EOverall, this pilot study showed that reduction in the expression of the ERCC1 gene increased the sensitivity of NSCLC cells to platinum-based chemotherapy. The observations in this pilot study need to be replicated in larger trials, however.\u003C\/p\u003E\u003Cul class=\u0022copyright-statement\u0022\u003E\u003Cli class=\u0022fn\u0022 id=\u0022copyright-statement-1\u0022\u003E\u00a9 2014 MD Conference Express\u00ae\u003C\/li\u003E\u003C\/ul\u003E\u003Cspan class=\u0022highwire-journal-article-marker-end\u0022\u003E\u003C\/span\u003E\u003C\/div\u003E\u003Cspan id=\u0022related-urls\u0022\u003E\u003C\/span\u003E\u003C\/div\u003E\u003Ca href=\u0022http:\/\/mdc.sagepub.com\/content\/14\/3\/8.abstract\u0022 class=\u0022hw-link hw-link-article-abstract\u0022 data-icon-position=\u0022\u0022 data-hide-link-title=\u00220\u0022\u003EView Summary\u003C\/a\u003E\u003C\/div\u003E  \u003C\/div\u003E\n\n  \n  \u003C\/div\u003E\n\u003C\/div\u003E\n  \u003C\/div\u003E\n\u003C\/div\u003E\n\u003C\/div\u003E\u003Cscript type=\u0022text\/javascript\u0022 src=\u0022http:\/\/mdc.sagepub.com\/sites\/all\/modules\/highwire\/highwire\/plugins\/highwire_markup_process\/js\/highwire_openurl.js?nzpakd\u0022\u003E\u003C\/script\u003E\n\u003C\/body\u003E\u003C\/html\u003E"}