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               <h2><a href="https://www.litmetric.com/detail/32820151/The-different-role-of-YKL-40-in-glioblastoma-is-a-function-of-MGMT-promoter-methylation-status" >The different role of YKL-40 in glioblastoma is a function of MGMT promoter methylation status.</a></h2>
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                <div class="publication-auther"><a href="https://www.litmetric.com/author/Wei-Jun+Chen" class="tag" style="margin-bottom: 5px;">Wei-Jun Chen</a> <a href="https://www.litmetric.com/author/Xiang+Zhang" class="tag" style="margin-bottom: 5px;">Xiang Zhang</a> <a href="https://www.litmetric.com/author/Hua+Han" class="tag" style="margin-bottom: 5px;">Hua Han</a> <a href="https://www.litmetric.com/author/Jian-Nan+Lv" class="tag" style="margin-bottom: 5px;">Jian-Nan Lv</a> <a href="https://www.litmetric.com/author/En-Ming+Kang" class="tag" style="margin-bottom: 5px;">En-Ming Kang</a> <a href="https://www.litmetric.com/author/Yu-Lian+Zhang" class="tag" style="margin-bottom: 5px;">Yu-Lian Zhang</a> <a href="https://www.litmetric.com/author/Wei-Ping+Liu" class="tag" style="margin-bottom: 5px;">Wei-Ping Liu</a> <a href="https://www.litmetric.com/author/Xiao-Sheng+He" class="tag" style="margin-bottom: 5px;">Xiao-Sheng He</a> <a href="https://www.litmetric.com/author/James+Wang" class="tag" style="margin-bottom: 5px;">James Wang</a> <a href="https://www.litmetric.com/author/Gui-Huai+Wang" class="tag" style="margin-bottom: 5px;">Gui-Huai Wang</a> <a href="https://www.litmetric.com/author/Yan-Bing+Yu" class="tag" style="margin-bottom: 5px;">Yan-Bing Yu</a> <a href="https://www.litmetric.com/author/Wei+Zhang" class="tag" style="margin-bottom: 5px;">Wei Zhang</a></div>                   
                    <p class="mb-0 dark-color fz15 fw500 list-inline-item ml15 mb5-sm ml0-xs"><i class="flaticon-contract vam fz20 me-2"></i> Cell Death Dis</p>
              
                   <p class="mb-0 dark-color fz15 fw500 list-inline-item mr15  mb5-sm ml0-xs"><i class="flaticon-place text-thm2 vam fz20 me-2"></i> Department of Neurosurgery, Xijing Hospital, <a href='https://www.litmetric.com/search/The+Fourth+Military+Medical+University%5BAffiliation%5D' style='text-decoration: underline'>The Fourth Military Medical University</a>, Xi'an, Shaanxi, PR China. </p>
                    
                     
                   <p class="mb-0 dark-color fz15 fw500 list-inline-item ml15 mb5-sm ml0-xs"><i class="flaticon-calendar vam fz20 me-2"></i> Published: August 2020</p>
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                   <p class="text mb30"><p class="text mt10">Inter- and intratumoral heterogeneity is a hallmark of glioblastoma (GBM) that facilitates recurrence, treatment resistance, and worse prognosis. O-methylguanine-DNA methyltransferase (MGMT) promoter methylation is a significant prognostic marker for Temozolomide (TMZ) resistance in GBM patients. YKL-40 is a molecular marker for the mesenchymal subtype of GBMs and is responsible for TMZ resistance. However, underlying mechanisms by which MGMT epigenetics impacts patient outcomes and the function of YKL-40 are not fully determined. Herein, we performed in vitro and in vivo experiments, six human IDH1/2 wild-type glioblastoma stem-like cells (GSCs) were established and studied to further determine a potential interaction of YKL-40 and MGMT promoter methylation. We demonstrated that YKL-40 functioned differently in human IDH1/2 wild-type GSCs. In MGMT promoter-methylated (MGMT-m) GSCs, it acted as a tumor suppressor gene. On the other hand, in MGMT promoter-unmethylated (MGMT-um) GSCs, it promoted tumorigenesis. Notably, the reason that YKL-40 played different roles in GSCs could not be interpreted by the molecular classification of each GSCs, but is a function of MGMT promoter methylation status and involves the RAS-MEK-ERK pathway. YKL-40 mediated TMZ sensitivity by activating DNA damage responses (DDRs) in MGMT-m GSCs, and it mediated resistance to TMZ by inhibiting DDRs in MGMT-um GSCs. Our report demonstrated that MGMT promoter methylation status might influence a gene's function in human cancer. Moreover, our data also highlight the point that gene function should be investigated not only according to the molecular tumor classification, but also the epigenetic signature.</p><table class="table table-bordered table-striped downloadTable" >
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