2012
DOI: 10.1634/theoncologist.2010-0379
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Losses of Chromosome 5q and 14q Are Associated with Favorable Clinical Outcome of Patients with Gastric Cancer

Abstract: Purpose. To improve the clinical outcome of patients with gastric cancer, intensified combination strategies are currently in clinical development, including combinations of more extensive surgery, (neo)adjuvant chemotherapy, and radiotherapy. The present study used DNA copy number profiling to identify subgroups of patients with different clinical outcomes. We hypothesize that, by identification of subgroups, individual treatment strategies can be selected to improve clinical outcome and to reduce unnecessary… Show more

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Cited by 30 publications
(26 citation statements)
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“…Remarkably, in a number of tumors the HSP90AA1 gene is homozygously deleted, suggesting that these tumors may have a reduced level of malignancy. This hypothesis is supported by a comparative genome-wide analysis of 206 gastric cancer patients that reported loss of HSP90AA1 is indeed associated with favorable outcomes after surgery alone (Buffart et al 2012), and is in agreement with other studies reporting that the absence of Hsp90α in tumor biopsies may serve as a biomarker for positive clinical outcomes (Gallegos et al 2008; Cheng et al 2012). …”
Section: Hsp90α and Cancersupporting
confidence: 88%
“…Remarkably, in a number of tumors the HSP90AA1 gene is homozygously deleted, suggesting that these tumors may have a reduced level of malignancy. This hypothesis is supported by a comparative genome-wide analysis of 206 gastric cancer patients that reported loss of HSP90AA1 is indeed associated with favorable outcomes after surgery alone (Buffart et al 2012), and is in agreement with other studies reporting that the absence of Hsp90α in tumor biopsies may serve as a biomarker for positive clinical outcomes (Gallegos et al 2008; Cheng et al 2012). …”
Section: Hsp90α and Cancersupporting
confidence: 88%
“…52 Its protein product negatively regulates WNT signaling and its inactivation leads to β-catenin accumulation and transcriptional activation of genes (MYC, cyclin D1) related to cell proliferation. 53,54 As reported, the chromosome locus of APC is frequently deleted in GCs, [55][56][57][58][59] and its decreased copy number significantly associated with lymph node invasion and metastasis in GC patients. 55 Moreover, APC deletion was principally found in advanced GCs, suggesting that it might be involved in the progression but not initiation of GCs.…”
Section: Chromosomementioning
confidence: 78%
“…The carcinogenesis of GC is complicated, and most patients experienced asymptomatic presentation in the early stage, resulting metastases at diagnosis. Surgical intervention, chemotherapy and radiotherapy remain to be the most curative treatment options for metastases, but the results of such trials always lead to incidence of postoperative relapse, metastasis and clinical responses [2,3]. To improve the clinical outcome of GC treatment, it is important to clarify GC pathogenesis and to investigate the genes responsible for the progress, metastasis of gastric cancer [4].…”
Section: Introductionmentioning
confidence: 99%