FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2053226757> ?p ?o ?g. }

• W2053226757 endingPage "987" @default.
• W2053226757 startingPage "983" @default.
• W2053226757 abstract "Primary hepatocellular carcinoma (HCC) is one of the most common solid malignancies [1]. Despite recent improvements in surveillance, diagnosis and clinical treatment strategies, HCC prognosis remains dismal. Patients often experience high metastasis or recurrence rates, and postoperative 5-year survival ranges from 17 % to 53 % [2]. To date, many studies have reported aberrant gene expression in HCC, but molecular factors identified as potential therapeutic targets remain limited. Therefore, it is a challenging task to identify relevant biomarkers or potential pharmacological targets in clinical practice. The high mobility group A2 (HMGA2; also called HMGI-C) protein, a member of the high mobility group AT-hook (HMGA) family, is a small non-histone chromosomal protein that has no intrinsic transcriptional activity, but can modulate transcription by binding to DNA and altering chromatin architecture [3–5]. By interacting with many different transcription factors, HMGA2 is an important regulator of cell growth, differentiation, apoptosis, and transformation [5]. HMGA2 protein is expressed at a high level during embryogenesis, but is hardly detectable in adult human tissues [6, 7]. HMGA2 is frequently involved in chromosomal translocations that occur in benign human tumors, such as lipomas [8], uterine leiomyomas [9], and lung hamartomas [10]. Furthermore, increased HMGA2 expression has been detected in various human epithelialtype tumors, including breast cancers [11], lung cancers [12, 13], pancreatic carcinomas [14], thyroid carcinomas [15], and gastric cancers [16]. These studies suggest that HMGA2 protein overexpression may lead to neoplastic transformation. However, there have been no reports of HMGA2 expression in hepatocellular carcinoma. In this study, we investigated HMGA2 expression in HCC to determine its clinicopathologic and prognostic value." @default.
• W2053226757 created "2016-06-24" @default.
• W2053226757 creator A5024181294 @default.
• W2053226757 creator A5030711242 @default.
• W2053226757 creator A5032451912 @default.
• W2053226757 creator A5048485704 @default.
• W2053226757 date "2012-03-30" @default.
• W2053226757 modified "2023-09-23" @default.
• W2053226757 title "Expression of High Mobility GroupA2 is Associated with Poor Survival in Hepatocellular Carcinoma" @default.
• W2053226757 cites W1974514875 @default.
• W2053226757 cites W1986178112 @default.
• W2053226757 cites W2014929974 @default.
• W2053226757 cites W2016136785 @default.
• W2053226757 cites W2023865186 @default.
• W2053226757 cites W2026866722 @default.
• W2053226757 cites W2039620381 @default.
• W2053226757 cites W2040851084 @default.
• W2053226757 cites W2067213721 @default.
• W2053226757 cites W2074111101 @default.
• W2053226757 cites W2075111888 @default.
• W2053226757 cites W2082072812 @default.
• W2053226757 cites W2098914161 @default.
• W2053226757 cites W2107277218 @default.
• W2053226757 cites W2113405864 @default.
• W2053226757 cites W2127690474 @default.
• W2053226757 cites W2130937302 @default.
• W2053226757 cites W2134406847 @default.
• W2053226757 cites W2148043102 @default.
• W2053226757 cites W2153693413 @default.
• W2053226757 cites W2167837485 @default.
• W2053226757 doi "https://doi.org/10.1007/s12253-012-9514-z" @default.
• W2053226757 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/22461106" @default.
• W2053226757 hasPublicationYear "2012" @default.
• W2053226757 type Work @default.
• W2053226757 sameAs 2053226757 @default.
• W2053226757 citedByCount "11" @default.
• W2053226757 countsByYear W20532267572015 @default.
• W2053226757 countsByYear W20532267572017 @default.
• W2053226757 countsByYear W20532267572018 @default.
• W2053226757 countsByYear W20532267572019 @default.
• W2053226757 countsByYear W20532267572020 @default.
• W2053226757 countsByYear W20532267572021 @default.
• W2053226757 crossrefType "journal-article" @default.
• W2053226757 hasAuthorship W2053226757A5024181294 @default.
• W2053226757 hasAuthorship W2053226757A5030711242 @default.
• W2053226757 hasAuthorship W2053226757A5032451912 @default.
• W2053226757 hasAuthorship W2053226757A5048485704 @default.
• W2053226757 hasConcept C126322002 @default.
• W2053226757 hasConcept C143998085 @default.
• W2053226757 hasConcept C2777546739 @default.
• W2053226757 hasConcept C2778019345 @default.
• W2053226757 hasConcept C502942594 @default.
• W2053226757 hasConcept C71924100 @default.
• W2053226757 hasConcept C86803240 @default.
• W2053226757 hasConceptScore W2053226757C126322002 @default.
• W2053226757 hasConceptScore W2053226757C143998085 @default.
• W2053226757 hasConceptScore W2053226757C2777546739 @default.
• W2053226757 hasConceptScore W2053226757C2778019345 @default.
• W2053226757 hasConceptScore W2053226757C502942594 @default.
• W2053226757 hasConceptScore W2053226757C71924100 @default.
• W2053226757 hasConceptScore W2053226757C86803240 @default.
• W2053226757 hasIssue "4" @default.
• W2053226757 hasLocation W20532267571 @default.
• W2053226757 hasLocation W20532267572 @default.
• W2053226757 hasOpenAccess W2053226757 @default.
• W2053226757 hasPrimaryLocation W20532267571 @default.
• W2053226757 hasRelatedWork W2014435840 @default.
• W2053226757 hasRelatedWork W2020483997 @default.
• W2053226757 hasRelatedWork W2123895946 @default.
• W2053226757 hasRelatedWork W2390880042 @default.
• W2053226757 hasRelatedWork W2466683206 @default.
• W2053226757 hasRelatedWork W2790853126 @default.
• W2053226757 hasRelatedWork W4230673599 @default.
• W2053226757 hasRelatedWork W4232617294 @default.
• W2053226757 hasRelatedWork W4299696526 @default.
• W2053226757 hasRelatedWork W4323536446 @default.
• W2053226757 hasVolume "18" @default.
• W2053226757 isParatext "false" @default.
• W2053226757 isRetracted "false" @default.
• W2053226757 magId "2053226757" @default.
• W2053226757 workType "article" @default.