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The novel prognostic marker, EHMT2, is involved in cell proliferation via HSPD1 regulation in breast cancer.


ABSTRACT: Molecular classifications of breast cancer (BRC), such as human epidermal growth factor receptor 2 (HER2), luminal A and luminal B, have been developed to reduce unnecessary treatment by dividing patients with BRC into low? and high?risk progression groups. However, these methods do not cover all of the pathological characteristics of BRC, and investigations into novel prognostic/therapeutic markers are thus continually required. In this study, we identified the overexpression of the histone methyltransferase, euchromatic histone?lysine N?methyltransferase 2 (EHMT2) in BRC samples (n=1,222) and normal samples (n=113) derived from the TCGA portal by performing a BRC tissue microarray. EHMT2 overexpression was clearly associated with a poor prognosis in multiple cohorts of patients with BRC (total, n=1,644). Furthermore, the knockdown of EHMT2 expression affected cell apoptosis via the downregulation and re?localization of heat shock protein family D (Hsp60) member 1 (HSPD1). In addition, a statistically significant positive correlation between EHMT2 and HSPD1 expression was revealed in the clinical cohorts. On the whole, the findings of this study may assist the development of novel therapeutic strategies and provide a prognostic marker (EHMT2) for patients with BRC.

SUBMITTER: Kim SK 

PROVIDER: S-EPMC6254934 | biostudies-literature | 2019 Jan

REPOSITORIES: biostudies-literature

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The novel prognostic marker, EHMT2, is involved in cell proliferation via HSPD1 regulation in breast cancer.

Kim Seon-Kyu SK   Kim Kwangho K   Ryu Jea-Woon JW   Ryu Tae-Young TY   Lim Jung Hwa JH   Oh Jung-Hwa JH   Min Jeong-Ki JK   Jung Cho-Rok CR   Hamamoto Ryuji R   Son Mi-Young MY   Kim Dae-Soo DS   Cho Hyun-Soo HS  

International journal of oncology 20181026 1


Molecular classifications of breast cancer (BRC), such as human epidermal growth factor receptor 2 (HER2), luminal A and luminal B, have been developed to reduce unnecessary treatment by dividing patients with BRC into low‑ and high‑risk progression groups. However, these methods do not cover all of the pathological characteristics of BRC, and investigations into novel prognostic/therapeutic markers are thus continually required. In this study, we identified the overexpression of the histone met  ...[more]

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