Anxa5 mediates the in vitro malignant behaviours of murine hepatocarcinoma Hca-F cells with high lymph node metastasis potential preferentially via ERK2/p-ERK2/c-Jun/p-c-Jun(Ser73) and E-cadherin

Sun Xujuan; Wei Bin; Liu Shuqing; Guo Chunmei; Wu Na; Liu Qinlong; Sun Ming-Zhong

首页> 外文期刊>Biomedicine & pharmacotherapy =: Biomedecine & pharmacotherapie >Anxa5 mediates the in vitro malignant behaviours of murine hepatocarcinoma Hca-F cells with high lymph node metastasis potential preferentially via ERK2/p-ERK2/c-Jun/p-c-Jun(Ser73) and E-cadherin

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Anxa5 mediates the in vitro malignant behaviours of murine hepatocarcinoma Hca-F cells with high lymph node metastasis potential preferentially via ERK2/p-ERK2/c-Jun/p-c-Jun(Ser73) and E-cadherin

机译：Anxa5优先通过ERK2 / p-ERK2 / c-Jun / p-c-Jun（Ser73）和E-cadherin介导具有高淋巴结转移潜能的鼠肝癌Hca-F细胞的体外恶性行为

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Objective: Annexin A5 (Anxa5) is associated with the progression of some cancers, while its role and regulation mechanism in tumor lymphatic metastasis is rarely reported. This study aims to investigate the influence of Anxa5 knockdown on the malignant behaviours of murine hepatocarcinoma Hca-F cell line with high lymph node metastatic (LNM) potential and the underlying regulation mechanism.

机译：目的：膜联蛋白A5（Anxa5）与某些癌症的进展有关，而其在肿瘤淋巴转移中的作用和调节机制却鲜有报道。本研究旨在探讨Anxa5基因敲除对具有高淋巴结转移（LNM）潜能的鼠肝癌Hca-F细胞系恶性行为的影响及其潜在的调控机制。

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《Biomedicine & pharmacotherapy =: Biomedecine & pharmacotherapie 》 |2016年第null期| 共10页
作者
Sun Xujuan; Wei Bin; Liu Shuqing; Guo Chunmei; Wu Na; Liu Qinlong; Sun Ming-Zhong;
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原文格式 PDF
正文语种 eng
中图分类治疗学 ;
关键词
Anxa5; Hepatocarcinoma; Malignant behaviour; ERK2; c-Jun; E-cadherin;

机译：Anxa5;肝癌;恶性行为;ERK2;c-Jun;E-钙黏着蛋白;

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1. Anxa5 mediates the in vitro malignant behaviours of murine hepatocarcinoma Hca-F cells with high lymph node metastasis potential preferentially via ERK2/p-ERK2/c-Jun/p-c-Jun(Ser73) and E-cadherin [J] . Sun Xujuan, Wei Bin, Liu Shuqing, Biomedicine & pharmacotherapy =: Biomedecine & pharmacotherapie . 2016 ,第Null期

机译：Anxa5优先通过ERK2 / p-ERK2 / c-Jun / p-c-Jun（Ser73）和E-cadherin介导具有高淋巴结转移潜能的鼠肝癌Hca-F细胞的体外恶性行为
2. siRNA targeted against matrix metalloproteinase 11 inhibits the metastatic capability of murine hepatocarcinoma cell Hca-F to lymph nodes. [J] . Jia L, Wang S, Cao J, The international journal of biochemistry and cell biology . 2007 ,第11期

机译：针对基质金属蛋白酶11的siRNA抑制了鼠肝癌细胞Hca-F转移至淋巴结的能力。
3. CRKL knockdown promotes in vitro proliferation, migration and invasion, in vivo tumor malignancy and lymph node metastasis of murine hepatocarcinoma Hca-P cells [J] . Shi Ji, Meng Longlong, Sun Ming-Zhong, Biomedicine & pharmacotherapy =: Biomedecine & pharmacotherapie . 2015 ,第Null期

机译：CRKL抑制可促进鼠肝癌Hca-P细胞的体外增殖，迁移和侵袭，体内肿瘤恶性和淋巴结转移
4. ANXA11 regulates the tumorigenesis lymph node metastasis and 5-fluorouracil sensitivity of murine hepatocarcinoma Hca-P cells by targeting c-Jun [O] . Shuqing Liu, Chunmei Guo, Jiasheng Wang, 2016

机译：ANXA11通过靶向c-Jun调节鼠肝癌Hca-P细胞的肿瘤发生淋巴结转移和5-氟尿嘧啶敏感性
5. Retraction: Modification of Glycosylation Mediates the Invasive Properties of Murine Hepatocarcinoma Cell Lines to Lymph Nodes [O] . 2019

机译：收缩：糖基化的改性介导鼠肝癌细胞系的侵入性能，淋巴结

Anxa5 mediates the in vitro malignant behaviours of murine hepatocarcinoma Hca-F cells with high lymph node metastasis potential preferentially via ERK2/p-ERK2/c-Jun/p-c-Jun(Ser73) and E-cadherin

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