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首页> 外文期刊>Oncology reports >Suppression of bladder cancer cell tumorigenicity in an athymic mouse model by adenoviral vector-mediated transfer of LRIG1.
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Suppression of bladder cancer cell tumorigenicity in an athymic mouse model by adenoviral vector-mediated transfer of LRIG1.

机译:腺病毒载体介导的LRIG1转移抑制无胸腺小鼠模型中膀胱癌细胞致瘤性。

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摘要

Previous in vitro studies demonstrated that leucine-rich repeats and immunoglobulin-like domains 1 (LRIG1), a negative regulator of EGFR, is a novel agent for suppressing bladder cancer. However, the role that LRIG1 plays in bladder cancer growth in vivo has not been elucidated in animal or clinical studies. Thus, to evaluate the suppressive effects of LRIG1 on human invasive bladder cancer in vivo, we transferred LRIG1 into athymic mice bearing T24 invasive bladder cancer xenografts mediated by an adenoviral vector. Correlations between LRIG1 expression and tumorigenicity, EGFR expression, xenograft proliferation and angiogenesis were assessed, respectively. The results indicated that tumor volume growth was retarded via Ad-LRIG1 intratumoral injection. In addition LRIG1 upregulation was well correlated with a reduction in EGFR expression and the proliferation rate of xenografts. Furthermore, microvessel densities were reduced and correlated with Ad-LRIG1 administration. No significant macroscopic and microscopic pathological abnormality was observed in the liver, kidney and lungs of Ad-LRIG1-administered mice. This new insight provides evidence that downregulation of EGFR expression by LRIG1 may comprise a potential novel and safe therapeutic approach for improving the prognosis of invasive bladder cancer.
机译:先前的体外研究表明,富含亮氨酸的重复序列和免疫球蛋白样结构域1(LRIG1)是EGFR的负调节剂,是抑制膀胱癌的新型药物。然而,在动物或临床研究中尚未阐明LRIG1在体内膀胱癌生长中的作用。因此,为了评估LRIG1在体内对人浸润性膀胱癌的抑制作用,我们将LRIG1转移到携带由腺病毒载体介导的T24浸润性膀胱癌异种移植物的无胸腺小鼠中。分别评估了LRIG1表达与致瘤性,EGFR表达,异种移植物增殖和血管生成之间的相关性。结果表明通过肿瘤内注射Ad-LRIG1,肿瘤体积的生长受到阻碍。此外,LRIG1的上调与EGFR表达的降低和异种移植物的增殖率密切相关。此外,微血管密度降低并与Ad-LRIG1给药相关。在Ad-LRIG1给药小鼠的肝,肾和肺中未观察到明显的宏观和微观病理异常。这一新见解提供了证据,表明LRIG1下调EGFR表达可能是改善浸润性膀胱癌预后的潜在新颖安全的治疗方法。

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