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喉癌淋巴结转移和无病生存期与 MASPIN 核表达相关,而与 EGFR 表达无关:108 例系列研究。

Laryngeal carcinoma lymph node metastasis and disease-free survival correlate with MASPIN nuclear expression but not with EGFR expression: a series of 108 cases.

机构信息

Otolaryngology Section, Department of Medical and Surgical Specialties, University of Padova, Via Giustiniani 2, 35128 Padua, Italy.

出版信息

Eur Arch Otorhinolaryngol. 2010 Jul;267(7):1103-10. doi: 10.1007/s00405-009-1186-2. Epub 2010 Jan 6.

DOI:10.1007/s00405-009-1186-2
PMID:20052590
Abstract

Despite advances in laryngeal squamous cell carcinoma (LSCC) treatment, patient survival has not improved in the last two decades. Novel, more effective strategies should be based on receptor-mediated LSCC-targeted therapy. The epidermal growth factor receptor (EGFR) is the most widely studied molecular target. MASPIN multifaceted anti-tumor effects have been rarely evaluated in LSCC. The aims of this study were to investigate EGFR and MASPIN expression and the role of sub-cellular MASPIN localization in LSSC. MASPIN and EGFR expression and the sub-cellular localization of MASPIN were assessed using a computerized image analysis system in 108 consecutive cases of operable LSCC. The rates of occurrence of lymph node metastases and recurrent disease were lower in patients with a nuclear pattern of MASPIN expression (p = 0.004, p = 0.0028). As expected, the loco-regional recurrence rate was lower in N0 patients (p = 0.009), but the disease recurrence rate was even lower in N0 patients with a nuclear localization of MASPIN (p = 0.020). Disease-free survival was longer in cases of LSCC with a nuclear MASPIN pattern (p = 0.003). The intensity of EGFR reactivity and the EGFR area fraction were unrelated to the clinico-pathological and prognostic parameters in LSCC. A nuclear MASPIN pattern is a promising prognostic indicator in LSCC, but further evidence is needed before elective neck dissection can be considered for cN0 LSCCs with a non-nuclear MASPIN pattern. Although a better understanding of the mechanisms behind sub-cellular MASPIN localization is mandatory, re-activating nuclear MASPIN in association with specific chemotherapeutic agents may be an important goal in the treatment of LSCC.

摘要

尽管喉鳞状细胞癌(LSCC)的治疗取得了进展,但在过去的二十年中,患者的生存率并未提高。新的、更有效的策略应该基于受体介导的 LSCC 靶向治疗。表皮生长因子受体(EGFR)是研究最广泛的分子靶标。MASPIN 的多方面抗肿瘤作用在 LSCC 中很少被评估。本研究旨在探讨 EGFR 和 MASPIN 的表达以及亚细胞 MASPIN 定位在 LSCC 中的作用。在 108 例可手术 LSCC 连续病例中,使用计算机图像分析系统评估 MASPIN 和 EGFR 的表达以及 MASPIN 的亚细胞定位。具有核型 MASPIN 表达的患者发生淋巴结转移和复发病例的比率较低(p=0.004,p=0.0028)。正如预期的那样,N0 患者的局部区域复发率较低(p=0.009),但核型 MASPIN 定位的 N0 患者的疾病复发率更低(p=0.020)。具有核型 MASPIN 模式的 LSCC 患者的无病生存率更长(p=0.003)。EGFR 反应性的强度和 EGFR 面积分数与 LSCC 的临床病理和预后参数无关。核型 MASPIN 模式是 LSCC 有前途的预后指标,但需要进一步的证据,才能考虑对具有非核型 MASPIN 模式的 cN0 LSCC 进行选择性颈部解剖。尽管需要更好地了解亚细胞 MASPIN 定位背后的机制,但与特定化疗药物联合重新激活核型 MASPIN 可能是治疗 LSCC 的一个重要目标。

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本文引用的文献

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Maspin polymorphism associated with apoptosis susceptibility and in vivo tumorigenesis.与凋亡易感性和体内肿瘤发生相关的乳清酸性蛋白多态性
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Elderly patients at higher risk of laryngeal carcinoma recurrence could be identified by a panel of two biomarkers (nm23-H1 and CD105) and pN+ status.通过由两种生物标志物(nm23-H1和CD105)及pN+状态组成的指标体系,可识别出喉癌复发风险较高的老年患者。
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Protein mislocalization: mechanisms, functions and clinical applications in cancer.蛋白质错误定位:癌症中的机制、功能及临床应用
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A prognostic role for Nm23-H1 in laryngeal carcinoma treated with postoperative radiotherapy: an introductory investigation.Nm23-H1 在喉癌术后放疗中的预后作用:初步研究。
Eur Arch Otorhinolaryngol. 2013 Jan;270(1):197-203. doi: 10.1007/s00405-012-2133-1. Epub 2012 Aug 3.
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Laryngeal carcinoma prognosis after postoperative radiotherapy correlates with CD105 expression, but not with angiogenin or EGFR expression.喉癌术后放疗的预后与 CD105 表达相关,而与血管生成素或 EGFR 表达无关。
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