Terlizzi Michela, Colarusso Chiara, De Rosa Ilaria, Somma Pasquale, Curcio Carlo, Aquino Rita P, Panico Luigi, Salvi Rosario, Zito Marino Federica, Botti Gerardo, Pinto Aldo, Sorrentino Rosalinda
Department of Pharmacy (DIFARMA), University of Salerno, Italy and ImmunePharma s.r.l., Via Giovanni Paolo II 132, Fisciano, 84084, Salerno, Italy.
ImmunePharma srl, Department of Pharmacy, University of Salerno, 84084, Fisciano, SA, Italy.
J Exp Clin Cancer Res. 2020 Nov 13;39(1):242. doi: 10.1186/s13046-020-01754-0.
Therapy/prognosis of Non-Small Cell Lung Cancer (NSCLC) patients are strongly related to gene alteration/s or protein expression. However, more than 50% of NSCLC patients are negative to key drugable biomarkers.
We used human samples of NSCLC and mouse models of lung adenocarcinoma.
We showed that caspase-4 was highly present in the tumor mass compared to non-cancerous human tissues. Interestingly, the orthologue murine caspase-11 promoted lung carcinogenesis in mice. Carcinogen-exposed caspase-11 knockout mice had lower tumor lesions than wild type mice, due to the relevance of caspase-11 in the structural lung cell as demonstrated by bone marrow transplantation and adoptive transfer experiments. Similarly to what observed in mice, caspase-4 was correlated to the stage of lung cancer in humans in that it induced cell proliferation in a K-Ras, c-MyC and IL-1α dependent manner. Caspase-4 positive adenocarcinoma (79.3%) and squamous carcinoma (88.2%) patients had lower median survival than patients who had lower levels of caspase-4. Moreover, PD-L1 expression and gene mutation (i.e. EGFR) were not correlated to caspase-4 expression. Instead, NSCLC patients who had K-Ras or c-MyC gene alteration were positively correlated to higher levels of caspase-4 and lower survival rate.
We identified a subgroup of NSCLC patients as caspase-4 positive among which double and triple positive caspase-4, K-Ras and/or c-MyC patients which prognosis was poor. Because K-Ras and c-MyC are still undrugable, the identification of caspase-4 as a novel oncoprotein could introduce novelty in the clinical yet unmet needs for NSCLC patients.
非小细胞肺癌(NSCLC)患者的治疗/预后与基因改变或蛋白质表达密切相关。然而,超过50%的NSCLC患者对关键的可靶向生物标志物呈阴性。
我们使用了NSCLC的人类样本和肺腺癌的小鼠模型。
我们发现,与非癌性人类组织相比,caspase-4在肿瘤块中高度表达。有趣的是,同源的小鼠caspase-11促进了小鼠的肺癌发生。致癌物暴露的caspase-11基因敲除小鼠的肿瘤病变比野生型小鼠少,这是由于骨髓移植和过继转移实验证明了caspase-11在肺结构细胞中的相关性。与在小鼠中观察到的情况类似,caspase-4与人类肺癌的分期相关,因为它以依赖K-Ras、c-Myc和IL-1α的方式诱导细胞增殖。caspase-4阳性的腺癌(79.3%)和鳞癌(88.2%)患者中位生存期低于caspase-4水平较低的患者。此外,PD-L1表达和基因突变(即EGFR)与caspase-4表达无关。相反,具有K-Ras或c-Myc基因改变的NSCLC患者与较高水平的caspase-4和较低的生存率呈正相关。
我们在NSCLC患者中鉴定出一个caspase-4阳性亚组,其中caspase-4、K-Ras和/或c-Myc双阳性和三阳性患者预后较差。由于K-Ras和c-Myc仍然不可靶向,将caspase-4鉴定为一种新的癌蛋白可能为NSCLC患者尚未满足的临床需求带来新的突破。
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