Guarnaccia Laura, Navone Stefania Elena, Begani Laura, Barilla Emanuela, Garzia Emanuele, Campanella Rolando, Miozzo Monica, Fontana Laura, Alotta Giovanni, Cordiglieri Chiara, Gaudino Chiara, Schisano Luigi, Ampollini Antonella, Riboni Laura, Locatelli Marco, Marfia Giovanni
Laboratory of Experimental Neurosurgery and Cell Therapy, Neurosurgery Unit, Foundation IRCCS Ca' Granda Ospedale Maggiore Policlinico, Milan, Italy.
Andremacon Srl, Milan, Italy.
Front Oncol. 2024 Aug 2;14:1355202. doi: 10.3389/fonc.2024.1355202. eCollection 2024.
Glioblastoma -wildtype (GBM) is the most malignant brain tumor in adults, with a poor prognosis of approximately 15 months after diagnosis. Most patients suffer from a recurrence in <1 year, and this renders GBM a life-threatening challenge. Among molecular mechanisms driving GBM aggressiveness, angiogenesis mediated by GBM endothelial cells (GECs) deserves consideration as a therapeutic turning point. In this scenario, calpains, a family of ubiquitously expressed calcium-dependent cysteine proteases, emerged as promising targets to be investigated as a novel therapeutic strategy and prognostic tissue biomarkers.
To explore this hypothesis, GECs were isolated from n=10 GBM biopsies and characterized phenotypically by immunofluorescence. The expression levels of calpains were evaluated by qRT-PCR and Western blot, and their association with patients' prognosis was estimated by Pearson correlation and Kaplan-Meier survival analysis. Calpain targeting efficacy was assessed by a time- and dose-dependent proliferation curve, MTT assay for viability, caspase-3/7 activity, migration and angiogenesis , and gene and protein expression level modification.
Immunofluorescence confirmed the endothelial phenotype of our primary GECs. A significant overexpression was observed for calpain-1/2/3 (CAPN) and calpain-small-subunits-1/2 (CAPNS1), whereas calpastatin gene, the calpain natural inhibitor, was reported to be downregulated. A significant negative correlation was observed between CAPN1/CAPNS1 and patient overall survival. GEC challenging revealed that the inhibition of calpain-1 exerts the strongest proapoptotic efficacy, so GEC mortality reached the 80%, confirmed by the increased activity of caspase-3/7. Functional assays revealed a strong affection of migration and angiogenesis. Gene and protein expression proved a downregulation of MAPK, VEGF/VEGFRs, and Bcl-2, and an upregulation of caspases and Bax-family mediators.
Overall, the differential expression of calpains and their correlation with patient survival suggest a novel promising target pathway, whose blockade showed encouraging results toward precision medicine strategies.
胶质母细胞瘤野生型(GBM)是成人中最恶性的脑肿瘤,诊断后的预后较差,约为15个月。大多数患者在1年内复发,这使GBM成为一个危及生命的挑战。在驱动GBM侵袭性的分子机制中,由GBM内皮细胞(GECs)介导的血管生成值得作为治疗的转折点加以考虑。在这种情况下,钙蛋白酶是一类普遍表达的钙依赖性半胱氨酸蛋白酶,作为一种新的治疗策略和预后组织生物标志物,有望成为研究的靶点。
为了探究这一假设,从10例GBM活检组织中分离出GECs,并通过免疫荧光对其进行表型鉴定。通过qRT-PCR和蛋白质印迹法评估钙蛋白酶的表达水平,并通过Pearson相关性分析和Kaplan-Meier生存分析评估其与患者预后的关系。通过时间和剂量依赖性增殖曲线、MTT活力测定、caspase-3/7活性、迁移和血管生成以及基因和蛋白质表达水平的改变来评估钙蛋白酶靶向疗效。
免疫荧光证实了我们原代GECs的内皮表型。观察到钙蛋白酶-1/2/3(CAPN)和钙蛋白酶小亚基-1/2(CAPNS1)有显著过表达,而钙蛋白酶天然抑制剂钙蛋白酶抑制蛋白基因据报道下调。观察到CAPN1/CAPNS1与患者总生存期之间存在显著负相关。对GECs的研究表明,抑制钙蛋白酶-1具有最强的促凋亡效果,因此GECs死亡率达到80%,caspase-3/7活性增加证实了这一点。功能分析显示迁移和血管生成受到强烈影响。基因和蛋白质表达证明丝裂原活化蛋白激酶(MAPK)、血管内皮生长因子/血管内皮生长因子受体(VEGF/VEGFRs)和Bcl-2下调,而半胱天冬酶和Bax家族介质上调。
总体而言,钙蛋白酶的差异表达及其与患者生存的相关性提示了一条新的有前景的靶点途径,其阻断对精准医学策略显示出令人鼓舞的结果。
