Mondaza-Hernandez José L, Hindi Nadia, Fernandez-Serra Antonio, Ramos Rafael, Gonzalez-Cámpora Ricardo, Gómez-Mateo María Carmen, Martinez-Trufero Javier, Lavernia Javier, Lopez-Pousa Antonio, Laínez Nuria, Martinez-Garcia Jeronimo, Valverde Claudia, Vaz-Salgado María Ángeles, Garcia-Plaza Gabriel, Marin-Borrero Isabel, Carrillo-Garcia Jaime, Martin-Ruiz Marta, Romero Pablo, Gutierrez Antonio, López-Guerrero Jose A, Moura David S, Martin-Broto Javier
Health Research Institute Fundacion Jimenez Diaz, Universidad Autonoma de Madrid, Madrid, Spain.
University Hospital General de Villalba, Madrid, Spain.
Ther Adv Med Oncol. 2024 Nov 4;16:17588359241293951. doi: 10.1177/17588359241293951. eCollection 2024.
Alveolar soft-part sarcoma (ASPS) is a rare tumor driven by the ASPSCR1-TFE3 fusion protein, with a propensity for metastasis. Prognostic factors remain poorly understood, and traditional chemotherapies are largely ineffective. Recent interest lies in immune checkpoint inhibitors (ICIs), yet predictive biomarkers for treatment response are lacking. Previous studies have shown promising results with ICIs in ASPS, indicating a need for further investigation into biomarkers associated with immune response.
To identify prognostic biomarkers in ASPS and to explore the role of immune-related markers, particularly L1CAM, in predicting patient outcomes.
A retrospective cohort study of 19 ASPS patients registered in the GEIS database. The study involved the collection of clinical and histopathological data, followed by an analysis of immune markers and gene expression profiles to identify potential prognostic indicators.
Clinical and histopathological data were retrospectively collected from the GEIS-26 study cohort of 19 ASPS patients. Immunohistochemistry was performed to evaluate immune markers programmed death-1 ligand (PD-L1), programmed death-1, FAS, FASL, CD8, CD3, and CD4. An HTG ImmunOncology panel was conducted on formalin-fixed paraffin-embedded samples to explore gene expression. Effects of differentially expressed genes on survival were explored by Kaplan-Meier.
PD-L1 positivity was widely observed (63%) in tumors, and CD8+ lymphocytic infiltration was common. High CD8 density correlated with greater overall survival (OS) while not statistically significant. No associations were found for other immune markers. was identified as differentially expressed in patients with low CD8 infiltration and correlated negatively with OS.
High expression correlated with poorer OS, highlighting its potential as a prognostic marker and therapeutic target in ASPS. Immunomodulatory interventions may hold promise, as evidenced by PD-L1 expression and CD8+ infiltration. Further research, including larger cohorts and international collaborations, is needed to validate these findings and explore therapeutic strategies targeting in ASPS.
肺泡软组织肉瘤(ASPS)是一种由ASPSCR1-TFE3融合蛋白驱动的罕见肿瘤,具有转移倾向。预后因素仍知之甚少,传统化疗大多无效。最近人们对免疫检查点抑制剂(ICI)产生了兴趣,但缺乏治疗反应的预测生物标志物。先前的研究表明ICI在ASPS中取得了有前景的结果,这表明需要进一步研究与免疫反应相关的生物标志物。
确定ASPS中的预后生物标志物,并探讨免疫相关标志物,特别是L1细胞黏附分子(L1CAM)在预测患者预后中的作用。
对GEIS数据库中登记的19例ASPS患者进行回顾性队列研究。该研究包括收集临床和组织病理学数据,随后分析免疫标志物和基因表达谱以确定潜在的预后指标。
从19例ASPS患者的GEIS-26研究队列中回顾性收集临床和组织病理学数据。进行免疫组织化学以评估免疫标志物程序性死亡-1配体(PD-L1)、程序性死亡-1、FAS、FAS配体、CD8、CD3和CD4。对福尔马林固定石蜡包埋样本进行HTG免疫肿瘤学检测以探索基因表达。通过Kaplan-Meier法探讨差异表达基因对生存的影响。
在肿瘤中广泛观察到PD-L1阳性(63%),并且CD8 +淋巴细胞浸润很常见。高CD8密度与更好的总生存期(OS)相关,但无统计学意义。未发现其他免疫标志物有相关性。被确定为在低CD8浸润患者中差异表达,并且与OS呈负相关。
高表达与较差的OS相关,突出了其作为ASPS预后标志物和治疗靶点的潜力。免疫调节干预可能具有前景,PD-L1表达和CD8 +浸润证明了这一点。需要进一步的研究,包括更大的队列和国际合作,以验证这些发现并探索针对ASPS中 的治疗策略。
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