B7-H3和CSPG4共同靶向作为三阴性乳腺癌的泛CAR-T细胞治疗
B7-H3 and CSPG4 co-targeting as Pan-CAR-T cell treatment of triple-negative breast cancer.
作者信息
Stucchi Simone, Borea Roberto, Garcia-Recio Susana, Zingarelli Manuela, Rädler Patrick D, Camerini Elena, Marnata Pellegry Caroline, O'Connor Siobhan, Earp H Shelton, Carey Lisa A, Perou Charles M, Savoldo Barbara, Dotti Gianpietro
机构信息
Lineberger Cancer Center, University of North Carolina, Chapel Hill, North Carolina, USA.
Department of Genetics, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina, USA.
出版信息
J Immunother Cancer. 2025 May 26;13(5):e011533. doi: 10.1136/jitc-2025-011533.
PURPOSE
Chimeric antigen receptor T (CAR-T) cell therapy is under clinical investigation in patients with metastatic triple-negative breast cancer (TNBC). However, the identification of targetable antigens remains a high priority to avoid toxicity and prevent tumor escape.
EXPERIMENTAL DESIGN
Here we analyzed the gene expression of B7-H3 () and chondroitin sulfate proteoglycan 4 () in 98 TNBC samples identified in the AURORA US Network and Rapid Autopsy RNA sequencing data set at University of North Carolina (UNC). We then performed immunohistochemistry analysis for B7-H3 and CSPG4 protein expression in 151 TNBC samples collected at UNC. Finally, the validity of the proposed B7-H3 and CSGP4 co-targeting was tested in clinically relevant TNBC patient derived xenograft (PDX) models.
RESULTS
We observed that and genes are broadly and comparably expressed in TNBC samples, and gene expression is generally conserved in tumor metastases. None of the TNBC analyzed met the criteria for simultaneous low expression of and genes. Immunohistochemistry analysis showed a median H-score of 138 (105-168, lower and upper quartile, respectively) for B7-H3 expression and a median H-score of 33 (14-78 lower and upper quartile, respectively) for CSPG4 expression. Notably, 49% of the TNBC cores with B7-H3 H-score ≤105 exhibited a CSPG4 H-score exceeding its median value, and 37% and 18% of the TNBC cores with low B7-H3 expression scored CSPG4 expression above its median H-score or exceeded its upper quartile, respectively, confirming that at least one of these two proteins is expressed in 94% of the analyzed tumors. Finally, optimized dual-specific B7-H3 and CSPG4 CAR-T cells eradicated tumors with mixed antigen expression in TNBC PDX models.
CONCLUSIONS
These data highlight the clinical potential of the proposed approach that could be applicable to the great majority of patients with TNBC as well as most of patients with breast cancer in general.
目的
嵌合抗原受体T(CAR-T)细胞疗法正在转移性三阴性乳腺癌(TNBC)患者中进行临床研究。然而,确定可靶向抗原仍然是当务之急,以避免毒性并防止肿瘤逃逸。
实验设计
在此,我们分析了在AURORA美国网络中鉴定的98个TNBC样本以及北卡罗来纳大学(UNC)的快速尸检RNA测序数据集中B7-H3( )和硫酸软骨素蛋白聚糖4( )的基因表达。然后,我们对在UNC收集的151个TNBC样本进行了B7-H3和CSPG4蛋白表达的免疫组织化学分析。最后,在临床相关的TNBC患者来源异种移植(PDX)模型中测试了所提出的B7-H3和CSGP4共同靶向的有效性。
结果
我们观察到 和 基因在TNBC样本中广泛且相对均匀地表达,并且基因表达在肿瘤转移中通常是保守的。所分析的TNBC中没有一个符合 和 基因同时低表达的标准。免疫组织化学分析显示,B7-H3表达的H评分中位数为138(分别为下四分位数105和上四分位数168),CSPG4表达的H评分中位数为33(分别为下四分位数14和上四分位数78)。值得注意的是,B7-H3 H评分≤105的TNBC核心样本中有49%的CSPG4 H评分超过其中位数,B7-H3低表达的TNBC核心样本中分别有37%和18%的CSPG4表达高于其H评分中位数或超过其上四分位数,证实这两种蛋白中至少有一种在94%的分析肿瘤中表达。最后,优化的双特异性B7-H3和CSPG4 CAR-T细胞在TNBC PDX模型中根除了具有混合抗原表达的肿瘤。
结论
这些数据突出了所提出方法的临床潜力,该方法可能适用于绝大多数TNBC患者以及大多数乳腺癌患者。
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