叶酸水解酶-1(FOLH1)是默克尔细胞癌中基于抗体的近距离放射治疗的新靶点。
Folate hydrolase-1 (FOLH1) is a novel target for antibody-based brachytherapy in Merkel cell carcinoma.
作者信息
Ramirez-Fort M K, Meier-Schiesser B, Lachance K, Mahase S S, Church C D, Niaz M J, Liu H, Navarro V, Nikolopoulou A, Kazakov D V, Contassot E, Nguyen D P, Sach J, Hadravsky L, Sheng Y, Tagawa S T, Wu X, Lange C S, French L E, Nghiem P T, Bander N H
机构信息
Department of Life Sciences, BioFort®, Guaynabo, Puerto Rico, USA.
Department of Urology, Weill Cornell Medicine, New York, New York, USA.
出版信息
Skin Health Dis. 2021 Mar;1(1). doi: 10.1002/ski2.9. Epub 2020 Nov 28.
BACKGROUNDS
Folate Hydrolase-1 (FOLH1; PSMA) is a type II transmembrane protein, luminally expressed by solid tumour neo-vasculature. Monoclonal antibody (mAb), J591, is a vehicle for mAb-based brachytherapy in FOLH1+ cancers. Brachytherapy is a form of radiotherapy that involves placing a radioactive material a short distance from the target tissue (e.g., on the skin or internally); brachytherapy is commonly accomplished with the use of catheters, needles, metal seeds and antibody or small peptide conjugates. Herein, FOLH1 expression in primary (p) and metastatic (m) Merkel cell carcinoma (MCC) is characterized to determine its targeting potential for J591-brachytherapy.
MATERIALS & METHODS: Paraffin sections from pMCC and mMCC were evaluated by immunohistochemistry for FOLH1. Monte Carlo simulation was performed using the physical properties of conjugated radioisotope lutetium-177. Kaplan-Meier survival curves were calculated based on patient outcome data and FOLH1 expression.
RESULTS
Eighty-one MCC tumours were evaluated. 67% (54/81) of all cases, 77% (24/31) pMCC and 60% (30/50) mMCC tumours were FOLH1+. Monte Carlo simulation showed highly localized ionizing tracks of electrons emitted from the targeted neo-vessel. 42% (34/81) of patients with FOLH1+/- MCC had available survival data f or analysis. No significant differences in our limited data set were detected based on FOLH1 status ( = 0.4718; = 0.6470), staining intensity score ( = 0.6966; = 0.9841) or by grouping staining intensity scores (- and + vs. ++, +++, +++) ( = 0.8022; = 0.8496) for MCC-specific survival or recurrence free survival, respectively.
CONCLUSIONS
We report the first evidence of prevalent FOLH1 expression within MCC-associated neo-vessels, in 60-77% of patients in a large MCC cohort. Given this data, and the need for alternatives to immune therapies it is appropriate to explore the safety and efficacy o f FOLH1-targeted brachytherapy for MCC.
背景
叶酸水解酶-1(FOLH1;前列腺特异性膜抗原)是一种II型跨膜蛋白,由实体瘤新生血管在管腔内表达。单克隆抗体(mAb)J591是用于FOLH1阳性癌症中基于单克隆抗体的近距离放射治疗的载体。近距离放射治疗是一种放射治疗形式,涉及将放射性物质放置在距靶组织短距离处(例如在皮肤上或体内);近距离放射治疗通常通过使用导管、针、金属种子以及抗体或小肽缀合物来完成。在此,对原发性(p)和转移性(m)默克尔细胞癌(MCC)中FOLH1的表达进行表征,以确定其对J591近距离放射治疗的靶向潜力。
材料与方法
通过免疫组织化学对pMCC和mMCC的石蜡切片进行FOLH1评估。使用共轭放射性同位素镥-177的物理性质进行蒙特卡罗模拟。根据患者结局数据和FOLH1表达计算Kaplan-Meier生存曲线。
结果
评估了81例MCC肿瘤。所有病例的67%(54/81)、pMCC的77%(24/31)和mMCC肿瘤的60%(30/50)为FOLH1阳性。蒙特卡罗模拟显示从靶向新生血管发射的电子具有高度局部化的电离轨迹。42%(34/81)的FOLH1+/-MCC患者有可用的生存数据用于分析。在我们有限的数据集中,基于FOLH1状态(P = 0.4718;P = 0.6470)、染色强度评分(P = 0.6966;P = 0.9841)或通过将染色强度评分分组(-和+与++、+++、++++)(P = 0.8022;P = 0.8496),分别在MCC特异性生存或无复发生存方面未检测到显著差异。
结论
我们报告了首个证据,表明在一个大型MCC队列中,60%-77%的患者的MCC相关新生血管中普遍存在FOLH1表达。鉴于这些数据以及对免疫疗法替代方案的需求,探索针对MCC的FOLH1靶向近距离放射治疗的安全性和有效性是合适的。
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