使用循环小细胞外囊泡衍生的血浆gelsolin 预测上皮性卵巢癌患者的化疗反应性。
Predicting chemoresponsiveness in epithelial ovarian cancer patients using circulating small extracellular vesicle-derived plasma gelsolin.
机构信息
Chronic Disease Program, Ottawa Hospital Research Institute, The Ottawa Hospital, Ottawa, ON, K1Y 4E9, Canada.
Department of Cellular and Molecular Medicine, Faculty of Medicine, University of Ottawa, Ottawa, ON, K1H 8L1, Canada.
出版信息
J Ovarian Res. 2023 Jan 16;16(1):14. doi: 10.1186/s13048-022-01086-x.
BACKGROUND
Resistance to chemotherapy continues to be a challenge when treating epithelial ovarian cancer (EOC), contributing to low patient survival rates. While CA125, the conventional EOC biomarker, has been useful in monitoring patients' response to therapy, there are no biomarkers used to predict treatment response prior to chemotherapy. Previous work in vitro showed that plasma gelsolin (pGSN) is highly expressed in chemoresistant EOC cell lines, where it is secreted in small extracellular vesicles (sEVs). Whether sEVs from tumour cells are secreted into the circulation of EOC patients and could be used to predict patient chemoresponsiveness is yet to be determined. This study aims to identify if sEV-pGSN in the circulation could be a predictive biomarker for chemoresistance in EOC.
METHODS
Sandwich ELISA was used to measure pGSN concentrations from plasma samples of 96 EOC patients (primarily high grade serous EOC). sEVs were isolated using ExoQuick ULTRA and characterized using western blot, nanoparticle tracking analysis, and electron microscopy after which pGSN was measured from the sEVs. Patients were stratified as platinum sensitive or resistant groups based on first progression free interval (PFI) of 6 or 12 months.
RESULTS
Total circulating pGSN was significantly decreased and sEV-pGSN increased in patients with a PFI ≤ 12 months (chemoresistant) compared to those with a PFI > 12 months (chemosensitive). The ratio of total pGSN to sEV-pGSN further differentiated these groups and was a strong predictive marker for chemoresistance (sensitivity: 73.91%, specificity: 72.46%). Predetermined CA125 was not different between chemosensitive and chemoresistant groups and was not predictive of chemoresponsiveness prior to treatment. When CA125 was combined with the ratio of total pGSN/sEV-pGSN, it was a significant predictor of chemoresponsiveness, but the test performance was not as robust as the total pGSN/sEV-pGSN alone.
CONCLUSIONS
Total pGSN/sEV-pGSN was the best predictor of chemoresponsiveness prior to treatment, outperforming the individual biomarkers (CA125, total pGSN, and sEV-pGSN). This multianalyte predictor of chemoresponsiveness could help to inform physicians' treatment and follow up plan at the time of EOC diagnosis, thus improving patients' outcomes.
背景
在治疗上皮性卵巢癌(EOC)时,化疗耐药性仍然是一个挑战,这导致患者的生存率较低。虽然 CA125 是传统的 EOC 生物标志物,在监测患者对治疗的反应方面非常有用,但在化疗前没有用于预测治疗反应的生物标志物。之前的体外研究表明,血浆凝胶蛋白(pGSN)在耐药性 EOC 细胞系中高度表达,并以小细胞外囊泡(sEVs)的形式分泌。肿瘤细胞来源的 sEV 是否分泌到 EOC 患者的循环中,并可用于预测患者的化疗反应性,目前尚不清楚。本研究旨在确定循环中的 sEV-pGSN 是否可作为 EOC 化疗耐药性的预测性生物标志物。
方法
使用夹心 ELISA 法测量 96 名 EOC 患者(主要为高级别浆液性 EOC)的血浆样本中的 pGSN 浓度。使用 ExoQuick ULTRA 分离 sEVs,并通过 Western blot、纳米颗粒跟踪分析和电子显微镜进行表征,然后测量 sEV 中的 pGSN。根据首次无进展间隔(PFI)为 6 或 12 个月,将患者分为铂类敏感或耐药组。
结果
与 PFI>12 个月(化疗敏感)的患者相比,PFI≤12 个月(化疗耐药)的患者总循环 pGSN 显著降低,sEV-pGSN 增加。总 pGSN 与 sEV-pGSN 的比值进一步区分了这些组,是化疗耐药性的强预测标志物(灵敏度:73.91%,特异性:72.46%)。预先确定的 CA125 在化疗敏感和耐药组之间没有差异,并且不能预测治疗前的化疗反应性。当 CA125 与总 pGSN/sEV-pGSN 的比值结合时,它是化疗反应性的显著预测因子,但该检测的性能不如总 pGSN/sEV-pGSN 单独使用时稳健。
结论
总 pGSN/sEV-pGSN 是化疗前预测化疗反应性的最佳标志物,优于单独的生物标志物(CA125、总 pGSN 和 sEV-pGSN)。这种化疗反应性的多分析物预测因子可帮助医生在 EOC 诊断时制定治疗和随访计划,从而改善患者的预后。
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