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评估 PTGR1 的表达模式,PTGR1 是尿路上皮癌酰基辅酶 A 敏感的潜在生物标志物。

Assessing expression patterns of PTGR1, a potential biomarker for acylfulven sensitivity in urothelial carcinoma.

机构信息

Department of Oncology, Copenhagen University Hospital, Rigshospitalet, Copenhagen, Denmark.

Department of Clinical Medicine, Copenhagen University, Copenhagen, Denmark.

出版信息

Sci Rep. 2024 Nov 10;14(1):27448. doi: 10.1038/s41598-024-79334-x.

Abstract

BACKGROUND

Metastatic urothelial carcinoma (mUC) has a poor prognosis, despite recent therapeutic advancements. Prostaglandin Reductase 1 (PTGR1) is essential for activating acylfulvens, a promising class of drugs for treating a subset of urothelial carcinoma (UC) patients. The efficacy of acylfulvens depends on PTGR1 activity and defects in the nucleotide excision repair (NER) pathway, notably ERCC2 mutations present in 10-15% of bladder tumors. This study identifies patients eligible to be included in acylfulven clinical trials based on the presence of PTGR-1 by immunohistochemistry (IHC) staining, RNA expression level and mutations in the NER pathway. Additionally, it evaluates PTGR-1 expression as a prognostic biomarker.

METHODS

Three PTGR-1 antibodies were tested in a kidney cancer cell line A498 and in tissues with known PTGR1 expression (liver, tonsils, pancreas, small intestine, etc.). Patients with untreated mUC receiving 1st line platinum from Dec. 2019 to Dec. 2021 in the Capital Region, Denmark, were included retrospectively. FFPE tumor samples were collected, and tissue microarrays (TMAs) were constructed. TMAs were stained with the best-performing PTGR1 antibody, RNA expression was analyzed using Nanostring nCounter PanCancer panel and gene mutations were assessed using a targeted genomic panel (TSO-500). Kaplan-Meier and multivariate Cox regression assessed overall survival and covariate impacts.

RESULTS

The AB181131 PTGR1 antibody was the most reliable in validation tissues. Tumors from 71 mUC patients were used to construct the TMA, and 40% of tumors scored positive for PTGR1 by IHC staining. A normalized PTGR1 RNA cutoff at 2,550 normalized counts achieved an AUC of 0.9, defining 35 samples as positive with a sensitivity of 96% and specificity of 85% in relation to IHC-positivity. Differential expression showed a significant upregulation of PTGR1 RNA in PTGR1 IHC-positive cases. NER-deficiency and PTGR1 positivity (mutations in ERCC1, ERCC2, ERCC3, ERCC4) was seen in 9 patients (13%). Median overall survival was 16 months in the cohort. Overall survival (OS) analysis indicates that overexpression of PTGR1 RNA was associated with a reduced median OS (12 months vs. 25 months, p = 0.039, log-rank).

CONCLUSION

PTGR1 IHC staining pattern using the Abcam AB181131 antibody is highly correlated with PTGR1 RNA expression. 13% in our cohort were identified as NER deficient and PTGR1 positive. Lower levels of PTGR1 indicates better outcome in this cohort.

摘要

背景

转移性尿路上皮癌(mUC)预后较差,尽管最近有了治疗进展。前列腺素还原酶 1(PTGR1)对于激活酰基辅酶 A 衍生物(酰基辅酶 A 衍生物是治疗一部分尿路上皮癌(UC)患者的有前途的药物类别)至关重要。酰基辅酶 A 衍生物的疗效取决于 PTGR1 活性和核苷酸切除修复(NER)途径的缺陷,特别是在 10-15%的膀胱癌中存在 ERCC2 突变。本研究通过免疫组织化学(IHC)染色、RNA 表达水平和 NER 途径中的突变,确定了根据 PTGR-1 存在有资格被纳入酰基辅酶 A 衍生物临床试验的患者。此外,它还评估了 PTGR-1 表达作为预后生物标志物。

方法

在肾癌细胞系 A498 中测试了三种 PTGR-1 抗体,并在具有已知 PTGR1 表达的组织(肝脏、扁桃体、胰腺、小肠等)中进行了测试。本研究回顾性纳入了 2019 年 12 月至 2021 年 12 月期间在丹麦首都地区接受一线铂类药物治疗的未经治疗的 mUC 患者。收集 FFPE 肿瘤样本,并构建组织微阵列(TMA)。使用表现最佳的 PTGR1 抗体对 TMA 进行染色,使用 Nanostring nCounter PanCancer 面板分析 RNA 表达,并使用靶向基因组面板(TSO-500)评估基因突变。Kaplan-Meier 和多变量 Cox 回归评估总生存期和协变量的影响。

结果

AB181131 PTGR1 抗体在验证组织中最可靠。来自 71 名 mUC 患者的肿瘤用于构建 TMA,40%的肿瘤通过 IHC 染色呈 PTGR1 阳性。归一化的 PTGR1 RNA 截断值为 2550 个归一化计数,获得了 0.9 的 AUC,将 35 个样本定义为阳性,与 IHC 阳性相比,其敏感性为 96%,特异性为 85%。差异表达显示 PTGR1 RNA 在 PTGR1 IHC 阳性病例中显著上调。在 9 名患者(13%)中观察到 NER 缺陷和 PTGR1 阳性(ERCC1、ERCC2、ERCC3、ERCC4 突变)。队列的中位总生存期为 16 个月。总生存(OS)分析表明,PTGR1 RNA 的过表达与中位 OS 降低相关(12 个月与 25 个月,p=0.039,对数秩)。

结论

使用 Abcam AB181131 抗体的 PTGR1 IHC 染色模式与 PTGR1 RNA 表达高度相关。我们的队列中有 13%被鉴定为 NER 缺陷和 PTGR1 阳性。该队列中 PTGR1 水平较低表明预后较好。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bd97/11551215/a30f76444d90/41598_2024_79334_Fig1_HTML.jpg

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