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聚糖生物标志物簇的异质性作为胰腺癌复发的一个指标

Heterogeneity of Glycan Biomarker Clusters as an Indicator of Recurrence in Pancreatic Cancer.

作者信息

Wisniewski Luke, Braak Samuel, Klamer Zachary, Gao ChongFeng, Shi Chanjuan, Allen Peter, Haab Brian B

机构信息

Department of Cell Biology, Van Andel Institute, Grand Rapids, MI, USA.

Department of Surgery, Duke University School of Medicine, Durham, NC, USA.

出版信息

bioRxiv. 2023 Jan 6:2023.01.05.522607. doi: 10.1101/2023.01.05.522607.

Abstract

Outcomes following tumor resection vary dramatically among patients with pancreatic cancer. A challenge in defining predictive biomarkers is to discern within the complex tumor tissue the specific subpopulations and relationships that drive recurrence. Multiplexed immunofluorescence is valuable for such studies when supplied with markers of relevant subpopulations and analysis methods to sort out the intra-tumor relationships that are informative of tumor behavior. We hypothesized that the glycan biomarkers CA19-9 and STRA, which detect separate subpopulations of cancer cells, define intra-tumoral features associated with recurrence. We probed this question using automated signal thresholding and spatial cluster analysis applied to the immunofluorescence images of the STRA and CA19-9 glycan biomarkers in whole-block tumor sections. The tumors (N = 22) displayed extreme diversity between them in the amounts of the glycans and in the levels of spatial clustering, but neither the amounts nor the clusters of the individual and combined glycans associated with recurrence. The combined glycans, however, marked divergent types of spatial clusters, alternatively only STRA, only CA19-9, or both. The co-occurrence of more than one cluster type within a tumor associated significantly with disease recurrence, in contrast to the independent occurrence of each type of cluster. In addition, intra-tumoral regions with heterogeneity in biomarker clusters spatially aligned with pathology-confirmed cancer cells, whereas regions with homogeneous biomarker clusters aligned with various non-cancer cells. Thus, the STRA and CA19-9 glycans are markers of distinct and co-occurring subpopulations of cancer cells that in combination are associated with recurrence. Furthermore, automated signal thresholding and spatial clustering provides a tool for quantifying intra-tumoral subpopulations that are informative of outcome.

摘要

胰腺癌患者肿瘤切除后的预后差异很大。定义预测性生物标志物的一个挑战是在复杂的肿瘤组织中辨别驱动复发的特定亚群及其关系。当提供相关亚群的标志物和分析方法以梳理出与肿瘤行为相关的肿瘤内关系时,多重免疫荧光对于此类研究很有价值。我们假设糖基生物标志物CA19-9和STRA可检测癌细胞的不同亚群,它们定义了与复发相关的肿瘤内特征。我们使用自动信号阈值化和空间聚类分析来探究这个问题,该分析应用于整块肿瘤切片中STRA和CA19-9糖基生物标志物的免疫荧光图像。这些肿瘤(N = 22)在聚糖含量和空间聚类水平上表现出极大的多样性,但单个聚糖和联合聚糖的含量及聚类均与复发无关。然而,联合聚糖标记了不同类型的空间聚类,即仅STRA、仅CA19-9或两者皆有。与每种聚类类型独立出现相比,肿瘤内出现不止一种聚类类型与疾病复发显著相关。此外,生物标志物聚类具有异质性的肿瘤内区域在空间上与病理证实的癌细胞对齐,而生物标志物聚类均匀的区域则与各种非癌细胞对齐。因此,STRA和CA19-9聚糖是癌细胞不同且同时出现的亚群的标志物,它们共同作用与复发相关。此外,自动信号阈值化和空间聚类提供了一种量化肿瘤内亚群的工具,这些亚群对预后具有指示作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/28fb/9881915/f419d5e72e02/nihpp-2023.01.05.522607v1-f0001.jpg

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