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https://doi.org/10.3389/fonc.2022.939460
Title: | Pro-metastatic and mesenchymal gene expression signatures characterize circulating tumor cells of neuroblastoma patients with bone marrow metastases and relapse | Authors: | Loh, Amos HP Angelina, Clara Wong, Meng Kang Tan, Sheng Hui Sukhatme, Sarvesh A Yeo, Trifanny Lim, Su Bin Lee, York Tien Soh, Shui Yen Leung, Wing Chang, Kenneth TE Chua, Yong Wei Alkaff, Syed MF Lim, Tony KH Lim, Chwee Teck Chen, Zhi Xiong |
Keywords: | Science & Technology Life Sciences & Biomedicine Oncology circulating tumor cells neuroblastoma minimal residual disease microfluidic bone marrow metastasis MINIMAL RESIDUAL DISEASE TYROSINE-HYDROXYLASE PERIPHERAL-BLOOD MOLECULAR-DETECTION UP-REGULATION CANCER CHILDREN ENRICHMENT MARKERS TIME |
Issue Date: | 13-Sep-2022 | Publisher: | FRONTIERS MEDIA SA | Citation: | Loh, Amos HP, Angelina, Clara, Wong, Meng Kang, Tan, Sheng Hui, Sukhatme, Sarvesh A, Yeo, Trifanny, Lim, Su Bin, Lee, York Tien, Soh, Shui Yen, Leung, Wing, Chang, Kenneth TE, Chua, Yong Wei, Alkaff, Syed MF, Lim, Tony KH, Lim, Chwee Teck, Chen, Zhi Xiong (2022-09-13). Pro-metastatic and mesenchymal gene expression signatures characterize circulating tumor cells of neuroblastoma patients with bone marrow metastases and relapse. FRONTIERS IN ONCOLOGY 12. ScholarBank@NUS Repository. https://doi.org/10.3389/fonc.2022.939460 | Abstract: | Existing marker-based methods of minimal residual disease (MRD) determination in neuroblastoma do not effectively enrich for the circulating disease cell population. Given the relative size differential of neuroblastoma tumor cells over normal hematogenous cells, we hypothesized that cell size-based separation could enrich circulating tumor cells (CTCs) from blood samples and disseminated tumor cells (DTCs) from bone marrow aspirates (BMA) of neuroblastoma patients, and that their gene expression profiles could vary dynamically with various disease states over the course of treatment. Using a spiral microfluidic chip, peripheral blood of 17 neuroblastoma patients at 3 serial treatment timepoints (diagnosis, n=17; post-chemotherapy, n=11; and relapse, n=3), and bone marrow samples at diagnosis were enriched for large intact circulating cells. Profiling the resulting enriched samples with immunohistochemistry and mRNA expression of 1490 cancer-related genes via NanoString, 13 of 17 samples contained CTCs displaying cytologic atypia, TH and PHOX2B expression and/or upregulation of cancer-associated genes. Gene signatures reflecting pro-metastatic processes and the neuroblastoma mesenchymal super-enhancer state were consistently upregulated in 7 of 13 samples, 6 of which also had metastatic high-risk disease. Expression of 8 genes associated with PI3K and GCPR signaling were significantly upregulated in CTCs of patients with bone marrow metastases versus patients without. Correspondingly, in patients with marrow metastases, differentially-expressed gene signatures reflected upregulation of immune regulation in bone marrow DTCs versus paired CTCs samples. In patients who later developed disease relapse, 5 genes involved in immune cell regulation, JAK/STAT signaling and the neuroblastoma mesenchymal super-enhancer state (OLFML2B, STAT1, ARHGDIB, STAB1, TLR2) were upregulated in serial CTC samples over their disease course, despite urinary catecholamines and bone marrow aspirates not indicating the disease recurrences. In summary, using a label-free cell size-based separation method, we enriched and characterized intact circulating cells in peripheral blood indicative of neuroblastoma CTCs, as well as their DTC counterparts in the bone marrow. Expression profiles of pro-metastatic genes in CTCs correlated with the presence of bone marrow metastases at diagnosis, while longitudinal profiling identified persistently elevated expression of genes in CTCs that may serve as novel predictive markers of hematogenous MRD in neuroblastoma patients that subsequently relapse. | Source Title: | FRONTIERS IN ONCOLOGY | URI: | https://scholarbank.nus.edu.sg/handle/10635/239175 | ISSN: | 2234-943X | DOI: | 10.3389/fonc.2022.939460 |
Appears in Collections: | Staff Publications Elements |
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