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多光谱氟-19磁共振成像能够对肿瘤相关巨噬细胞进行纵向和非侵入性监测。

Multispectral fluorine-19 MRI enables longitudinal and noninvasive monitoring of tumor-associated macrophages.

作者信息

Croci Davide, Santalla Méndez Rui, Temme Sebastian, Soukup Klara, Fournier Nadine, Zomer Anoek, Colotti Roberto, Wischnewski Vladimir, Flögel Ulrich, van Heeswijk Ruud B, Joyce Johanna A

机构信息

Department of Oncology, University of Lausanne, Lausanne 1011, Switzerland.

Ludwig Institute for Cancer Research, University of Lausanne, Lausanne 1011, Switzerland.

出版信息

Sci Transl Med. 2022 Oct 19;14(667):eabo2952. doi: 10.1126/scitranslmed.abo2952.

Abstract

High-grade gliomas, the most common and aggressive primary brain tumors, are characterized by a complex tumor microenvironment (TME). Among the immune cells infiltrating the glioma TME, tumor-associated microglia and macrophages (TAMs) constitute the major compartment. In patients with gliomas, increased TAM abundance is associated with more aggressive disease. Alterations in TAM phenotypes and functions have been reported in preclinical models of multiple cancers during tumor development and after therapeutic interventions, including radiotherapy and molecular targeted therapies. These findings indicate that it is crucial to evaluate TAM abundance and dynamics over time. Current techniques to quantify TAMs in patients rely mainly on histological staining of tumor biopsies. Although informative, these techniques require an invasive procedure to harvest the tissue sample and typically only result in a snapshot of a small region at a single point in time. Fluorine isotope 19 MRI (F MRI) represents a powerful means to noninvasively and longitudinally monitor myeloid cells in pathological conditions by intravenously injecting perfluorocarbon-containing nanoparticles (PFC-NP). In this study, we demonstrated the feasibility and power of F MRI in preclinical models of gliomagenesis, breast-to-brain metastasis, and breast cancer and showed that the major cellular source of F signal consists of TAMs. Moreover, multispectral F MRI with two different PFC-NP allowed us to identify spatially and temporally distinct TAM niches in radiotherapy-recurrent murine gliomas. Together, we have imaged TAMs noninvasively and longitudinally with integrated cellular, spatial, and temporal resolution, thus revealing important biological insights into the critical functions of TAMs, including in disease recurrence.

摘要

高级别胶质瘤是最常见且侵袭性最强的原发性脑肿瘤,其特征在于复杂的肿瘤微环境(TME)。在浸润胶质瘤TME的免疫细胞中,肿瘤相关小胶质细胞和巨噬细胞(TAM)构成了主要部分。在胶质瘤患者中,TAM丰度增加与疾病更具侵袭性相关。在多种癌症的临床前模型中,在肿瘤发展过程以及包括放疗和分子靶向治疗在内的治疗干预后,均报道了TAM表型和功能的改变。这些发现表明,评估TAM丰度及其随时间的动态变化至关重要。目前用于量化患者体内TAM的技术主要依赖于肿瘤活检组织的组织学染色。尽管这些技术提供了信息,但它们需要侵入性操作来获取组织样本,并且通常只能得到单个时间点小区域的快照。氟同位素19磁共振成像(F MRI)是一种强大的手段,可通过静脉注射含全氟化碳的纳米颗粒(PFC-NP),在病理条件下对髓样细胞进行无创和纵向监测。在本研究中,我们证明了F MRI在胶质瘤发生、脑转移和乳腺癌临床前模型中的可行性和有效性,并表明F信号的主要细胞来源是TAM。此外,使用两种不同PFC-NP的多光谱F MRI使我们能够在放疗复发的小鼠胶质瘤中识别出空间和时间上不同的TAM生态位。总之,我们以综合的细胞、空间和时间分辨率对TAM进行了无创和纵向成像,从而揭示了关于TAM关键功能的重要生物学见解,包括在疾病复发中的作用。

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