Self-driven immune checkpoint blockade and spatiotemporal-sensitive immune response monitoring in acute myeloid leukemia using an all-in-one turn-on bionanoprobe†

IF 6.1 3区 医学 Q1 MATERIALS SCIENCE, BIOMATERIALS
Dangui Zhang, Honglian Wu, Tianci Wang, Yuting Wang, Sixi Liu, Feiqiu Wen, Gerile Oudeng and Mo Yang
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Abstract

Immune checkpoint (ICP) blockade (ICB) is one of the most promising immunotherapies for acute myeloid leukemia (AML). However, owing to their heterogeneity, AML cells may cause uncoordinated metabolic fluxes and heterogeneous immune responses, inducing the release of a spatiotemporally sensitive immune response marker. Timely and in situ detection of immune responses in ICB therapy is important for therapeutic strategy adjustment. Herein, we constructed an all-in-one nanoprobe for self-driving ICB and simultaneously detecting an immune response in the same AML cell in vivo, thus enabling accurate evaluation of heterogenetic immune responses in living AML mice without additional drug treatment or probe processes. The nature-inspire polydopamine (PDA) nanoparticles loaded with an ICP blocker were targeted to the leukocyte immunoglobulin like receptor B4 (a new ICP) of AML cells to induce the release of immune response marker granzyme B (GrB). The PDA nanoparticles were additionally paired with carbon-derived graphene quantum dots (GQDs) to construct a full-organic ‘turn-on’ bionanoprobe that can transfer fluorescence resonance energy for GrB detection. This multifunctional nanoprobe was validated for triggering ICB therapy and monitoring the changes of GrB levels in real-time both in vitro and in vivo. The organic nanoprobe showed excellent permeability and retention in tumor cells and high biocompatibility in vivo. This bionanoprobe orderly interacted with the upstream ICP molecules and downstream signal molecule GrB, thereby achieving in situ immune response signals within the therapeutic efficacy evaluation window.

Abstract Image

自驱动免疫检查点阻断和时空敏感免疫反应监测在急性髓系白血病中使用一体化开启生物纳米探针。
免疫检查点阻断(ICP)是治疗急性粒细胞白血病(AML)最有前景的免疫疗法之一。然而,由于其异质性,AML细胞可能导致不协调的代谢通量和异质性免疫反应,从而诱导时空敏感的免疫反应标记物的释放。及时原位检测ICB治疗中的免疫反应对于调整治疗策略非常重要。在此,我们构建了一种用于自驱动ICB的一体式纳米探针,同时在体内检测同一AML细胞中的免疫反应,从而能够在没有额外药物治疗或探针过程的情况下准确评估活体AML小鼠的异质性免疫反应。将负载有ICP阻断剂的自然激发的聚多巴胺(PDA)纳米颗粒靶向AML细胞的白细胞免疫球蛋白样受体B4(一种新的ICP),以诱导免疫反应标记物颗粒酶B(GrB)的释放。PDA纳米颗粒还与碳衍生的石墨烯量子点(GQDs)配对,以构建一个完全有机的“开启”仿生探针,该探针可以转移用于GrB检测的荧光共振能量。这种多功能纳米探针被验证可以触发ICB治疗,并在体外和体内实时监测GrB水平的变化。该有机纳米探针在肿瘤细胞中表现出优异的渗透性和滞留性,在体内具有较高的生物相容性。该生物探针与上游ICP分子和下游信号分子GrB有序相互作用,从而在疗效评估窗口内实现原位免疫反应信号。
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来源期刊
Journal of Materials Chemistry B
Journal of Materials Chemistry B MATERIALS SCIENCE, BIOMATERIALS-
CiteScore
11.50
自引率
4.30%
发文量
866
期刊介绍: Journal of Materials Chemistry A, B & C cover high quality studies across all fields of materials chemistry. The journals focus on those theoretical or experimental studies that report new understanding, applications, properties and synthesis of materials. Journal of Materials Chemistry A, B & C are separated by the intended application of the material studied. Broadly, applications in energy and sustainability are of interest to Journal of Materials Chemistry A, applications in biology and medicine are of interest to Journal of Materials Chemistry B, and applications in optical, magnetic and electronic devices are of interest to Journal of Materials Chemistry C.Journal of Materials Chemistry B is a Transformative Journal and Plan S compliant. Example topic areas within the scope of Journal of Materials Chemistry B are listed below. This list is neither exhaustive nor exclusive: Antifouling coatings Biocompatible materials Bioelectronics Bioimaging Biomimetics Biomineralisation Bionics Biosensors Diagnostics Drug delivery Gene delivery Immunobiology Nanomedicine Regenerative medicine & Tissue engineering Scaffolds Soft robotics Stem cells Therapeutic devices
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