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癌症患者和健康供体血浆中细胞外小囊泡的腺苷能活性评估。

Assessment of adenosinergic activity of small extracellular vesicles in plasma of cancer patients and healthy donors.

作者信息

Hong Chang Sook, Menchikova Elizabeth V, Najjar Yana, Whiteside Theresa L, Jackson Edwin K

机构信息

Department of Pathology, University of Pittsburgh School of Medicine, Pittsburgh, PA, USA.

Cancer Research, UPMC Hillman Cancer Center, Pittsburgh, PA, USA.

出版信息

Oncoimmunology. 2025 Dec;14(1):2444704. doi: 10.1080/2162402X.2024.2444704. Epub 2024 Dec 20.

Abstract

The adenosinergic pathway converting endogenous ATP to adenosine (ADO) is a major immunosuppressive pathway in cancer. Emerging data indicate that plasma small extracellular vesicles (sEV) express CD39 and CD73 and produce ADO. Using a noninvasive, highly sensitive newly developed assay, metabolism of N-etheno-labeled eATP, eADP or eAMP by ecto-nucleotidases on the external surface of sEV was measured using high pressure liquid chromatography with fluorescence detection. Ecto-nucleotidase activity in sEV isolated from plasma of randomly selected cancer patients and healthy donors (HDs) was compared. Relative to sEV of HDs, sEV from the plasma of melanoma patients metabolized eATP to eADP and eAMP to eADO with significantly greater efficiency. Activities of both CD39 and CD73 were elevated, as determined by the use of pharmacologic inhibitors selective for these enzymes. In contrast, metabolic activity of CD39 and CD73 on sEV isolated from plasma of patients with head and neck cancer was comparable to that of HDs, suggesting that the activity of ecto-nucleotidases on sEV may differ depending on the cancer type or cancer stage. The N-etheno-purine assay measuring contributions of ecto-nucleotidases residing on the surface of sEV to the extracellular ATP to ADO pathway can discriminate cancer patients from HDs, differentiate among different cancer types, and potentially identify patients most likely to benefit from anti-adenosinergic therapy designed to inhibit the adenosine-mediated immune suppression.

摘要

将内源性三磷酸腺苷(ATP)转化为腺苷(ADO)的腺苷能途径是癌症中的一条主要免疫抑制途径。新出现的数据表明,血浆小细胞外囊泡(sEV)表达CD39和CD73并产生ADO。使用一种新开发的非侵入性、高灵敏度检测方法,通过带有荧光检测的高压液相色谱法测量sEV外表面上的外切核苷酸酶对N-乙烯基标记的eATP、eADP或eAMP的代谢。比较了从随机选择的癌症患者和健康供体(HD)血浆中分离出的sEV中的外切核苷酸酶活性。相对于HD的sEV,黑色素瘤患者血浆中的sEV将eATP代谢为eADP以及将eAMP代谢为eADO的效率显著更高。通过使用对这些酶具有选择性的药理抑制剂确定,CD39和CD73的活性均升高。相比之下,从头颈癌患者血浆中分离出的sEV上CD39和CD73的代谢活性与HD的相当,这表明sEV上外切核苷酸酶的活性可能因癌症类型或癌症阶段而异。测量sEV表面上的外切核苷酸酶对细胞外ATP至ADO途径贡献的N-乙烯基嘌呤检测方法可以区分癌症患者和HD,区分不同癌症类型,并有可能识别出最有可能从旨在抑制腺苷介导的免疫抑制的抗腺苷能疗法中受益的患者。

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