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高比例的CD16 +单核细胞与慢性淋巴细胞白血病患者的骨侵蚀程度相关:白血病B细胞在单核细胞分化和破骨细胞成熟中的作用。

A High Percentage of CD16+ Monocytes Correlates with the Extent of Bone Erosion in Chronic Lymphocytic Leukemia Patients: The Impact of Leukemic B Cells in Monocyte Differentiation and Osteoclast Maturation.

作者信息

Giannoni Paolo, Marini Cecilia, Cutrona Giovanna, Todoerti Katia, Neri Antonino, Ibatici Adalberto, Sambuceti Gianmario, Pigozzi Simona, Mora Marco, Ferrarini Manlio, Fais Franco, de Totero Daniela

机构信息

Department of Experimental Medicine, Biology Section, University of Genova, 16132 Genova, Italy.

CNR Institute of Bioimages and Molecular Physiology, 20054 Milano, Italy.

出版信息

Cancers (Basel). 2022 Dec 3;14(23):5979. doi: 10.3390/cancers14235979.

Abstract

Significant skeletal alterations are present in Chronic Lymphocytic Leukemia (CLL) patients; bone erosion, particularly evident in the long bone shaft, appeared increased in the progressive disease stage. Moreover, the partial colonization of the bone with reactive bone marrow we documented via PET-FDG imaging suggests that neoplastic cell overgrowth contributes to bone derangement. Indeed, cytokines released by leukemic B cells impair osteoblast differentiation and enhance osteoclast formation in vitro. CD16, Fcγ-RIIIa, has been previously indicated as a marker of osteoclast precursors. We demonstrate, here, that the percentage of circulating monocytes, CD16+, is significantly higher in CLL patients than in normal controls and directly correlated with the extent of bone erosion. When we assessed if healthy monocytes, treated with a CLL-conditioned medium, modulated RANK, RANKL and CD16, we observed that all these molecules were up-regulated and CD16 to a greater extent. Altogether, these findings suggest that leukemic cells facilitate osteoclast differentiation. Interestingly, the evidence that monocytes, polarized toward the M2 phenotype, were characterized by high CD16 expression and showed a striking propensity to differentiate toward osteoclasts may provide further explanations for the enhanced levels of bone erosion detected, in agreement with the high number of immunosuppressive-M2 cells present in these patients.

摘要

慢性淋巴细胞白血病(CLL)患者存在显著的骨骼改变;骨侵蚀在长骨干尤为明显,在疾病进展阶段有所增加。此外,我们通过PET-FDG成像记录到反应性骨髓对骨的部分定植,这表明肿瘤细胞过度生长导致了骨紊乱。事实上,白血病B细胞释放的细胞因子在体外会损害成骨细胞分化并增强破骨细胞形成。CD16,即Fcγ-RIIIa,先前已被指出是破骨细胞前体的标志物。我们在此证明,CLL患者循环单核细胞(CD16+)的百分比显著高于正常对照,且与骨侵蚀程度直接相关。当我们评估用CLL条件培养基处理的健康单核细胞是否调节RANK、RANKL和CD16时,我们观察到所有这些分子均上调,且CD16上调程度更大。总之,这些发现表明白血病细胞促进破骨细胞分化。有趣的是,向M2表型极化的单核细胞具有高CD16表达且表现出向破骨细胞分化的显著倾向,这一证据可能为检测到的骨侵蚀水平升高提供进一步解释,这与这些患者中存在大量免疫抑制性M2细胞一致。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6bca/9740193/e312a3709313/cancers-14-05979-g001.jpg

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